Novel drug fails to prevent contrast-induced nephropathy

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Novel drug fails to prevent contrast-induced nephropathy

CHICAGO – CMX-2043, a novel agent intended for prevention of contrast-induced nephropathy, failed in the phase II, double-blind, placebo-controlled CARIN clinical trial presented at the annual meeting of the American College of Cardiology.

The drug had also shown promise in small preliminary studies for the prevention of periprocedural myocardial infarction in patients undergoing coronary stenting. There again, however, CMX-2043 – a derivative of alpha lipoic acid with antioxidant and cell membrane–stabilizing properties – proved ineffective in the 361-patient, 31-center phase II trial, reported Dr. Deepak L. Bhatt, professor of medicine at Harvard Medical School and executive director of interventional cardiovascular programs at Brigham and Women’s Hospital, both in Boston.

Dr. Deepak L. Bhatt

All participants in CARIN had baseline severe impairment of kidney function or mild to moderate renal impairment plus another risk factor, such as diabetes or age greater than 75 years. One hour prior to coronary angiography, they received various doses of CMX-2043 or placebo.

Unfortunately, no difference between the four treatment arms was present in terms of the primary study endpoint: the incidence of acute kidney injury as defined by at least a 0.3 mg/dL rise in serum creatinine from baseline on day 4. No dose response to CMX-2043 was evident, nor did the investigational agent have any impact on the risk of major adverse cardiovascular events.

Immediately prior to Dr. Bhatt’s presentation, Dr. Michelle L. O’Donoghue of Brigham and Women’s Hospital presented the equally negative results of the LATITUDE-TIMI 60 trial, a phase III trial of the investigational mitogen-activated protein kinase inhibitor losmapimod, a drug developed to improve outcomes in patients with an acute coronary syndrome.

“It’s a bit distressing” to witness back to back presentations of clinical trials that proved resoundingly negative despite very strong-looking preliminary data, commented discussant Dr. Anthony N. DeMaria, professor of medicine at the University of California, San Diego. What’s going on here? he asked.

“I think it’s a fundamental truth that a lot of things that look good in preclinical work, even when backed up by a lot of solid science, don’t pan out in human studies,” Dr. Bhatt replied. “That’s a challenge, and probably in no other arena more so than in tackling inflammation and antioxidant therapy.

“There’s a graveyard of compounds that have not worked, and now we’ve perhaps added another one,” Dr. Bhatt continued. “But it doesn’t mean that scientific inquiry isn’t important, because I think eventually we’ll have drugs for these problems, whether it’s reperfusion injury or contrast-induced nephropathy. It’ll probably just take a lot more time and effort.”

The one solace regarding the CARIN trial, in Dr. Bhatt’s view, is that it highlighted the advantages of what is known as an adaptive trial design. Instead of jumping from positive early-phase results straight to a definitive 10,000-patient phase III clinical trial, investigators were able to obtain answers regarding the drug’s ability to prevent two major problems in patients undergoing coronary angiography – contrast-induced nephropathy and major adverse cardiac events – by means of a single 361-patient trial that was comparatively inexpensive.

Acute kidney injury secondary to exposure to contrast agents remains a significant problem, with an incidence of 20%-25% in high-risk patients. Numerous proposed prophylactic agents have ultimately proved not useful, including sodium bicarbonate, N-acetylcysteine, and intravenous fenoldopam.

Indeed, the only preventive measures of proven effectiveness are hydration with saline for 12 hours preangioplasty, and limiting the volume of contrast agent used. In real-world clinical practice, however, it’s often impractical to administer the optimal 12 hours of saline because of hospital pressure to get patients out quickly, Dr. Bhatt observed.

“There remains an important unmet clinical need to find agents that reduce the occurrence of contrast nephropathy,” he stressed.

Ischemix funded the CARIN trial. Dr. Bhatt reported receiving a research grant from the company that was directed to Brigham and Women’s Hospital.

bjancin@frontlinemedcom.com

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CHICAGO – CMX-2043, a novel agent intended for prevention of contrast-induced nephropathy, failed in the phase II, double-blind, placebo-controlled CARIN clinical trial presented at the annual meeting of the American College of Cardiology.

The drug had also shown promise in small preliminary studies for the prevention of periprocedural myocardial infarction in patients undergoing coronary stenting. There again, however, CMX-2043 – a derivative of alpha lipoic acid with antioxidant and cell membrane–stabilizing properties – proved ineffective in the 361-patient, 31-center phase II trial, reported Dr. Deepak L. Bhatt, professor of medicine at Harvard Medical School and executive director of interventional cardiovascular programs at Brigham and Women’s Hospital, both in Boston.

Dr. Deepak L. Bhatt

All participants in CARIN had baseline severe impairment of kidney function or mild to moderate renal impairment plus another risk factor, such as diabetes or age greater than 75 years. One hour prior to coronary angiography, they received various doses of CMX-2043 or placebo.

Unfortunately, no difference between the four treatment arms was present in terms of the primary study endpoint: the incidence of acute kidney injury as defined by at least a 0.3 mg/dL rise in serum creatinine from baseline on day 4. No dose response to CMX-2043 was evident, nor did the investigational agent have any impact on the risk of major adverse cardiovascular events.

Immediately prior to Dr. Bhatt’s presentation, Dr. Michelle L. O’Donoghue of Brigham and Women’s Hospital presented the equally negative results of the LATITUDE-TIMI 60 trial, a phase III trial of the investigational mitogen-activated protein kinase inhibitor losmapimod, a drug developed to improve outcomes in patients with an acute coronary syndrome.

“It’s a bit distressing” to witness back to back presentations of clinical trials that proved resoundingly negative despite very strong-looking preliminary data, commented discussant Dr. Anthony N. DeMaria, professor of medicine at the University of California, San Diego. What’s going on here? he asked.

“I think it’s a fundamental truth that a lot of things that look good in preclinical work, even when backed up by a lot of solid science, don’t pan out in human studies,” Dr. Bhatt replied. “That’s a challenge, and probably in no other arena more so than in tackling inflammation and antioxidant therapy.

“There’s a graveyard of compounds that have not worked, and now we’ve perhaps added another one,” Dr. Bhatt continued. “But it doesn’t mean that scientific inquiry isn’t important, because I think eventually we’ll have drugs for these problems, whether it’s reperfusion injury or contrast-induced nephropathy. It’ll probably just take a lot more time and effort.”

The one solace regarding the CARIN trial, in Dr. Bhatt’s view, is that it highlighted the advantages of what is known as an adaptive trial design. Instead of jumping from positive early-phase results straight to a definitive 10,000-patient phase III clinical trial, investigators were able to obtain answers regarding the drug’s ability to prevent two major problems in patients undergoing coronary angiography – contrast-induced nephropathy and major adverse cardiac events – by means of a single 361-patient trial that was comparatively inexpensive.

Acute kidney injury secondary to exposure to contrast agents remains a significant problem, with an incidence of 20%-25% in high-risk patients. Numerous proposed prophylactic agents have ultimately proved not useful, including sodium bicarbonate, N-acetylcysteine, and intravenous fenoldopam.

Indeed, the only preventive measures of proven effectiveness are hydration with saline for 12 hours preangioplasty, and limiting the volume of contrast agent used. In real-world clinical practice, however, it’s often impractical to administer the optimal 12 hours of saline because of hospital pressure to get patients out quickly, Dr. Bhatt observed.

“There remains an important unmet clinical need to find agents that reduce the occurrence of contrast nephropathy,” he stressed.

Ischemix funded the CARIN trial. Dr. Bhatt reported receiving a research grant from the company that was directed to Brigham and Women’s Hospital.

bjancin@frontlinemedcom.com

CHICAGO – CMX-2043, a novel agent intended for prevention of contrast-induced nephropathy, failed in the phase II, double-blind, placebo-controlled CARIN clinical trial presented at the annual meeting of the American College of Cardiology.

The drug had also shown promise in small preliminary studies for the prevention of periprocedural myocardial infarction in patients undergoing coronary stenting. There again, however, CMX-2043 – a derivative of alpha lipoic acid with antioxidant and cell membrane–stabilizing properties – proved ineffective in the 361-patient, 31-center phase II trial, reported Dr. Deepak L. Bhatt, professor of medicine at Harvard Medical School and executive director of interventional cardiovascular programs at Brigham and Women’s Hospital, both in Boston.

Dr. Deepak L. Bhatt

All participants in CARIN had baseline severe impairment of kidney function or mild to moderate renal impairment plus another risk factor, such as diabetes or age greater than 75 years. One hour prior to coronary angiography, they received various doses of CMX-2043 or placebo.

Unfortunately, no difference between the four treatment arms was present in terms of the primary study endpoint: the incidence of acute kidney injury as defined by at least a 0.3 mg/dL rise in serum creatinine from baseline on day 4. No dose response to CMX-2043 was evident, nor did the investigational agent have any impact on the risk of major adverse cardiovascular events.

Immediately prior to Dr. Bhatt’s presentation, Dr. Michelle L. O’Donoghue of Brigham and Women’s Hospital presented the equally negative results of the LATITUDE-TIMI 60 trial, a phase III trial of the investigational mitogen-activated protein kinase inhibitor losmapimod, a drug developed to improve outcomes in patients with an acute coronary syndrome.

“It’s a bit distressing” to witness back to back presentations of clinical trials that proved resoundingly negative despite very strong-looking preliminary data, commented discussant Dr. Anthony N. DeMaria, professor of medicine at the University of California, San Diego. What’s going on here? he asked.

“I think it’s a fundamental truth that a lot of things that look good in preclinical work, even when backed up by a lot of solid science, don’t pan out in human studies,” Dr. Bhatt replied. “That’s a challenge, and probably in no other arena more so than in tackling inflammation and antioxidant therapy.

“There’s a graveyard of compounds that have not worked, and now we’ve perhaps added another one,” Dr. Bhatt continued. “But it doesn’t mean that scientific inquiry isn’t important, because I think eventually we’ll have drugs for these problems, whether it’s reperfusion injury or contrast-induced nephropathy. It’ll probably just take a lot more time and effort.”

The one solace regarding the CARIN trial, in Dr. Bhatt’s view, is that it highlighted the advantages of what is known as an adaptive trial design. Instead of jumping from positive early-phase results straight to a definitive 10,000-patient phase III clinical trial, investigators were able to obtain answers regarding the drug’s ability to prevent two major problems in patients undergoing coronary angiography – contrast-induced nephropathy and major adverse cardiac events – by means of a single 361-patient trial that was comparatively inexpensive.

Acute kidney injury secondary to exposure to contrast agents remains a significant problem, with an incidence of 20%-25% in high-risk patients. Numerous proposed prophylactic agents have ultimately proved not useful, including sodium bicarbonate, N-acetylcysteine, and intravenous fenoldopam.

Indeed, the only preventive measures of proven effectiveness are hydration with saline for 12 hours preangioplasty, and limiting the volume of contrast agent used. In real-world clinical practice, however, it’s often impractical to administer the optimal 12 hours of saline because of hospital pressure to get patients out quickly, Dr. Bhatt observed.

“There remains an important unmet clinical need to find agents that reduce the occurrence of contrast nephropathy,” he stressed.

Ischemix funded the CARIN trial. Dr. Bhatt reported receiving a research grant from the company that was directed to Brigham and Women’s Hospital.

bjancin@frontlinemedcom.com

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Novel drug fails to prevent contrast-induced nephropathy
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Key clinical point: There continues to be a major unmet need for agents that reduce the risk of contrast-induced nephropathy.

Major finding: The once-promising investigational antioxidant and cell membrane stabilizer CMX-2043 proved ineffective for prevention of renal or cardiac injuries in patients undergoing coronary angiography.

Data source: This randomized, double-blind, placebo-controlled, 31-center, phase II study involved 361 patients with baseline renal impairment, all of whom were scheduled for coronary angiography.

Disclosures: Ischemix funded the study. Dr. Bhatt reported receiving a research grant from the company that was directed to Brigham and Women’s Hospital.

Stem cells show heart failure benefits in phase II trial

Results merit phase III trial follow-up
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Stem cells show heart failure benefits in phase II trial

CHICAGO – After rattling around in early-stage clinical studies for more than a decade, stem cell therapy for heart failure may have finally gained the efficacy evidence to send it to the next level: large-scale, phase III trials.

Patients with ischemic cardiomyopathy and severe heart failure showed a statistically significant 37% relative reduction in their combined rate of death and cardiovascular hospitalization during 1 year of follow-up after autologous stem cell injections to their left ventricular myocardium in a multicenter, fully blinded control, phase II trial with 109 North American patients.

Mitchel L. Zoler/Frontline Medical News
Dr. Timothy D. Henry

The treatment used a technique in commercial development by Vericel that selectively expands ex vivo bone marrow cells taken from the heart failure patient. Clinicians inject 0.4 mL aliquots of the expanded cells – enriched for mesenchymal stem cells and M2 macrophages – via a transcatheter approach into the left ventricular myocardium using 12-17 injections per patient. The bone marrow preparation during ex vivo expansion is called ixmyelocel-T.

This treatment now needs testing in more patients, Dr. Timothy D. Henry said at the annual meeting of the American College of Cardiology. “We need a new generation of cell trials in larger studies with completely double-blind, placebo controls using a more uniform preparation of cells,” said Dr. Henry.

“To the best of our knowledge, ixCELL-DCM is the largest randomized, double-blind clinical trial to date for cell therapy use in congestive heart failure,” said Dr. Henry and his associates in their report. The concept of stem cell therapy to replace damaged myocardium “has been very attractive, but most clinical trials to date have been small and unblinded, and used unselected bone marrow cells,” explained Dr. Henry, director of cardiology at the Cedars-Sinai Heart Institute in Los Angeles.

The ixCELL-DCM study ran at 31 sites in the United States and Canada. About 90% of patients had New York Heart Association class III disease, the average left ventricular ejection fraction was about 25%, patients on average would cover about 310 m during a 6-minute walk test, and the average serum level of NT-ProBNP was about 1,900 pg/L. Patients in the control arm all underwent the same bone marrow retrieval and transcatheter injection into the left ventricle, but the injections only contained carrier material without active cells.

The primary endpoint of death or a cardiovascular event, primarily hospitalization, occurred at a rate of 110 events per 100 patient years during 1-year follow-up of 51 patients in the sham-treatment group. In the active-treatment arm, the endpoint occurred at a rate of 70 events per 100 patient years among 58 patients. The difference was primarily driven by a 3% death rate with cell therapy, compared with a 14% rate in the controls, and a 38% hospitalization rate, compared with a 47% rate among controls.

The study results appeared online concurrent with Dr. Henry’s report (Lancet. 2016 Apr 5. doi: 10.1016/S0140-6736[16]30137-4).

The results showed no significant differences between the active and sham groups for changes in left ventricular size, ejection fraction, and 6-minute walk distance.

“This trial was designed to look at events. It is not a cause for concern that we did not see effects on heart function,” Dr. Henry said. The current results were also generally consistent with results from two earlier, controlled, phase II studies with a total of 61 patients (Circ Res. 2014 Sep 26;115[8]:730-7).

In the safety analysis, done in 114 patients, the rates of all adverse events and major adverse cardiovascular events were similar in the two arms. The rate of serious adverse events was significantly reduced in the patients treated with expanded bone marrow cells, compared with the controls.

The high rate of death and hospitalization of patients with severe heart failure “is a very large, unmet need, so it’s a natural to go to a larger trial,” Dr. Henry said. “The cell preparation was very safe and easy to do.”

Another pressing research issue is to try to understand the mechanism by which the cell treatment improves clinical outcomes, with improved heart function or improved exercise capacity apparently excluded as mechanisms.

The trial was sponsored by Vericel, the company developing the ex vivo protocol for selective marrow cell expansion. Dr. Henry has been a consultant to or received honoraria from Abbott Vascular, Baxter, Capricor, Cytori, Eli Lilly, and the Medicines Company, and he has received research grants from Aastrom, Baxter International, Mesoblast, and Vericel.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

References

Body

The results reported by Dr. Henry come from one of the first trials of stem cell or bone marrow treatment of failing hearts that used clinical outcomes as the primary endpoint. In contrast, prior studies focused on changes in functional characteristics of patients, such as 6-minute walk distance or left ventricular ejection fraction or size. What makes Dr. Henry’s study distinctive is that it showed benefit for a clinical outcome: the rate of death or cardiovascular hospitalization.

Another distinct difference, compared with the vast majority of earlier trials, was the way the bone marrow was handled prior to placement in a heart. The bone marrow cells underwent a 12-day period of ex vivo treatment designed to expand the content of certain mesenchymal stem cells and macrophages.

The current study was also larger than most prior reported studies, with 114 randomized patients available for the safety analysis and 109 for the efficacy analysis. But by no means was this a large study; in fact, it is relatively small. Although it produced a statistically significant result for the primary endpoint, the efficacy needs expanded testing in larger numbers.

It’s currently unclear how the expanded bone marrow cell injections improve clinical status and lead to reduced deaths and hospitalization. The results show essentially no impact from the treatment on ejection fraction or 6-minute walk distance, raising the question of what alternative mechanisms link this treatment to improved clinical outcomes.

Until now, it has not been possible to move beyond early-stage trial designs for cell therapy of failing hearts. Now, for the first time, we have study results that suggest a phase III trial is indicated.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

Dr. John A. Jarcho is a deputy editor of the New England Journal of Medicine and a cardiologist at Brigham and Women’s Hospital, both in Boston. He had no disclosures. He made these comments as a discussant of Dr. Henry’s report and in an interview.

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The results reported by Dr. Henry come from one of the first trials of stem cell or bone marrow treatment of failing hearts that used clinical outcomes as the primary endpoint. In contrast, prior studies focused on changes in functional characteristics of patients, such as 6-minute walk distance or left ventricular ejection fraction or size. What makes Dr. Henry’s study distinctive is that it showed benefit for a clinical outcome: the rate of death or cardiovascular hospitalization.

Another distinct difference, compared with the vast majority of earlier trials, was the way the bone marrow was handled prior to placement in a heart. The bone marrow cells underwent a 12-day period of ex vivo treatment designed to expand the content of certain mesenchymal stem cells and macrophages.

The current study was also larger than most prior reported studies, with 114 randomized patients available for the safety analysis and 109 for the efficacy analysis. But by no means was this a large study; in fact, it is relatively small. Although it produced a statistically significant result for the primary endpoint, the efficacy needs expanded testing in larger numbers.

It’s currently unclear how the expanded bone marrow cell injections improve clinical status and lead to reduced deaths and hospitalization. The results show essentially no impact from the treatment on ejection fraction or 6-minute walk distance, raising the question of what alternative mechanisms link this treatment to improved clinical outcomes.

Until now, it has not been possible to move beyond early-stage trial designs for cell therapy of failing hearts. Now, for the first time, we have study results that suggest a phase III trial is indicated.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

Dr. John A. Jarcho is a deputy editor of the New England Journal of Medicine and a cardiologist at Brigham and Women’s Hospital, both in Boston. He had no disclosures. He made these comments as a discussant of Dr. Henry’s report and in an interview.

Body

The results reported by Dr. Henry come from one of the first trials of stem cell or bone marrow treatment of failing hearts that used clinical outcomes as the primary endpoint. In contrast, prior studies focused on changes in functional characteristics of patients, such as 6-minute walk distance or left ventricular ejection fraction or size. What makes Dr. Henry’s study distinctive is that it showed benefit for a clinical outcome: the rate of death or cardiovascular hospitalization.

Another distinct difference, compared with the vast majority of earlier trials, was the way the bone marrow was handled prior to placement in a heart. The bone marrow cells underwent a 12-day period of ex vivo treatment designed to expand the content of certain mesenchymal stem cells and macrophages.

The current study was also larger than most prior reported studies, with 114 randomized patients available for the safety analysis and 109 for the efficacy analysis. But by no means was this a large study; in fact, it is relatively small. Although it produced a statistically significant result for the primary endpoint, the efficacy needs expanded testing in larger numbers.

It’s currently unclear how the expanded bone marrow cell injections improve clinical status and lead to reduced deaths and hospitalization. The results show essentially no impact from the treatment on ejection fraction or 6-minute walk distance, raising the question of what alternative mechanisms link this treatment to improved clinical outcomes.

Until now, it has not been possible to move beyond early-stage trial designs for cell therapy of failing hearts. Now, for the first time, we have study results that suggest a phase III trial is indicated.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

Dr. John A. Jarcho is a deputy editor of the New England Journal of Medicine and a cardiologist at Brigham and Women’s Hospital, both in Boston. He had no disclosures. He made these comments as a discussant of Dr. Henry’s report and in an interview.

Title
Results merit phase III trial follow-up
Results merit phase III trial follow-up

CHICAGO – After rattling around in early-stage clinical studies for more than a decade, stem cell therapy for heart failure may have finally gained the efficacy evidence to send it to the next level: large-scale, phase III trials.

Patients with ischemic cardiomyopathy and severe heart failure showed a statistically significant 37% relative reduction in their combined rate of death and cardiovascular hospitalization during 1 year of follow-up after autologous stem cell injections to their left ventricular myocardium in a multicenter, fully blinded control, phase II trial with 109 North American patients.

Mitchel L. Zoler/Frontline Medical News
Dr. Timothy D. Henry

The treatment used a technique in commercial development by Vericel that selectively expands ex vivo bone marrow cells taken from the heart failure patient. Clinicians inject 0.4 mL aliquots of the expanded cells – enriched for mesenchymal stem cells and M2 macrophages – via a transcatheter approach into the left ventricular myocardium using 12-17 injections per patient. The bone marrow preparation during ex vivo expansion is called ixmyelocel-T.

This treatment now needs testing in more patients, Dr. Timothy D. Henry said at the annual meeting of the American College of Cardiology. “We need a new generation of cell trials in larger studies with completely double-blind, placebo controls using a more uniform preparation of cells,” said Dr. Henry.

“To the best of our knowledge, ixCELL-DCM is the largest randomized, double-blind clinical trial to date for cell therapy use in congestive heart failure,” said Dr. Henry and his associates in their report. The concept of stem cell therapy to replace damaged myocardium “has been very attractive, but most clinical trials to date have been small and unblinded, and used unselected bone marrow cells,” explained Dr. Henry, director of cardiology at the Cedars-Sinai Heart Institute in Los Angeles.

The ixCELL-DCM study ran at 31 sites in the United States and Canada. About 90% of patients had New York Heart Association class III disease, the average left ventricular ejection fraction was about 25%, patients on average would cover about 310 m during a 6-minute walk test, and the average serum level of NT-ProBNP was about 1,900 pg/L. Patients in the control arm all underwent the same bone marrow retrieval and transcatheter injection into the left ventricle, but the injections only contained carrier material without active cells.

The primary endpoint of death or a cardiovascular event, primarily hospitalization, occurred at a rate of 110 events per 100 patient years during 1-year follow-up of 51 patients in the sham-treatment group. In the active-treatment arm, the endpoint occurred at a rate of 70 events per 100 patient years among 58 patients. The difference was primarily driven by a 3% death rate with cell therapy, compared with a 14% rate in the controls, and a 38% hospitalization rate, compared with a 47% rate among controls.

The study results appeared online concurrent with Dr. Henry’s report (Lancet. 2016 Apr 5. doi: 10.1016/S0140-6736[16]30137-4).

The results showed no significant differences between the active and sham groups for changes in left ventricular size, ejection fraction, and 6-minute walk distance.

“This trial was designed to look at events. It is not a cause for concern that we did not see effects on heart function,” Dr. Henry said. The current results were also generally consistent with results from two earlier, controlled, phase II studies with a total of 61 patients (Circ Res. 2014 Sep 26;115[8]:730-7).

In the safety analysis, done in 114 patients, the rates of all adverse events and major adverse cardiovascular events were similar in the two arms. The rate of serious adverse events was significantly reduced in the patients treated with expanded bone marrow cells, compared with the controls.

The high rate of death and hospitalization of patients with severe heart failure “is a very large, unmet need, so it’s a natural to go to a larger trial,” Dr. Henry said. “The cell preparation was very safe and easy to do.”

Another pressing research issue is to try to understand the mechanism by which the cell treatment improves clinical outcomes, with improved heart function or improved exercise capacity apparently excluded as mechanisms.

The trial was sponsored by Vericel, the company developing the ex vivo protocol for selective marrow cell expansion. Dr. Henry has been a consultant to or received honoraria from Abbott Vascular, Baxter, Capricor, Cytori, Eli Lilly, and the Medicines Company, and he has received research grants from Aastrom, Baxter International, Mesoblast, and Vericel.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

CHICAGO – After rattling around in early-stage clinical studies for more than a decade, stem cell therapy for heart failure may have finally gained the efficacy evidence to send it to the next level: large-scale, phase III trials.

Patients with ischemic cardiomyopathy and severe heart failure showed a statistically significant 37% relative reduction in their combined rate of death and cardiovascular hospitalization during 1 year of follow-up after autologous stem cell injections to their left ventricular myocardium in a multicenter, fully blinded control, phase II trial with 109 North American patients.

Mitchel L. Zoler/Frontline Medical News
Dr. Timothy D. Henry

The treatment used a technique in commercial development by Vericel that selectively expands ex vivo bone marrow cells taken from the heart failure patient. Clinicians inject 0.4 mL aliquots of the expanded cells – enriched for mesenchymal stem cells and M2 macrophages – via a transcatheter approach into the left ventricular myocardium using 12-17 injections per patient. The bone marrow preparation during ex vivo expansion is called ixmyelocel-T.

This treatment now needs testing in more patients, Dr. Timothy D. Henry said at the annual meeting of the American College of Cardiology. “We need a new generation of cell trials in larger studies with completely double-blind, placebo controls using a more uniform preparation of cells,” said Dr. Henry.

“To the best of our knowledge, ixCELL-DCM is the largest randomized, double-blind clinical trial to date for cell therapy use in congestive heart failure,” said Dr. Henry and his associates in their report. The concept of stem cell therapy to replace damaged myocardium “has been very attractive, but most clinical trials to date have been small and unblinded, and used unselected bone marrow cells,” explained Dr. Henry, director of cardiology at the Cedars-Sinai Heart Institute in Los Angeles.

The ixCELL-DCM study ran at 31 sites in the United States and Canada. About 90% of patients had New York Heart Association class III disease, the average left ventricular ejection fraction was about 25%, patients on average would cover about 310 m during a 6-minute walk test, and the average serum level of NT-ProBNP was about 1,900 pg/L. Patients in the control arm all underwent the same bone marrow retrieval and transcatheter injection into the left ventricle, but the injections only contained carrier material without active cells.

The primary endpoint of death or a cardiovascular event, primarily hospitalization, occurred at a rate of 110 events per 100 patient years during 1-year follow-up of 51 patients in the sham-treatment group. In the active-treatment arm, the endpoint occurred at a rate of 70 events per 100 patient years among 58 patients. The difference was primarily driven by a 3% death rate with cell therapy, compared with a 14% rate in the controls, and a 38% hospitalization rate, compared with a 47% rate among controls.

The study results appeared online concurrent with Dr. Henry’s report (Lancet. 2016 Apr 5. doi: 10.1016/S0140-6736[16]30137-4).

The results showed no significant differences between the active and sham groups for changes in left ventricular size, ejection fraction, and 6-minute walk distance.

“This trial was designed to look at events. It is not a cause for concern that we did not see effects on heart function,” Dr. Henry said. The current results were also generally consistent with results from two earlier, controlled, phase II studies with a total of 61 patients (Circ Res. 2014 Sep 26;115[8]:730-7).

In the safety analysis, done in 114 patients, the rates of all adverse events and major adverse cardiovascular events were similar in the two arms. The rate of serious adverse events was significantly reduced in the patients treated with expanded bone marrow cells, compared with the controls.

The high rate of death and hospitalization of patients with severe heart failure “is a very large, unmet need, so it’s a natural to go to a larger trial,” Dr. Henry said. “The cell preparation was very safe and easy to do.”

Another pressing research issue is to try to understand the mechanism by which the cell treatment improves clinical outcomes, with improved heart function or improved exercise capacity apparently excluded as mechanisms.

The trial was sponsored by Vericel, the company developing the ex vivo protocol for selective marrow cell expansion. Dr. Henry has been a consultant to or received honoraria from Abbott Vascular, Baxter, Capricor, Cytori, Eli Lilly, and the Medicines Company, and he has received research grants from Aastrom, Baxter International, Mesoblast, and Vericel.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Key clinical point: Severe, ischemic heart failure patients had a significant cut in death and cardiovascular hospitalizations 1 year after endovascular myocardial injection with selectively expanded autologous bone marrow cells in a fully blinded, placebo-controlled phase II study.

Major finding: Cell-treated patients had a 37% drop in death and cardiovascular hospitalization relative to controls in 1-year follow-up.

Data source: A multicenter, fully blinded study with 109 patients for the per protocol efficacy analysis, and 114 patients for the safety analysis.

Disclosures: The trial was sponsored by Vericel, the company developing the ex vivo protocol for selective marrow cell expansion. Dr. Henry has been a consultant to or received honoraria from Abbott Vascular, Baxter, Capricor, Cytori, Eli Lilly, and the Medicines Company, and he has received research grants from Aastrom, Baxter International, Mesoblast, and Vericel.

Early antiarrhythmic drugs boost survival in shock-refractory cardiac arrest

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Early antiarrhythmic drugs boost survival in shock-refractory cardiac arrest

CHICAGO – Paramedic-administered amiodarone or lidocaine during resuscitation of patients with shock-refractory ventricular fibrillation or ventricular tachycardia of out-of-hospital cardiac arrest significantly improves survival, according to the findings of the largest-ever clinical trial of out-of-hospital cardiac arrest.

However, the survival advantage was limited to bystander-witnessed arrest. The reason for this difference in the Amiodarone, Lidocaine or Placebo Study (ALPS) is that observed arrest is a good surrogate for earlier recognition and treatment of an out-of-hospital cardiac arrest (OHCA), Dr. Peter J. Kudenchuk explained in presenting the study findings at the annual meeting of the American College of Cardiology.

Dr. Peter Kudenchuk

“The message from this trial is that, if you give these drugs to everyone across the board with out-of-hospital shock-refractory VF/VT cardiac arrest, you’ll help those who can be helped and you won’t hurt those who are beyond help,” said Dr. Kudenchuk, professor of medicine at the University of Washington, Seattle.

ALPS was a randomized, blinded, placebo-controlled clinical trial of 3,026 patients with shock-refractory VF/VT OHCA at 10 U.S. and Canadian sites participating in the Resuscitation Outcomes Consortium. Subjects were randomized to paramedic-administered treatment with prefilled syringes of amiodarone, lidocaine, or placebo. Time to treatment averaged 19 minutes from the initial call made to emergency services.

The primary endpoint in ALPS was survival to hospital discharge. Rates were 24.4% in the amiodarone group, 23.7% with lidocaine, and 21% with placebo. Differences in survival rates between the antiarrhythmic drug and placebo groups approached but did not achieve statistical significance.

Survival to hospital discharge in the 1,934 participants with bystander-witnessed arrest was a prespecified secondary endpoint. That outcome was achieved in 27.7% of the amiodarone group and 27.8% who got lidocaine, compared with 22.7% of placebo-treated patients. Those differences were statistically significant and clinically meaningful, Dr. Kudenchuk asserted.

“Though these differences – an absolute 5% improvement over placebo – may seem small, were we to implement this as policy, upwards of 1,800 more lives could potentially be saved each year in the United States alone,” said Dr. Kudenchuk, an electrophysiologist and cardiologist.

Bystander-witnessed OHCA was 2.3-fold more common than unwitnessed arrest. In the unwitnessed arrest subgroup there was no hint of benefit for either amiodarone or lidocaine.

“Many patients with unwitnessed arrest have already sustained mortal ischemic damage by the time they’re found,” he observed. “If you go into a morgue and give the best drug in the world, you’re not going to save anybody.”

Moreover, among the roughly 5% of patients whose OHCA was witnessed by EMS personnel, survival to hospital discharge was a whopping absolute 22% greater with antiarrhythmic drug therapy than with placebo.

“Taken together, these findings suggest that treatment sooner after heart collapse may be a critical determinant of drug effect,” Dr. Kudenchuk continued.

He said the ALPS findings are generalizable to all communities across North America where the local EMS system follows the Resuscitation Outcomes Consortium philosophy that early defibrillation and good CPR are the cornerstones of effective management of OHCA, without which no treatment can be effective.

Current use of these drugs across the United States is not standardized. “It is really a free-for-all,” according to Dr. Kudenchuk. “Some agencies strictly use lidocaine, others may use amiodarone. Some use both. And some use neither. I think in part that’s because current guideline recommendations give these drugs a class IIb recommendation – meaning they’re optional – because up until this point there have been no data to support their effectiveness in changing outcome.”

In his view, the ALPS data clearly warrant upgrading the strength of the recommendation for antiarrhythmic drug therapy in the next iteration of the guidelines. Although he is on the guideline committee, Dr. Kudenchuk added, he cannot predict what the committee as a whole will decide.

ALPS will not lead to a change in practice such that paramedic-administered antiarrhythmic agents are given only to patients with witnessed arrest, Dr. Kudenchuk said. It’s not practical for rescue personnel in the midst of the fray to try to figure out whether an OHCA was witnessed or not. Plus, there’s an ethical issue involved.

“If we’d wanted to hit the headlines with a major trial with a positive outcome we would have selected only people with witnessed cardiac arrest from the get-go to do this trial, since we guessed that’s where the money was going to be. The reality is you can’t treat people that way. Everyone has to have a chance,” he said.

Asked which antiarrhythmic drug the next edition of the resuscitation guidelines should recommend preferentially, he said ALPS wasn’t powered to distinguish between amiodarone and lidocaine. “If I were writing the guidelines, I would simply say either or both happens to be okay.”

 

 

An important footnote is that ALPS utilized a new, Food and Drug Administration–approved formulation of amiodarone, known as Nexterone, designed to reduce hypotensive effects. Had investigators employed the more familiar version of the drug, the safety results wouldn’t have been as good.

Out-of-hospital cardiac arrest accounts for roughly 350,000 deaths per year in the United States

Simultaneously with Dr. Kudenchuk’s presentation of the ALPS findings at ACC 16 in Chicago, the results were published online (N Engl J Med. 2016 Apr 4; doi: 10.1056/NEJMoa1514204).

He reported having no financial conflicts regarding the ALPS study, which was funded by the National Heart, Lung, and Blood Institute, the Canadian Institutes of Health Research, the American Heart Association, the U.S. Army, and Defense Research and Development Canada.

bjancin@frontlinemedcom.com

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CHICAGO – Paramedic-administered amiodarone or lidocaine during resuscitation of patients with shock-refractory ventricular fibrillation or ventricular tachycardia of out-of-hospital cardiac arrest significantly improves survival, according to the findings of the largest-ever clinical trial of out-of-hospital cardiac arrest.

However, the survival advantage was limited to bystander-witnessed arrest. The reason for this difference in the Amiodarone, Lidocaine or Placebo Study (ALPS) is that observed arrest is a good surrogate for earlier recognition and treatment of an out-of-hospital cardiac arrest (OHCA), Dr. Peter J. Kudenchuk explained in presenting the study findings at the annual meeting of the American College of Cardiology.

Dr. Peter Kudenchuk

“The message from this trial is that, if you give these drugs to everyone across the board with out-of-hospital shock-refractory VF/VT cardiac arrest, you’ll help those who can be helped and you won’t hurt those who are beyond help,” said Dr. Kudenchuk, professor of medicine at the University of Washington, Seattle.

ALPS was a randomized, blinded, placebo-controlled clinical trial of 3,026 patients with shock-refractory VF/VT OHCA at 10 U.S. and Canadian sites participating in the Resuscitation Outcomes Consortium. Subjects were randomized to paramedic-administered treatment with prefilled syringes of amiodarone, lidocaine, or placebo. Time to treatment averaged 19 minutes from the initial call made to emergency services.

The primary endpoint in ALPS was survival to hospital discharge. Rates were 24.4% in the amiodarone group, 23.7% with lidocaine, and 21% with placebo. Differences in survival rates between the antiarrhythmic drug and placebo groups approached but did not achieve statistical significance.

Survival to hospital discharge in the 1,934 participants with bystander-witnessed arrest was a prespecified secondary endpoint. That outcome was achieved in 27.7% of the amiodarone group and 27.8% who got lidocaine, compared with 22.7% of placebo-treated patients. Those differences were statistically significant and clinically meaningful, Dr. Kudenchuk asserted.

“Though these differences – an absolute 5% improvement over placebo – may seem small, were we to implement this as policy, upwards of 1,800 more lives could potentially be saved each year in the United States alone,” said Dr. Kudenchuk, an electrophysiologist and cardiologist.

Bystander-witnessed OHCA was 2.3-fold more common than unwitnessed arrest. In the unwitnessed arrest subgroup there was no hint of benefit for either amiodarone or lidocaine.

“Many patients with unwitnessed arrest have already sustained mortal ischemic damage by the time they’re found,” he observed. “If you go into a morgue and give the best drug in the world, you’re not going to save anybody.”

Moreover, among the roughly 5% of patients whose OHCA was witnessed by EMS personnel, survival to hospital discharge was a whopping absolute 22% greater with antiarrhythmic drug therapy than with placebo.

“Taken together, these findings suggest that treatment sooner after heart collapse may be a critical determinant of drug effect,” Dr. Kudenchuk continued.

He said the ALPS findings are generalizable to all communities across North America where the local EMS system follows the Resuscitation Outcomes Consortium philosophy that early defibrillation and good CPR are the cornerstones of effective management of OHCA, without which no treatment can be effective.

Current use of these drugs across the United States is not standardized. “It is really a free-for-all,” according to Dr. Kudenchuk. “Some agencies strictly use lidocaine, others may use amiodarone. Some use both. And some use neither. I think in part that’s because current guideline recommendations give these drugs a class IIb recommendation – meaning they’re optional – because up until this point there have been no data to support their effectiveness in changing outcome.”

In his view, the ALPS data clearly warrant upgrading the strength of the recommendation for antiarrhythmic drug therapy in the next iteration of the guidelines. Although he is on the guideline committee, Dr. Kudenchuk added, he cannot predict what the committee as a whole will decide.

ALPS will not lead to a change in practice such that paramedic-administered antiarrhythmic agents are given only to patients with witnessed arrest, Dr. Kudenchuk said. It’s not practical for rescue personnel in the midst of the fray to try to figure out whether an OHCA was witnessed or not. Plus, there’s an ethical issue involved.

“If we’d wanted to hit the headlines with a major trial with a positive outcome we would have selected only people with witnessed cardiac arrest from the get-go to do this trial, since we guessed that’s where the money was going to be. The reality is you can’t treat people that way. Everyone has to have a chance,” he said.

Asked which antiarrhythmic drug the next edition of the resuscitation guidelines should recommend preferentially, he said ALPS wasn’t powered to distinguish between amiodarone and lidocaine. “If I were writing the guidelines, I would simply say either or both happens to be okay.”

 

 

An important footnote is that ALPS utilized a new, Food and Drug Administration–approved formulation of amiodarone, known as Nexterone, designed to reduce hypotensive effects. Had investigators employed the more familiar version of the drug, the safety results wouldn’t have been as good.

Out-of-hospital cardiac arrest accounts for roughly 350,000 deaths per year in the United States

Simultaneously with Dr. Kudenchuk’s presentation of the ALPS findings at ACC 16 in Chicago, the results were published online (N Engl J Med. 2016 Apr 4; doi: 10.1056/NEJMoa1514204).

He reported having no financial conflicts regarding the ALPS study, which was funded by the National Heart, Lung, and Blood Institute, the Canadian Institutes of Health Research, the American Heart Association, the U.S. Army, and Defense Research and Development Canada.

bjancin@frontlinemedcom.com

CHICAGO – Paramedic-administered amiodarone or lidocaine during resuscitation of patients with shock-refractory ventricular fibrillation or ventricular tachycardia of out-of-hospital cardiac arrest significantly improves survival, according to the findings of the largest-ever clinical trial of out-of-hospital cardiac arrest.

However, the survival advantage was limited to bystander-witnessed arrest. The reason for this difference in the Amiodarone, Lidocaine or Placebo Study (ALPS) is that observed arrest is a good surrogate for earlier recognition and treatment of an out-of-hospital cardiac arrest (OHCA), Dr. Peter J. Kudenchuk explained in presenting the study findings at the annual meeting of the American College of Cardiology.

Dr. Peter Kudenchuk

“The message from this trial is that, if you give these drugs to everyone across the board with out-of-hospital shock-refractory VF/VT cardiac arrest, you’ll help those who can be helped and you won’t hurt those who are beyond help,” said Dr. Kudenchuk, professor of medicine at the University of Washington, Seattle.

ALPS was a randomized, blinded, placebo-controlled clinical trial of 3,026 patients with shock-refractory VF/VT OHCA at 10 U.S. and Canadian sites participating in the Resuscitation Outcomes Consortium. Subjects were randomized to paramedic-administered treatment with prefilled syringes of amiodarone, lidocaine, or placebo. Time to treatment averaged 19 minutes from the initial call made to emergency services.

The primary endpoint in ALPS was survival to hospital discharge. Rates were 24.4% in the amiodarone group, 23.7% with lidocaine, and 21% with placebo. Differences in survival rates between the antiarrhythmic drug and placebo groups approached but did not achieve statistical significance.

Survival to hospital discharge in the 1,934 participants with bystander-witnessed arrest was a prespecified secondary endpoint. That outcome was achieved in 27.7% of the amiodarone group and 27.8% who got lidocaine, compared with 22.7% of placebo-treated patients. Those differences were statistically significant and clinically meaningful, Dr. Kudenchuk asserted.

“Though these differences – an absolute 5% improvement over placebo – may seem small, were we to implement this as policy, upwards of 1,800 more lives could potentially be saved each year in the United States alone,” said Dr. Kudenchuk, an electrophysiologist and cardiologist.

Bystander-witnessed OHCA was 2.3-fold more common than unwitnessed arrest. In the unwitnessed arrest subgroup there was no hint of benefit for either amiodarone or lidocaine.

“Many patients with unwitnessed arrest have already sustained mortal ischemic damage by the time they’re found,” he observed. “If you go into a morgue and give the best drug in the world, you’re not going to save anybody.”

Moreover, among the roughly 5% of patients whose OHCA was witnessed by EMS personnel, survival to hospital discharge was a whopping absolute 22% greater with antiarrhythmic drug therapy than with placebo.

“Taken together, these findings suggest that treatment sooner after heart collapse may be a critical determinant of drug effect,” Dr. Kudenchuk continued.

He said the ALPS findings are generalizable to all communities across North America where the local EMS system follows the Resuscitation Outcomes Consortium philosophy that early defibrillation and good CPR are the cornerstones of effective management of OHCA, without which no treatment can be effective.

Current use of these drugs across the United States is not standardized. “It is really a free-for-all,” according to Dr. Kudenchuk. “Some agencies strictly use lidocaine, others may use amiodarone. Some use both. And some use neither. I think in part that’s because current guideline recommendations give these drugs a class IIb recommendation – meaning they’re optional – because up until this point there have been no data to support their effectiveness in changing outcome.”

In his view, the ALPS data clearly warrant upgrading the strength of the recommendation for antiarrhythmic drug therapy in the next iteration of the guidelines. Although he is on the guideline committee, Dr. Kudenchuk added, he cannot predict what the committee as a whole will decide.

ALPS will not lead to a change in practice such that paramedic-administered antiarrhythmic agents are given only to patients with witnessed arrest, Dr. Kudenchuk said. It’s not practical for rescue personnel in the midst of the fray to try to figure out whether an OHCA was witnessed or not. Plus, there’s an ethical issue involved.

“If we’d wanted to hit the headlines with a major trial with a positive outcome we would have selected only people with witnessed cardiac arrest from the get-go to do this trial, since we guessed that’s where the money was going to be. The reality is you can’t treat people that way. Everyone has to have a chance,” he said.

Asked which antiarrhythmic drug the next edition of the resuscitation guidelines should recommend preferentially, he said ALPS wasn’t powered to distinguish between amiodarone and lidocaine. “If I were writing the guidelines, I would simply say either or both happens to be okay.”

 

 

An important footnote is that ALPS utilized a new, Food and Drug Administration–approved formulation of amiodarone, known as Nexterone, designed to reduce hypotensive effects. Had investigators employed the more familiar version of the drug, the safety results wouldn’t have been as good.

Out-of-hospital cardiac arrest accounts for roughly 350,000 deaths per year in the United States

Simultaneously with Dr. Kudenchuk’s presentation of the ALPS findings at ACC 16 in Chicago, the results were published online (N Engl J Med. 2016 Apr 4; doi: 10.1056/NEJMoa1514204).

He reported having no financial conflicts regarding the ALPS study, which was funded by the National Heart, Lung, and Blood Institute, the Canadian Institutes of Health Research, the American Heart Association, the U.S. Army, and Defense Research and Development Canada.

bjancin@frontlinemedcom.com

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Key clinical point: Routine use of injectable amiodarone or lidocaine by paramedics in cases of shock-refractory VF/VT out-of-hospital cardiac arrest would save at least 1,800 lives per year in the U.S.

Major finding: Survival to hospital discharge was an absolute 5% greater when such patients got the antiarrhythmic compared with placebo.

Data source: A blinded, randomized, placebo-controlled clinical trial of 3,026 subjects at 10 sites.

Disclosures: The National Heart, Lung, and Blood Institute, the Canadian Institutes of Health Research, the American Heart Association, the U.S. Army, and Defense Research and Development Canada funded the ALPS trial. The presenter reported having no financial conflicts of interest.

FIRE AND ICE trial called a win for cryoablation of AF

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FIRE AND ICE trial called a win for cryoablation of AF

CHICAGO – The largest-ever randomized trial of catheter ablation of atrial fibrillation has ended in a draw between radiofrequency and cryoballoon ablation in safety and efficacy – and that actually represents a win for cryoablation, a simpler and far more easily mastered procedure, Dr. Karl-Heinz Kuck said at the annual meeting of the American College of Cardiology.

“We can teach physicians how to do cryoablation much more easily. That will allow more patients with atrial fibrillation to get access to catheter ablation, which is what we really need,” according to Dr. Kuck, principal investigator in the poetically named FIRE AND ICE trial and head of cardiology at St. Georg Hospital in Hamburg (Germany).

Dr. Karl-Heinz Kuck

FIRE AND ICE included 769 patients in eight European countries. The participants, all of whom had antiarrhythmic drug–refractory paroxysmal atrial fibrillation (AF), were randomized to radiofrequency ablation – the long-time standard – or to cryoablation, a newer technology. Radiofrequency ablation was guided by three-dimensional electroanatomic mapping, while cryoablation utilized fluoroscopic guidance.

The primary efficacy endpoint was the 1-year rate of clinical failure, defined as an occurrence of AF, atrial flutter, or atrial tachycardia lasting for at least 30 seconds, or repeat ablation or the use of antiarrhythmic drugs following a 90-day postprocedural blanking period. The clinical failure rate was 34.6% in the cryoballoon group and similar at 35.9% in the radiofrequency group.

Serious treatment-related adverse events occurred in 10.2% of the cryoballoon group and 12.8% of the radiofrequency group, a nonsignificant difference. No procedural deaths occurred in the study.

There were, however, several significant procedural differences. Procedure time averaged 124 minutes in the cryoablation group, nearly 20 minutes less than the 142 minutes for radiofrequency ablation. However, the 17-minute fluoroscopy time in the radiofrequency group was 5 minutes shorter than for cryoablation.

Dr. Kuck said the study underestimates the true procedural differences because FIRE AND ICE was carried out by extremely experienced operators. In routine clinical practice involving non-elite operators, it’s not unusual for radiofrequency ablation fluoroscopy times to be two or even three times longer than the 17 minutes seen in the study. Plus, FIRE AND ICE was conducted when the procedure entailed two applications of the cryoballoon. Now only one application is recommended, cutting an additional 12 minutes off the total procedure time, he added.

Radiofrequency ablation takes longer because it entails creating a series of point-to-point lesions in a circle to isolate the pulmonary veins. With cryoablation, the balloon is moved into position, inflated, and a 3-minute-freeze is administered to create a circle of necrotic tissue in a single-step procedure.

Dr. Hugh Calkins, MD

Discussant Dr. Hugh G. Calkins praised the FIRE AND ICE investigators’ use of a rigorous definition of recurrence that required as little as a 30-second episode of atrial arrhythmia.

“That’s a very high bar, so I think the results are very impressive,” said Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

He commented that “this study is a clear reminder that 90% success rates just don’t happen in this field,” despite what some practitioners have claimed.

Asked how he predicts the study results will influence the field of AF ablation, Dr. Kuck replied that he foresees much wider adoption of cryoablation and a stronger endorsement of the technology in updated guideline recommendations.

“I personally believe this will be the most important development in our field in the next several years,” he added.

The electrophysiologist noted that even though current guidelines give a class Ia recommendation to catheter ablation of paroxysmal AF that’s refractory to at least one antiarrhythmic drug, at present only 4% of such patients actually undergo the procedure.

“Having just 4% of patients with AF undergo catheter ablation cannot be what we are looking for as physicians,” Dr. Kuck said. “I believe if we want to roll out catheter ablation for AF, we need simple and safe tools. This trial elegantly shows that with a simpler device that allows single-shot isolation of the pulmonary veins, we can get the same safety and efficacy as with radiofrequency ablation. I often tell people that radiofrequency ablation of atrial fibrillation is the most challenging procedure in all cardiology. We do this procedure from the groin in a moving heart. It’s a very complex technology.”

His dream, he continued, is that cryoablation will eventually enable patients with atrial fibrillation to be managed the same way electrophysiologists treat patients with Wolff-Parkinson-White syndrome; with the first episode, the patient goes to the electrophysiology catheterization lab for an ablation procedure.

 

 

“I think there’s a great message here: The cryoballoon will move catheter ablation from a niche procedure performed in specialized centers by the few guys in the world who can do it really well out into the broader world. To do that you need a tool that is safe, simple, and can be handled by the average doctor,” Dr. Kuck said.

Discussant Dr. Anthony DeMaria commented that it would be premature at this point to start thinking about cryoablation as a first approach to new-onset AF, given the roughly 35% clinical failure rate at 1 year seen in FIRE AND ICE. That rate doubtless would have been even higher had patients been equipped with implantable loop recorders, added Dr. DeMaria, professor of medicine at the University of California, San Diego.

Dr. Kuck conceded that the high recurrence rate is one of the great unsolved limitations of catheter ablation of AF.

“We don’t know how to get the pulmonary veins permanently isolated,” he said. “We can create acute lesions, but over time what we’ve seen is recovery of tissue and then reconduction by the pulmonary veins. I believe that 20% of the 40% recurrence rate is due to reconduction from the pulmonary veins, and the rest is probably due to triggers coming from other sites.”

The FIRE AND ICE trial was funded in part by Medtronic, which markets the Arctic Front Advance cryoablation catheter used in the study. Dr. Kuck reported serving on a speakers’ bureau for Medtronic and acting as a consultant to Biosense Webster, Edwards, and St. Jude.

Simultaneous with Dr. Kuck’s presentation at ACC 16, the results of FIRE AND ICE were published online (N Engl J Med. 2016 Apr 4. doi: 10.1056/NEJMoa1602014).

bjancin@frontlinemedcom.com

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CHICAGO – The largest-ever randomized trial of catheter ablation of atrial fibrillation has ended in a draw between radiofrequency and cryoballoon ablation in safety and efficacy – and that actually represents a win for cryoablation, a simpler and far more easily mastered procedure, Dr. Karl-Heinz Kuck said at the annual meeting of the American College of Cardiology.

“We can teach physicians how to do cryoablation much more easily. That will allow more patients with atrial fibrillation to get access to catheter ablation, which is what we really need,” according to Dr. Kuck, principal investigator in the poetically named FIRE AND ICE trial and head of cardiology at St. Georg Hospital in Hamburg (Germany).

Dr. Karl-Heinz Kuck

FIRE AND ICE included 769 patients in eight European countries. The participants, all of whom had antiarrhythmic drug–refractory paroxysmal atrial fibrillation (AF), were randomized to radiofrequency ablation – the long-time standard – or to cryoablation, a newer technology. Radiofrequency ablation was guided by three-dimensional electroanatomic mapping, while cryoablation utilized fluoroscopic guidance.

The primary efficacy endpoint was the 1-year rate of clinical failure, defined as an occurrence of AF, atrial flutter, or atrial tachycardia lasting for at least 30 seconds, or repeat ablation or the use of antiarrhythmic drugs following a 90-day postprocedural blanking period. The clinical failure rate was 34.6% in the cryoballoon group and similar at 35.9% in the radiofrequency group.

Serious treatment-related adverse events occurred in 10.2% of the cryoballoon group and 12.8% of the radiofrequency group, a nonsignificant difference. No procedural deaths occurred in the study.

There were, however, several significant procedural differences. Procedure time averaged 124 minutes in the cryoablation group, nearly 20 minutes less than the 142 minutes for radiofrequency ablation. However, the 17-minute fluoroscopy time in the radiofrequency group was 5 minutes shorter than for cryoablation.

Dr. Kuck said the study underestimates the true procedural differences because FIRE AND ICE was carried out by extremely experienced operators. In routine clinical practice involving non-elite operators, it’s not unusual for radiofrequency ablation fluoroscopy times to be two or even three times longer than the 17 minutes seen in the study. Plus, FIRE AND ICE was conducted when the procedure entailed two applications of the cryoballoon. Now only one application is recommended, cutting an additional 12 minutes off the total procedure time, he added.

Radiofrequency ablation takes longer because it entails creating a series of point-to-point lesions in a circle to isolate the pulmonary veins. With cryoablation, the balloon is moved into position, inflated, and a 3-minute-freeze is administered to create a circle of necrotic tissue in a single-step procedure.

Dr. Hugh Calkins, MD

Discussant Dr. Hugh G. Calkins praised the FIRE AND ICE investigators’ use of a rigorous definition of recurrence that required as little as a 30-second episode of atrial arrhythmia.

“That’s a very high bar, so I think the results are very impressive,” said Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

He commented that “this study is a clear reminder that 90% success rates just don’t happen in this field,” despite what some practitioners have claimed.

Asked how he predicts the study results will influence the field of AF ablation, Dr. Kuck replied that he foresees much wider adoption of cryoablation and a stronger endorsement of the technology in updated guideline recommendations.

“I personally believe this will be the most important development in our field in the next several years,” he added.

The electrophysiologist noted that even though current guidelines give a class Ia recommendation to catheter ablation of paroxysmal AF that’s refractory to at least one antiarrhythmic drug, at present only 4% of such patients actually undergo the procedure.

“Having just 4% of patients with AF undergo catheter ablation cannot be what we are looking for as physicians,” Dr. Kuck said. “I believe if we want to roll out catheter ablation for AF, we need simple and safe tools. This trial elegantly shows that with a simpler device that allows single-shot isolation of the pulmonary veins, we can get the same safety and efficacy as with radiofrequency ablation. I often tell people that radiofrequency ablation of atrial fibrillation is the most challenging procedure in all cardiology. We do this procedure from the groin in a moving heart. It’s a very complex technology.”

His dream, he continued, is that cryoablation will eventually enable patients with atrial fibrillation to be managed the same way electrophysiologists treat patients with Wolff-Parkinson-White syndrome; with the first episode, the patient goes to the electrophysiology catheterization lab for an ablation procedure.

 

 

“I think there’s a great message here: The cryoballoon will move catheter ablation from a niche procedure performed in specialized centers by the few guys in the world who can do it really well out into the broader world. To do that you need a tool that is safe, simple, and can be handled by the average doctor,” Dr. Kuck said.

Discussant Dr. Anthony DeMaria commented that it would be premature at this point to start thinking about cryoablation as a first approach to new-onset AF, given the roughly 35% clinical failure rate at 1 year seen in FIRE AND ICE. That rate doubtless would have been even higher had patients been equipped with implantable loop recorders, added Dr. DeMaria, professor of medicine at the University of California, San Diego.

Dr. Kuck conceded that the high recurrence rate is one of the great unsolved limitations of catheter ablation of AF.

“We don’t know how to get the pulmonary veins permanently isolated,” he said. “We can create acute lesions, but over time what we’ve seen is recovery of tissue and then reconduction by the pulmonary veins. I believe that 20% of the 40% recurrence rate is due to reconduction from the pulmonary veins, and the rest is probably due to triggers coming from other sites.”

The FIRE AND ICE trial was funded in part by Medtronic, which markets the Arctic Front Advance cryoablation catheter used in the study. Dr. Kuck reported serving on a speakers’ bureau for Medtronic and acting as a consultant to Biosense Webster, Edwards, and St. Jude.

Simultaneous with Dr. Kuck’s presentation at ACC 16, the results of FIRE AND ICE were published online (N Engl J Med. 2016 Apr 4. doi: 10.1056/NEJMoa1602014).

bjancin@frontlinemedcom.com

CHICAGO – The largest-ever randomized trial of catheter ablation of atrial fibrillation has ended in a draw between radiofrequency and cryoballoon ablation in safety and efficacy – and that actually represents a win for cryoablation, a simpler and far more easily mastered procedure, Dr. Karl-Heinz Kuck said at the annual meeting of the American College of Cardiology.

“We can teach physicians how to do cryoablation much more easily. That will allow more patients with atrial fibrillation to get access to catheter ablation, which is what we really need,” according to Dr. Kuck, principal investigator in the poetically named FIRE AND ICE trial and head of cardiology at St. Georg Hospital in Hamburg (Germany).

Dr. Karl-Heinz Kuck

FIRE AND ICE included 769 patients in eight European countries. The participants, all of whom had antiarrhythmic drug–refractory paroxysmal atrial fibrillation (AF), were randomized to radiofrequency ablation – the long-time standard – or to cryoablation, a newer technology. Radiofrequency ablation was guided by three-dimensional electroanatomic mapping, while cryoablation utilized fluoroscopic guidance.

The primary efficacy endpoint was the 1-year rate of clinical failure, defined as an occurrence of AF, atrial flutter, or atrial tachycardia lasting for at least 30 seconds, or repeat ablation or the use of antiarrhythmic drugs following a 90-day postprocedural blanking period. The clinical failure rate was 34.6% in the cryoballoon group and similar at 35.9% in the radiofrequency group.

Serious treatment-related adverse events occurred in 10.2% of the cryoballoon group and 12.8% of the radiofrequency group, a nonsignificant difference. No procedural deaths occurred in the study.

There were, however, several significant procedural differences. Procedure time averaged 124 minutes in the cryoablation group, nearly 20 minutes less than the 142 minutes for radiofrequency ablation. However, the 17-minute fluoroscopy time in the radiofrequency group was 5 minutes shorter than for cryoablation.

Dr. Kuck said the study underestimates the true procedural differences because FIRE AND ICE was carried out by extremely experienced operators. In routine clinical practice involving non-elite operators, it’s not unusual for radiofrequency ablation fluoroscopy times to be two or even three times longer than the 17 minutes seen in the study. Plus, FIRE AND ICE was conducted when the procedure entailed two applications of the cryoballoon. Now only one application is recommended, cutting an additional 12 minutes off the total procedure time, he added.

Radiofrequency ablation takes longer because it entails creating a series of point-to-point lesions in a circle to isolate the pulmonary veins. With cryoablation, the balloon is moved into position, inflated, and a 3-minute-freeze is administered to create a circle of necrotic tissue in a single-step procedure.

Dr. Hugh Calkins, MD

Discussant Dr. Hugh G. Calkins praised the FIRE AND ICE investigators’ use of a rigorous definition of recurrence that required as little as a 30-second episode of atrial arrhythmia.

“That’s a very high bar, so I think the results are very impressive,” said Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

He commented that “this study is a clear reminder that 90% success rates just don’t happen in this field,” despite what some practitioners have claimed.

Asked how he predicts the study results will influence the field of AF ablation, Dr. Kuck replied that he foresees much wider adoption of cryoablation and a stronger endorsement of the technology in updated guideline recommendations.

“I personally believe this will be the most important development in our field in the next several years,” he added.

The electrophysiologist noted that even though current guidelines give a class Ia recommendation to catheter ablation of paroxysmal AF that’s refractory to at least one antiarrhythmic drug, at present only 4% of such patients actually undergo the procedure.

“Having just 4% of patients with AF undergo catheter ablation cannot be what we are looking for as physicians,” Dr. Kuck said. “I believe if we want to roll out catheter ablation for AF, we need simple and safe tools. This trial elegantly shows that with a simpler device that allows single-shot isolation of the pulmonary veins, we can get the same safety and efficacy as with radiofrequency ablation. I often tell people that radiofrequency ablation of atrial fibrillation is the most challenging procedure in all cardiology. We do this procedure from the groin in a moving heart. It’s a very complex technology.”

His dream, he continued, is that cryoablation will eventually enable patients with atrial fibrillation to be managed the same way electrophysiologists treat patients with Wolff-Parkinson-White syndrome; with the first episode, the patient goes to the electrophysiology catheterization lab for an ablation procedure.

 

 

“I think there’s a great message here: The cryoballoon will move catheter ablation from a niche procedure performed in specialized centers by the few guys in the world who can do it really well out into the broader world. To do that you need a tool that is safe, simple, and can be handled by the average doctor,” Dr. Kuck said.

Discussant Dr. Anthony DeMaria commented that it would be premature at this point to start thinking about cryoablation as a first approach to new-onset AF, given the roughly 35% clinical failure rate at 1 year seen in FIRE AND ICE. That rate doubtless would have been even higher had patients been equipped with implantable loop recorders, added Dr. DeMaria, professor of medicine at the University of California, San Diego.

Dr. Kuck conceded that the high recurrence rate is one of the great unsolved limitations of catheter ablation of AF.

“We don’t know how to get the pulmonary veins permanently isolated,” he said. “We can create acute lesions, but over time what we’ve seen is recovery of tissue and then reconduction by the pulmonary veins. I believe that 20% of the 40% recurrence rate is due to reconduction from the pulmonary veins, and the rest is probably due to triggers coming from other sites.”

The FIRE AND ICE trial was funded in part by Medtronic, which markets the Arctic Front Advance cryoablation catheter used in the study. Dr. Kuck reported serving on a speakers’ bureau for Medtronic and acting as a consultant to Biosense Webster, Edwards, and St. Jude.

Simultaneous with Dr. Kuck’s presentation at ACC 16, the results of FIRE AND ICE were published online (N Engl J Med. 2016 Apr 4. doi: 10.1056/NEJMoa1602014).

bjancin@frontlinemedcom.com

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Key clinical point: Cryoablation of atrial fibrillation offers significant advantages over radiofrequency ablation.

Major finding: In a rigorous randomized trial, cryoablation of atrial fibrillation had a 34.6% clinical failure rate at 1 year, similar to the 35.9% rate for radiofrequency ablation.

Data source: The FIRE AND ICE trial, which randomized 769 patients with paroxysmal atrial fibrillation in eight European countries.

Disclosures: FIRE AND ICE was funded in part by Medtronic. The presenter reported serving on a speakers’ bureau for the company.

VIDEO: Sapien 3 TAVR bests surgery in intermediate-risk patients

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CHICAGO – Transcatheter aortic valve replacement (TAVR) using Sapien 3 – the latest-generation valve – is associated with low mortality, stroke, and paravalvular regurgitation rates at 1 year in intermediate-risk patients, and is superior to surgical valve replacement, according to findings from the SAPIEN 3 study.

The mortality rate at 1 year in the 1,077 patients in the observational study was 7.4% overall and 6.5% in a transfemoral access subgroup, the disabling stroke rate was 2.3%, the aortic valve reintervention rate was 0.6%, and the moderate/severe paravalvular regurgitation rate was 1.5%, Dr. Vinod H. Thourani reported on behalf of the PARTNER trial investigators at the annual meeting of the American College of Cardiology. The findings were published simultaneously in The Lancet (2016 Apr 3. doi: 10.1016/So140-6736[19]30073-3).

Sherry Boschert/IMNG Medical Media
Dr. Vinod Thourani

A prespecified propensity score analysis comparing 963 SAPIEN 3 patients with 747 similar intermediate-risk patients from the PARTNER 2A trial who underwent surgical valve replacement showed that not only was Sapien 3 TAVR noninferior to surgery for the primary composite endpoint of mortality, strokes, and moderate or severe aortic regurgitation, it was also superior to surgery (pooled weighted proportion difference, –9.2% for each). The differences were highly statistically significant.

In fact, Sapien 3 TAVR “blew it out of the water” for both noninferiority and superiority vs. surgery, Dr. Thourani of Emory University, Atlanta said.

The propensity score incorporated 22 characteristics, and the analysis was conducted by blinded investigators. Even using the most conservative strategy for the analysis as approved by the Food and Drug Administration, with the heaviest weighting against TAVR, Sapien 3 TAVR was superior to surgery for the primary composite endpoint, he noted.

Of note, while Sapien 3 TAVR was superior for the individual components of mortality and stroke from the composite endpoint, surgery was superior to Sapien 3 TAVR for the component of moderate or greater aortic regurgitation, he said.

However, the findings represent “strong evidence that in intermediate-risk patients with severe aortic stenosis, SAPIEN 3, compared to surgery, improves clinical outcomes and is the preferred therapy,” he concluded.

In a video interview, he said that if approved by the FDA, “this will become the impetus for [use in] a lower-risk population of patients. Currently we have the inoperative and high-risk patients, and this will open up the intermediate-risk patients for having transcatheter valve therapies, and I think it becomes exceedingly powerful.”

Two ongoing industry-sponsored randomized trials in low-risk patients (those with a Society of Thoracic Surgeons score of less than 4) are underway, he noted.

Sapien 3 TAVR was previously shown to improve 30-day outcomes in intermediate-risk patients with severe aortic stenosis (Eur Heart J. 2016 Mar 31. doi: 10.1093/eurheartj/ehw112), but longer-term data were lacking, and no comparisons with surgery in intermediate-risk patients were available.

For the current study, patients with a mean age of 82 years were evaluated at 51 centers in the United States and Canada during February-September 2014. Subjects had a median Society of Thoracic Surgeons score of 5.2% (range, 4-8) and 73% had New York Heart Association class III/IV heart failure. Almost 90% were treated via the transfemoral route, Dr. Thourani said.

The Sapien 3 device is a balloon expandable valve that differs from prior-generation devices in that it has improved geometry of the trileaflet bovine pericardial valve, a longer cobalt alloy frame with more open outlet cells and denser inlet cells, a polyethylene terephthalate fabric skirt that provides an external circumferential seal to reduce paravalvular leak, four valve sizes, and lower-profile delivery catheters with more precise valve positioning inserted through 14 or 16 French sheaths for increased use of transfemoral access.

Discussant Dr. David E. Kandzari, director of interventional cardiology and chief scientific officer at Piedmont Heart Institute, Atlanta, congratulated Dr. Thourani and his colleagues on “a terrific trial and impactful result.”

“There are, with regard to the Sapien 3 technology, many reasons to believe that this could be an advancement above existing predicate technologies,” he said, specifically mentioning the improvements in the device, compared with prior generations, such as the modification to reduce paravalvular leak, which has been associated with worse outcomes for patients.

“In parallel, there were changes in practice, and one of them implemented in the context of SAPIEN 3 was the use of [computed tomography] imaging to help guide and inform the procedure itself,” he said, adding that the results of the trial “really open the door for at least two very broad pathways.”

First, they expand TAVR to intermediate-risk patients.

“Secondly, they lead the way even further with greater reassurance toward two large ongoing clinical trials in patients considered at low risk, as well,” he said.

 

 

The remarkable outcomes in regard to mortality and stroke are “clinically meaningful and some of the best outcomes we’ve ever witnessed with transcatheter therapy,” he said.

This study was funded by Edwards Lifesciences. Dr. Thourani disclosed that he has received consulting fees and/or research grants from Edwards Lifesciences, St. Jude Medical, Abbott Medical, Boston Scientific, Claret Medical, DirectFlow, Medtronic, and Sorin. Dr. Kandzari has received consultant fees and honoraria from Boston Scientific, The Medicines Company, and Medtronic.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

sworcester@frontlinemedcom.com

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CHICAGO – Transcatheter aortic valve replacement (TAVR) using Sapien 3 – the latest-generation valve – is associated with low mortality, stroke, and paravalvular regurgitation rates at 1 year in intermediate-risk patients, and is superior to surgical valve replacement, according to findings from the SAPIEN 3 study.

The mortality rate at 1 year in the 1,077 patients in the observational study was 7.4% overall and 6.5% in a transfemoral access subgroup, the disabling stroke rate was 2.3%, the aortic valve reintervention rate was 0.6%, and the moderate/severe paravalvular regurgitation rate was 1.5%, Dr. Vinod H. Thourani reported on behalf of the PARTNER trial investigators at the annual meeting of the American College of Cardiology. The findings were published simultaneously in The Lancet (2016 Apr 3. doi: 10.1016/So140-6736[19]30073-3).

Sherry Boschert/IMNG Medical Media
Dr. Vinod Thourani

A prespecified propensity score analysis comparing 963 SAPIEN 3 patients with 747 similar intermediate-risk patients from the PARTNER 2A trial who underwent surgical valve replacement showed that not only was Sapien 3 TAVR noninferior to surgery for the primary composite endpoint of mortality, strokes, and moderate or severe aortic regurgitation, it was also superior to surgery (pooled weighted proportion difference, –9.2% for each). The differences were highly statistically significant.

In fact, Sapien 3 TAVR “blew it out of the water” for both noninferiority and superiority vs. surgery, Dr. Thourani of Emory University, Atlanta said.

The propensity score incorporated 22 characteristics, and the analysis was conducted by blinded investigators. Even using the most conservative strategy for the analysis as approved by the Food and Drug Administration, with the heaviest weighting against TAVR, Sapien 3 TAVR was superior to surgery for the primary composite endpoint, he noted.

Of note, while Sapien 3 TAVR was superior for the individual components of mortality and stroke from the composite endpoint, surgery was superior to Sapien 3 TAVR for the component of moderate or greater aortic regurgitation, he said.

However, the findings represent “strong evidence that in intermediate-risk patients with severe aortic stenosis, SAPIEN 3, compared to surgery, improves clinical outcomes and is the preferred therapy,” he concluded.

In a video interview, he said that if approved by the FDA, “this will become the impetus for [use in] a lower-risk population of patients. Currently we have the inoperative and high-risk patients, and this will open up the intermediate-risk patients for having transcatheter valve therapies, and I think it becomes exceedingly powerful.”

Two ongoing industry-sponsored randomized trials in low-risk patients (those with a Society of Thoracic Surgeons score of less than 4) are underway, he noted.

Sapien 3 TAVR was previously shown to improve 30-day outcomes in intermediate-risk patients with severe aortic stenosis (Eur Heart J. 2016 Mar 31. doi: 10.1093/eurheartj/ehw112), but longer-term data were lacking, and no comparisons with surgery in intermediate-risk patients were available.

For the current study, patients with a mean age of 82 years were evaluated at 51 centers in the United States and Canada during February-September 2014. Subjects had a median Society of Thoracic Surgeons score of 5.2% (range, 4-8) and 73% had New York Heart Association class III/IV heart failure. Almost 90% were treated via the transfemoral route, Dr. Thourani said.

The Sapien 3 device is a balloon expandable valve that differs from prior-generation devices in that it has improved geometry of the trileaflet bovine pericardial valve, a longer cobalt alloy frame with more open outlet cells and denser inlet cells, a polyethylene terephthalate fabric skirt that provides an external circumferential seal to reduce paravalvular leak, four valve sizes, and lower-profile delivery catheters with more precise valve positioning inserted through 14 or 16 French sheaths for increased use of transfemoral access.

Discussant Dr. David E. Kandzari, director of interventional cardiology and chief scientific officer at Piedmont Heart Institute, Atlanta, congratulated Dr. Thourani and his colleagues on “a terrific trial and impactful result.”

“There are, with regard to the Sapien 3 technology, many reasons to believe that this could be an advancement above existing predicate technologies,” he said, specifically mentioning the improvements in the device, compared with prior generations, such as the modification to reduce paravalvular leak, which has been associated with worse outcomes for patients.

“In parallel, there were changes in practice, and one of them implemented in the context of SAPIEN 3 was the use of [computed tomography] imaging to help guide and inform the procedure itself,” he said, adding that the results of the trial “really open the door for at least two very broad pathways.”

First, they expand TAVR to intermediate-risk patients.

“Secondly, they lead the way even further with greater reassurance toward two large ongoing clinical trials in patients considered at low risk, as well,” he said.

 

 

The remarkable outcomes in regard to mortality and stroke are “clinically meaningful and some of the best outcomes we’ve ever witnessed with transcatheter therapy,” he said.

This study was funded by Edwards Lifesciences. Dr. Thourani disclosed that he has received consulting fees and/or research grants from Edwards Lifesciences, St. Jude Medical, Abbott Medical, Boston Scientific, Claret Medical, DirectFlow, Medtronic, and Sorin. Dr. Kandzari has received consultant fees and honoraria from Boston Scientific, The Medicines Company, and Medtronic.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

sworcester@frontlinemedcom.com

CHICAGO – Transcatheter aortic valve replacement (TAVR) using Sapien 3 – the latest-generation valve – is associated with low mortality, stroke, and paravalvular regurgitation rates at 1 year in intermediate-risk patients, and is superior to surgical valve replacement, according to findings from the SAPIEN 3 study.

The mortality rate at 1 year in the 1,077 patients in the observational study was 7.4% overall and 6.5% in a transfemoral access subgroup, the disabling stroke rate was 2.3%, the aortic valve reintervention rate was 0.6%, and the moderate/severe paravalvular regurgitation rate was 1.5%, Dr. Vinod H. Thourani reported on behalf of the PARTNER trial investigators at the annual meeting of the American College of Cardiology. The findings were published simultaneously in The Lancet (2016 Apr 3. doi: 10.1016/So140-6736[19]30073-3).

Sherry Boschert/IMNG Medical Media
Dr. Vinod Thourani

A prespecified propensity score analysis comparing 963 SAPIEN 3 patients with 747 similar intermediate-risk patients from the PARTNER 2A trial who underwent surgical valve replacement showed that not only was Sapien 3 TAVR noninferior to surgery for the primary composite endpoint of mortality, strokes, and moderate or severe aortic regurgitation, it was also superior to surgery (pooled weighted proportion difference, –9.2% for each). The differences were highly statistically significant.

In fact, Sapien 3 TAVR “blew it out of the water” for both noninferiority and superiority vs. surgery, Dr. Thourani of Emory University, Atlanta said.

The propensity score incorporated 22 characteristics, and the analysis was conducted by blinded investigators. Even using the most conservative strategy for the analysis as approved by the Food and Drug Administration, with the heaviest weighting against TAVR, Sapien 3 TAVR was superior to surgery for the primary composite endpoint, he noted.

Of note, while Sapien 3 TAVR was superior for the individual components of mortality and stroke from the composite endpoint, surgery was superior to Sapien 3 TAVR for the component of moderate or greater aortic regurgitation, he said.

However, the findings represent “strong evidence that in intermediate-risk patients with severe aortic stenosis, SAPIEN 3, compared to surgery, improves clinical outcomes and is the preferred therapy,” he concluded.

In a video interview, he said that if approved by the FDA, “this will become the impetus for [use in] a lower-risk population of patients. Currently we have the inoperative and high-risk patients, and this will open up the intermediate-risk patients for having transcatheter valve therapies, and I think it becomes exceedingly powerful.”

Two ongoing industry-sponsored randomized trials in low-risk patients (those with a Society of Thoracic Surgeons score of less than 4) are underway, he noted.

Sapien 3 TAVR was previously shown to improve 30-day outcomes in intermediate-risk patients with severe aortic stenosis (Eur Heart J. 2016 Mar 31. doi: 10.1093/eurheartj/ehw112), but longer-term data were lacking, and no comparisons with surgery in intermediate-risk patients were available.

For the current study, patients with a mean age of 82 years were evaluated at 51 centers in the United States and Canada during February-September 2014. Subjects had a median Society of Thoracic Surgeons score of 5.2% (range, 4-8) and 73% had New York Heart Association class III/IV heart failure. Almost 90% were treated via the transfemoral route, Dr. Thourani said.

The Sapien 3 device is a balloon expandable valve that differs from prior-generation devices in that it has improved geometry of the trileaflet bovine pericardial valve, a longer cobalt alloy frame with more open outlet cells and denser inlet cells, a polyethylene terephthalate fabric skirt that provides an external circumferential seal to reduce paravalvular leak, four valve sizes, and lower-profile delivery catheters with more precise valve positioning inserted through 14 or 16 French sheaths for increased use of transfemoral access.

Discussant Dr. David E. Kandzari, director of interventional cardiology and chief scientific officer at Piedmont Heart Institute, Atlanta, congratulated Dr. Thourani and his colleagues on “a terrific trial and impactful result.”

“There are, with regard to the Sapien 3 technology, many reasons to believe that this could be an advancement above existing predicate technologies,” he said, specifically mentioning the improvements in the device, compared with prior generations, such as the modification to reduce paravalvular leak, which has been associated with worse outcomes for patients.

“In parallel, there were changes in practice, and one of them implemented in the context of SAPIEN 3 was the use of [computed tomography] imaging to help guide and inform the procedure itself,” he said, adding that the results of the trial “really open the door for at least two very broad pathways.”

First, they expand TAVR to intermediate-risk patients.

“Secondly, they lead the way even further with greater reassurance toward two large ongoing clinical trials in patients considered at low risk, as well,” he said.

 

 

The remarkable outcomes in regard to mortality and stroke are “clinically meaningful and some of the best outcomes we’ve ever witnessed with transcatheter therapy,” he said.

This study was funded by Edwards Lifesciences. Dr. Thourani disclosed that he has received consulting fees and/or research grants from Edwards Lifesciences, St. Jude Medical, Abbott Medical, Boston Scientific, Claret Medical, DirectFlow, Medtronic, and Sorin. Dr. Kandzari has received consultant fees and honoraria from Boston Scientific, The Medicines Company, and Medtronic.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel

sworcester@frontlinemedcom.com

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Key clinical point: Transcatheter aortic valve replacement using Sapien 3 is associated with low mortality, stroke, and paravalvular regurgitation rates at 1 year in intermediate-risk patients, and is superior to surgical valve replacement.

Major finding: A propensity score analysis showed that Sapien 3 TAVR was superior to surgical valve replacement (pooled weighted proportion difference, –9.2%).

Data source: An observational study of 1,077 SAPIEN 3 patients, and a propensity score analysis comparing 963 SAPIEN 3 patients and 747 surgical valve replacement patients.

Disclosures: SAPIEN 3 was funded by Edwards Lifesciences. Dr. Thourani disclosed that he has received consulting fees from Edwards Lifesciences and St. Jude Medical, and research grants from Abbott Medical, Boston Scientific, Claret Medical, DirectFlow, Medtronic, and Sorin.

Similarities seen in rate and rhythm control for postsurgical AF

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CHICAGO – Rate and rhythm control proved equally effective for treatment of new-onset post–cardiac surgery atrial fibrillation in a randomized trial that was far and away the largest ever to examine the best way to address this common and costly arrhythmia, Dr. A. Marc Gillinov said at the annual meeting of the American College of Cardiology.

Thus, either strategy is acceptable. That being said, rate control gets the edge as the initial treatment strategy because it avoids the considerable toxicities accompanying amiodarone for rhythm control, most of which arise only after patients have been discharged from the hospital. In contrast, when rate control doesn’t work, it becomes evident while the patient is still in the hospital, according to Dr. Gillinov, a cardiothoracic surgeon at the Cleveland Clinic .

Dr. Marc Gillinov

Atrial fibrillation (AF) is the most common complication of cardiac surgery, with an incidence variously reported at 20%-50%. It results in lengthier hospital stays, greater cost of care, and increased risks of mortality, stroke, heart failure, and infection. Postoperative AF adds an estimated $1 billion per year to health care costs in the United States.

While current ACC/AHA/Heart Rhythm Society joint guidelines recommend rate control with a beta-blocker as first-line therapy for patients with this postoperative complication, with a class I, level-of-evidence A rating, upon closer inspection the evidence cited mainly involves extrapolation from studies looking at how to prevent postoperative AF. Because no persuasive evidence existed as to how best to treat this common and economically and medically costly condition, Dr. Gillinov and his coinvestigators in the National Institutes of Health–funded Cardiothoracic Surgical Trials Network carried out a randomized trial 10-fold larger than anything prior.

The 23-site study included 2,109 patients enrolled prior to cardiac surgery, of whom 40% underwent isolated coronary artery bypass grafting (CABG) while the other 60% had valve surgery, either alone or with CABG. These proportions reflect current cardiac surgery treatment patterns nationally. Overall, 33% of the cardiac surgery patients experienced postoperative AF. The incidence was 28% in patients who underwent isolated CABG but rose with increasing surgical complexity to nearly 50% in patients who had combined CABG and valve operations. The average time to onset of postoperative AF was 2.4 days.

A total of 523 patients with postoperative AF were randomized to rate or rhythm control. Rate control most often entailed use of a beta-blocker, while amiodarone was prescribed for rhythm control.

The primary endpoint in the trial was a measure of health care resource utilization: total days in hospital during a 60-day period starting from the time of randomization. This endpoint was a draw: a median of 5.1 days with rate control and 5.0 days with rhythm control.

At hospital discharge, 89.9% of patients in the rate control group and 93.5% in the rhythm control group had a stable heart rhythm without AF. From discharge to 60 days, 84.2% of patients in the rate control group and a similar 86.9% of the rhythm control group remained free of AF.

Rates of serious adverse events were similar in the two groups: 24.8 per 100 patient-months in the rate control arm and 26.4 per 100 patient-months in the rhythm control arm. Three patients in the rate control arm died during the 60-day study period, and two died in the rhythm control group.

Of note, roughly one-quarter of patients in each study arm crossed over to the other arm. In the rate control group, this was typically due to drug ineffectiveness, while in the rhythm control arm the switch was most often made in response to amiodarone side effects.

Roughly 43% of patients in each group were placed on anticoagulation with warfarin for 60 days according to study protocol, which called for such action if a patient remained in AF 48 hours after randomization.

There were five strokes, one case of transient ischemic attack, and four noncerebral thromboembolisms. Also, 21 bleeding events occurred, 17 of which were classified as serious; 90% of the bleeding events happened in patients on warfarin.

“I found the results very striking and very reassuring,” said discussant Hugh G. Calkins. “To me, the clinical message is clearly that rate control is the preference.”

It was troubling, however, to see that 10 thromboembolic events occurred in 523 patients over the course of just 60 days. “Should we be anticoagulating these postsurgical atrial fibrillation patients a lot more frequently?” asked Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

Dr. Gillinov replied that he and his colleagues in the Cardiothoracic Surgical Trials Network consider that to be the key remaining question regarding postoperative AF. They are now planning a clinical trial aimed at finding the optimal balance between stroke protection via anticoagulation and bleeding risk.

 

 

The National Institutes of Health and the Canadian Institutes of Health Research funded the work. Dr. Gillinov reported serving as a consultant to five surgical device companies, none of which played any role in the study.

Simultaneously with Dr. Gillinov’s presentation at ACC 16, the study results were published in the New England Journal of Medicine (doi: 10.1056/NEJMoa1602002).

bjancin@frontlinemedcom.com

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CHICAGO – Rate and rhythm control proved equally effective for treatment of new-onset post–cardiac surgery atrial fibrillation in a randomized trial that was far and away the largest ever to examine the best way to address this common and costly arrhythmia, Dr. A. Marc Gillinov said at the annual meeting of the American College of Cardiology.

Thus, either strategy is acceptable. That being said, rate control gets the edge as the initial treatment strategy because it avoids the considerable toxicities accompanying amiodarone for rhythm control, most of which arise only after patients have been discharged from the hospital. In contrast, when rate control doesn’t work, it becomes evident while the patient is still in the hospital, according to Dr. Gillinov, a cardiothoracic surgeon at the Cleveland Clinic .

Dr. Marc Gillinov

Atrial fibrillation (AF) is the most common complication of cardiac surgery, with an incidence variously reported at 20%-50%. It results in lengthier hospital stays, greater cost of care, and increased risks of mortality, stroke, heart failure, and infection. Postoperative AF adds an estimated $1 billion per year to health care costs in the United States.

While current ACC/AHA/Heart Rhythm Society joint guidelines recommend rate control with a beta-blocker as first-line therapy for patients with this postoperative complication, with a class I, level-of-evidence A rating, upon closer inspection the evidence cited mainly involves extrapolation from studies looking at how to prevent postoperative AF. Because no persuasive evidence existed as to how best to treat this common and economically and medically costly condition, Dr. Gillinov and his coinvestigators in the National Institutes of Health–funded Cardiothoracic Surgical Trials Network carried out a randomized trial 10-fold larger than anything prior.

The 23-site study included 2,109 patients enrolled prior to cardiac surgery, of whom 40% underwent isolated coronary artery bypass grafting (CABG) while the other 60% had valve surgery, either alone or with CABG. These proportions reflect current cardiac surgery treatment patterns nationally. Overall, 33% of the cardiac surgery patients experienced postoperative AF. The incidence was 28% in patients who underwent isolated CABG but rose with increasing surgical complexity to nearly 50% in patients who had combined CABG and valve operations. The average time to onset of postoperative AF was 2.4 days.

A total of 523 patients with postoperative AF were randomized to rate or rhythm control. Rate control most often entailed use of a beta-blocker, while amiodarone was prescribed for rhythm control.

The primary endpoint in the trial was a measure of health care resource utilization: total days in hospital during a 60-day period starting from the time of randomization. This endpoint was a draw: a median of 5.1 days with rate control and 5.0 days with rhythm control.

At hospital discharge, 89.9% of patients in the rate control group and 93.5% in the rhythm control group had a stable heart rhythm without AF. From discharge to 60 days, 84.2% of patients in the rate control group and a similar 86.9% of the rhythm control group remained free of AF.

Rates of serious adverse events were similar in the two groups: 24.8 per 100 patient-months in the rate control arm and 26.4 per 100 patient-months in the rhythm control arm. Three patients in the rate control arm died during the 60-day study period, and two died in the rhythm control group.

Of note, roughly one-quarter of patients in each study arm crossed over to the other arm. In the rate control group, this was typically due to drug ineffectiveness, while in the rhythm control arm the switch was most often made in response to amiodarone side effects.

Roughly 43% of patients in each group were placed on anticoagulation with warfarin for 60 days according to study protocol, which called for such action if a patient remained in AF 48 hours after randomization.

There were five strokes, one case of transient ischemic attack, and four noncerebral thromboembolisms. Also, 21 bleeding events occurred, 17 of which were classified as serious; 90% of the bleeding events happened in patients on warfarin.

“I found the results very striking and very reassuring,” said discussant Hugh G. Calkins. “To me, the clinical message is clearly that rate control is the preference.”

It was troubling, however, to see that 10 thromboembolic events occurred in 523 patients over the course of just 60 days. “Should we be anticoagulating these postsurgical atrial fibrillation patients a lot more frequently?” asked Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

Dr. Gillinov replied that he and his colleagues in the Cardiothoracic Surgical Trials Network consider that to be the key remaining question regarding postoperative AF. They are now planning a clinical trial aimed at finding the optimal balance between stroke protection via anticoagulation and bleeding risk.

 

 

The National Institutes of Health and the Canadian Institutes of Health Research funded the work. Dr. Gillinov reported serving as a consultant to five surgical device companies, none of which played any role in the study.

Simultaneously with Dr. Gillinov’s presentation at ACC 16, the study results were published in the New England Journal of Medicine (doi: 10.1056/NEJMoa1602002).

bjancin@frontlinemedcom.com

CHICAGO – Rate and rhythm control proved equally effective for treatment of new-onset post–cardiac surgery atrial fibrillation in a randomized trial that was far and away the largest ever to examine the best way to address this common and costly arrhythmia, Dr. A. Marc Gillinov said at the annual meeting of the American College of Cardiology.

Thus, either strategy is acceptable. That being said, rate control gets the edge as the initial treatment strategy because it avoids the considerable toxicities accompanying amiodarone for rhythm control, most of which arise only after patients have been discharged from the hospital. In contrast, when rate control doesn’t work, it becomes evident while the patient is still in the hospital, according to Dr. Gillinov, a cardiothoracic surgeon at the Cleveland Clinic .

Dr. Marc Gillinov

Atrial fibrillation (AF) is the most common complication of cardiac surgery, with an incidence variously reported at 20%-50%. It results in lengthier hospital stays, greater cost of care, and increased risks of mortality, stroke, heart failure, and infection. Postoperative AF adds an estimated $1 billion per year to health care costs in the United States.

While current ACC/AHA/Heart Rhythm Society joint guidelines recommend rate control with a beta-blocker as first-line therapy for patients with this postoperative complication, with a class I, level-of-evidence A rating, upon closer inspection the evidence cited mainly involves extrapolation from studies looking at how to prevent postoperative AF. Because no persuasive evidence existed as to how best to treat this common and economically and medically costly condition, Dr. Gillinov and his coinvestigators in the National Institutes of Health–funded Cardiothoracic Surgical Trials Network carried out a randomized trial 10-fold larger than anything prior.

The 23-site study included 2,109 patients enrolled prior to cardiac surgery, of whom 40% underwent isolated coronary artery bypass grafting (CABG) while the other 60% had valve surgery, either alone or with CABG. These proportions reflect current cardiac surgery treatment patterns nationally. Overall, 33% of the cardiac surgery patients experienced postoperative AF. The incidence was 28% in patients who underwent isolated CABG but rose with increasing surgical complexity to nearly 50% in patients who had combined CABG and valve operations. The average time to onset of postoperative AF was 2.4 days.

A total of 523 patients with postoperative AF were randomized to rate or rhythm control. Rate control most often entailed use of a beta-blocker, while amiodarone was prescribed for rhythm control.

The primary endpoint in the trial was a measure of health care resource utilization: total days in hospital during a 60-day period starting from the time of randomization. This endpoint was a draw: a median of 5.1 days with rate control and 5.0 days with rhythm control.

At hospital discharge, 89.9% of patients in the rate control group and 93.5% in the rhythm control group had a stable heart rhythm without AF. From discharge to 60 days, 84.2% of patients in the rate control group and a similar 86.9% of the rhythm control group remained free of AF.

Rates of serious adverse events were similar in the two groups: 24.8 per 100 patient-months in the rate control arm and 26.4 per 100 patient-months in the rhythm control arm. Three patients in the rate control arm died during the 60-day study period, and two died in the rhythm control group.

Of note, roughly one-quarter of patients in each study arm crossed over to the other arm. In the rate control group, this was typically due to drug ineffectiveness, while in the rhythm control arm the switch was most often made in response to amiodarone side effects.

Roughly 43% of patients in each group were placed on anticoagulation with warfarin for 60 days according to study protocol, which called for such action if a patient remained in AF 48 hours after randomization.

There were five strokes, one case of transient ischemic attack, and four noncerebral thromboembolisms. Also, 21 bleeding events occurred, 17 of which were classified as serious; 90% of the bleeding events happened in patients on warfarin.

“I found the results very striking and very reassuring,” said discussant Hugh G. Calkins. “To me, the clinical message is clearly that rate control is the preference.”

It was troubling, however, to see that 10 thromboembolic events occurred in 523 patients over the course of just 60 days. “Should we be anticoagulating these postsurgical atrial fibrillation patients a lot more frequently?” asked Dr. Calkins, professor of medicine and of pediatrics and director of the cardiac arrhythmia service at Johns Hopkins University, Baltimore.

Dr. Gillinov replied that he and his colleagues in the Cardiothoracic Surgical Trials Network consider that to be the key remaining question regarding postoperative AF. They are now planning a clinical trial aimed at finding the optimal balance between stroke protection via anticoagulation and bleeding risk.

 

 

The National Institutes of Health and the Canadian Institutes of Health Research funded the work. Dr. Gillinov reported serving as a consultant to five surgical device companies, none of which played any role in the study.

Simultaneously with Dr. Gillinov’s presentation at ACC 16, the study results were published in the New England Journal of Medicine (doi: 10.1056/NEJMoa1602002).

bjancin@frontlinemedcom.com

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Key clinical point: Rate control offers the advantage of simplicity over a rhythm control strategy in new-onset atrial fibrillation after cardiac surgery.

Major finding: Rate and rhythm control strategies for treatment of new-onset atrial fibrillation after cardiac surgery resulted in equal numbers of hospital days, similar serious complication rates, and low rates of persistent atrial fibrillation at 60 days of follow-up.

Data source: A randomized clinical trial of 523 patients with new-onset atrial fibrillation following cardiac surgery at 23 U.S. and Canadian academic medical centers.

Disclosures: The study was funded by the National Institutes of Health and the Canadian Institutes of Health Research and carried out through the Cardiothoracic Surgical Trials Network. The presenter reported having no relevant financial interests.

VIDEO: Fire and Ice - Which catheter ablation approach is best in AF?

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CHICAGO – The largest-ever randomized trial of catheter ablation for atrial fibrillation ended in a draw, but there may be a clear winner for some patients.

Safety and 1-year efficacy of radiofrequency ablation and cryoballoon ablation were roughly 65% in both treatment arms of the 769-patient Fire and Ice trial.

However, in an interview at the annual meeting of the American College of Cardiology, principal investigator Dr. Karl-Heinz Kuck of Asklepios Klinik St. Georg, Hamburg, Germany, explains why the results are actually a victory for cryoablation.

 

 

 

 

bjancin@frontlinemedcom.com

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CHICAGO – The largest-ever randomized trial of catheter ablation for atrial fibrillation ended in a draw, but there may be a clear winner for some patients.

Safety and 1-year efficacy of radiofrequency ablation and cryoballoon ablation were roughly 65% in both treatment arms of the 769-patient Fire and Ice trial.

However, in an interview at the annual meeting of the American College of Cardiology, principal investigator Dr. Karl-Heinz Kuck of Asklepios Klinik St. Georg, Hamburg, Germany, explains why the results are actually a victory for cryoablation.

 

 

 

 

bjancin@frontlinemedcom.com

CHICAGO – The largest-ever randomized trial of catheter ablation for atrial fibrillation ended in a draw, but there may be a clear winner for some patients.

Safety and 1-year efficacy of radiofrequency ablation and cryoballoon ablation were roughly 65% in both treatment arms of the 769-patient Fire and Ice trial.

However, in an interview at the annual meeting of the American College of Cardiology, principal investigator Dr. Karl-Heinz Kuck of Asklepios Klinik St. Georg, Hamburg, Germany, explains why the results are actually a victory for cryoablation.

 

 

 

 

bjancin@frontlinemedcom.com

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Coronary bypass shows compelling advantages in ischemic cardiomyopathy

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CHICAGO – Coronary artery bypass grafting plus guideline-directed medical therapy resulted in significantly lower all-cause mortality than did optimal medical therapy alone at 10 years of follow-up in the Surgical Treatment for Ischemic Heart Failure Extension Study (STICHES), Dr. Eric J. Velazquez reported at the annual meeting of the American College of Cardiology.

“We believe these results have the immediate clinical implications that the presence of severe left ventricular dysfunction should prompt an evaluation for the extent and severity of angiographic CAD, and that among patients with ischemic cardiomyopathy, CABG should be strongly considered in order to improve long-term survival,” declared Dr. Velazquez, professor of medicine in the division of cardiology at Duke University, Durham, N.C.

Bruce Jancin/Frontline Medical News
Dr. Eric J. Velazquez

STICHES included 1,212 patients in 22 countries, all with heart failure and an ejection fraction of 35% or less along with CAD deemed suitable for surgical revascularization. They were randomized to CABG plus guideline-directed medical therapy or to the medical therapy alone. The 98% successful follow-up rate over the course of 10 years in this trial drew audience praise as a herculean effort.

At a median 9.8 years of follow-up, all-cause mortality – the primary study endpoint – had occurred in 58.9% of the CABG group and 66.1% of medically managed patients. That translates to a 16% relative risk reduction and an absolute 8% difference in favor of CABG. The median survival extension conferred by CABG was 1.4 years. The number of patients needed to treat with CABG in order to prevent one death from any cause was 14.

The CABG group also did significantly better in terms of secondary endpoints. The cardiovascular mortality rate was 40.5% in the CABG group versus 49.3% with medical therapy, for a 21% relative risk reduction favoring CABG and a number needed to treat of 11. The composite endpoint of all-cause mortality or cardiovascular hospitalization occurred in 76.6% of the CABG group and 87% of the medically treated patients.

In an earlier analysis based upon 56 months of follow-up, there was a trend favoring CABG in terms of all-cause mortality, but it didn’t reach statistical significance (N Engl J Med. 2011;364:1607-16). With an additional 5 years of prospective follow-up, however, the divergence in outcome between the two study arms increased sufficiently that the difference achieved statistical significance. But the more impressive study finding, in Dr. Velazquez’s view, was the durability of the CABG benefits out to 10 years.

Discussant Dr. Jeroean J. Bax of Leiden (the Netherlands) University commented that while the solid advantage in outcomes displayed by the CABG group was noteworthy, he finds it sobering that even though the STICHES participants averaged only 60 years of age at entry, the majority were dead at 10 years’ follow-up. What, he asked, is the likely mechanism for the very high mortality seen in this population?

“My take-home after many years working with our team is that I believe these patients have very low reserve, and they are at risk any time they take a hit. I don’t believe just one mechanism is involved. In our previous analysis of the 5-year follow-up data, we showed the results can’t be explained solely by viability, ischemia, or functional recovery. I think the issue of arrhythmia reduction and substrate reduction is important. But for me, it’s a combination of many factors. Any additional hit for this high-risk population is not well tolerated; that’s what leads to death,” Dr. Velazquez replied.

Asked how he thinks multivessel percutaneous coronary intervention would perform as an alternative to CABG in patients with ischemic cardiomyopathy, Dr. Velazquez responded that he has no idea because it hasn’t been studied.

“I can picture reasons for and against PCI providing benefits similar to CABG,” he added.

Simultaneous with Dr. Velazquez’s presentation at ACC 16, the STICHES results were published online (N Engl J Med. 2016 April 3. doi:10.1056/NEJMoa1602001).

In an accompanying editorial, Dr. Robert A. Guyton and Dr. Andrew L. Smith of Emory University in Atlanta asserted that these strong results from STICHES make a compelling case that CABG for patients with ischemic cardiomyopathy should be upgraded in the ACC/AHA heart failure management guidelines from its current status as a class IIb recommendation that “might be considered” to class IIa, indicating it is “probably beneficial” (N Engl J Med. 2016 April 3. doi:10.1056/NEJMe1603615).

STICHES was funded by the National Institutes of Health. The study presenter reported having no financial conflicts regarding the study.

bjancin@frontlinemedcom.com

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CHICAGO – Coronary artery bypass grafting plus guideline-directed medical therapy resulted in significantly lower all-cause mortality than did optimal medical therapy alone at 10 years of follow-up in the Surgical Treatment for Ischemic Heart Failure Extension Study (STICHES), Dr. Eric J. Velazquez reported at the annual meeting of the American College of Cardiology.

“We believe these results have the immediate clinical implications that the presence of severe left ventricular dysfunction should prompt an evaluation for the extent and severity of angiographic CAD, and that among patients with ischemic cardiomyopathy, CABG should be strongly considered in order to improve long-term survival,” declared Dr. Velazquez, professor of medicine in the division of cardiology at Duke University, Durham, N.C.

Bruce Jancin/Frontline Medical News
Dr. Eric J. Velazquez

STICHES included 1,212 patients in 22 countries, all with heart failure and an ejection fraction of 35% or less along with CAD deemed suitable for surgical revascularization. They were randomized to CABG plus guideline-directed medical therapy or to the medical therapy alone. The 98% successful follow-up rate over the course of 10 years in this trial drew audience praise as a herculean effort.

At a median 9.8 years of follow-up, all-cause mortality – the primary study endpoint – had occurred in 58.9% of the CABG group and 66.1% of medically managed patients. That translates to a 16% relative risk reduction and an absolute 8% difference in favor of CABG. The median survival extension conferred by CABG was 1.4 years. The number of patients needed to treat with CABG in order to prevent one death from any cause was 14.

The CABG group also did significantly better in terms of secondary endpoints. The cardiovascular mortality rate was 40.5% in the CABG group versus 49.3% with medical therapy, for a 21% relative risk reduction favoring CABG and a number needed to treat of 11. The composite endpoint of all-cause mortality or cardiovascular hospitalization occurred in 76.6% of the CABG group and 87% of the medically treated patients.

In an earlier analysis based upon 56 months of follow-up, there was a trend favoring CABG in terms of all-cause mortality, but it didn’t reach statistical significance (N Engl J Med. 2011;364:1607-16). With an additional 5 years of prospective follow-up, however, the divergence in outcome between the two study arms increased sufficiently that the difference achieved statistical significance. But the more impressive study finding, in Dr. Velazquez’s view, was the durability of the CABG benefits out to 10 years.

Discussant Dr. Jeroean J. Bax of Leiden (the Netherlands) University commented that while the solid advantage in outcomes displayed by the CABG group was noteworthy, he finds it sobering that even though the STICHES participants averaged only 60 years of age at entry, the majority were dead at 10 years’ follow-up. What, he asked, is the likely mechanism for the very high mortality seen in this population?

“My take-home after many years working with our team is that I believe these patients have very low reserve, and they are at risk any time they take a hit. I don’t believe just one mechanism is involved. In our previous analysis of the 5-year follow-up data, we showed the results can’t be explained solely by viability, ischemia, or functional recovery. I think the issue of arrhythmia reduction and substrate reduction is important. But for me, it’s a combination of many factors. Any additional hit for this high-risk population is not well tolerated; that’s what leads to death,” Dr. Velazquez replied.

Asked how he thinks multivessel percutaneous coronary intervention would perform as an alternative to CABG in patients with ischemic cardiomyopathy, Dr. Velazquez responded that he has no idea because it hasn’t been studied.

“I can picture reasons for and against PCI providing benefits similar to CABG,” he added.

Simultaneous with Dr. Velazquez’s presentation at ACC 16, the STICHES results were published online (N Engl J Med. 2016 April 3. doi:10.1056/NEJMoa1602001).

In an accompanying editorial, Dr. Robert A. Guyton and Dr. Andrew L. Smith of Emory University in Atlanta asserted that these strong results from STICHES make a compelling case that CABG for patients with ischemic cardiomyopathy should be upgraded in the ACC/AHA heart failure management guidelines from its current status as a class IIb recommendation that “might be considered” to class IIa, indicating it is “probably beneficial” (N Engl J Med. 2016 April 3. doi:10.1056/NEJMe1603615).

STICHES was funded by the National Institutes of Health. The study presenter reported having no financial conflicts regarding the study.

bjancin@frontlinemedcom.com

CHICAGO – Coronary artery bypass grafting plus guideline-directed medical therapy resulted in significantly lower all-cause mortality than did optimal medical therapy alone at 10 years of follow-up in the Surgical Treatment for Ischemic Heart Failure Extension Study (STICHES), Dr. Eric J. Velazquez reported at the annual meeting of the American College of Cardiology.

“We believe these results have the immediate clinical implications that the presence of severe left ventricular dysfunction should prompt an evaluation for the extent and severity of angiographic CAD, and that among patients with ischemic cardiomyopathy, CABG should be strongly considered in order to improve long-term survival,” declared Dr. Velazquez, professor of medicine in the division of cardiology at Duke University, Durham, N.C.

Bruce Jancin/Frontline Medical News
Dr. Eric J. Velazquez

STICHES included 1,212 patients in 22 countries, all with heart failure and an ejection fraction of 35% or less along with CAD deemed suitable for surgical revascularization. They were randomized to CABG plus guideline-directed medical therapy or to the medical therapy alone. The 98% successful follow-up rate over the course of 10 years in this trial drew audience praise as a herculean effort.

At a median 9.8 years of follow-up, all-cause mortality – the primary study endpoint – had occurred in 58.9% of the CABG group and 66.1% of medically managed patients. That translates to a 16% relative risk reduction and an absolute 8% difference in favor of CABG. The median survival extension conferred by CABG was 1.4 years. The number of patients needed to treat with CABG in order to prevent one death from any cause was 14.

The CABG group also did significantly better in terms of secondary endpoints. The cardiovascular mortality rate was 40.5% in the CABG group versus 49.3% with medical therapy, for a 21% relative risk reduction favoring CABG and a number needed to treat of 11. The composite endpoint of all-cause mortality or cardiovascular hospitalization occurred in 76.6% of the CABG group and 87% of the medically treated patients.

In an earlier analysis based upon 56 months of follow-up, there was a trend favoring CABG in terms of all-cause mortality, but it didn’t reach statistical significance (N Engl J Med. 2011;364:1607-16). With an additional 5 years of prospective follow-up, however, the divergence in outcome between the two study arms increased sufficiently that the difference achieved statistical significance. But the more impressive study finding, in Dr. Velazquez’s view, was the durability of the CABG benefits out to 10 years.

Discussant Dr. Jeroean J. Bax of Leiden (the Netherlands) University commented that while the solid advantage in outcomes displayed by the CABG group was noteworthy, he finds it sobering that even though the STICHES participants averaged only 60 years of age at entry, the majority were dead at 10 years’ follow-up. What, he asked, is the likely mechanism for the very high mortality seen in this population?

“My take-home after many years working with our team is that I believe these patients have very low reserve, and they are at risk any time they take a hit. I don’t believe just one mechanism is involved. In our previous analysis of the 5-year follow-up data, we showed the results can’t be explained solely by viability, ischemia, or functional recovery. I think the issue of arrhythmia reduction and substrate reduction is important. But for me, it’s a combination of many factors. Any additional hit for this high-risk population is not well tolerated; that’s what leads to death,” Dr. Velazquez replied.

Asked how he thinks multivessel percutaneous coronary intervention would perform as an alternative to CABG in patients with ischemic cardiomyopathy, Dr. Velazquez responded that he has no idea because it hasn’t been studied.

“I can picture reasons for and against PCI providing benefits similar to CABG,” he added.

Simultaneous with Dr. Velazquez’s presentation at ACC 16, the STICHES results were published online (N Engl J Med. 2016 April 3. doi:10.1056/NEJMoa1602001).

In an accompanying editorial, Dr. Robert A. Guyton and Dr. Andrew L. Smith of Emory University in Atlanta asserted that these strong results from STICHES make a compelling case that CABG for patients with ischemic cardiomyopathy should be upgraded in the ACC/AHA heart failure management guidelines from its current status as a class IIb recommendation that “might be considered” to class IIa, indicating it is “probably beneficial” (N Engl J Med. 2016 April 3. doi:10.1056/NEJMe1603615).

STICHES was funded by the National Institutes of Health. The study presenter reported having no financial conflicts regarding the study.

bjancin@frontlinemedcom.com

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Key clinical point: CABG plus optimal medical therapy is the treatment of choice in patients with ischemic cardiomyopathy.

Major finding: The number of patients with ischemic cardiomyopathy who need to be treated with CABG plus optimal medical therapy instead of medical therapy alone in order to prevent one additional death due to any cause is 14.

Data source: This was a randomized, unblinded clinical trial involving 1,212 patients with ischemic cardiomyopathy in 22 countries.

Disclosures: STICHES was funded by the National Institutes of Health. The study presenter reported having no financial conflicts regarding the study.

High-dose vitamin D improves heart structure, function in chronic heart failure

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High-dose oral vitamin D supplements taken for 1 year significantly improved cardiac structure and function in patients with chronic heart failure secondary to left ventricular systolic dysfunction, according to results from a new study.

However, the same study. led by Dr. Klaus Witte of the University of Leeds (England), found that 6-minute walk distance – the study’s primary outcome measure – was not improved after a year’s supplementation with vitamin D.

©Joss/Fotolia.com

It is unclear why vitamin D deficiency co-occurs in a majority of people with chronic heart failure (CHF) due to left ventricular systolic dysfunction (LVSD) or to what degree reversing it can improve outcomes. However, vitamin D deficiency is thought to interfere with calcium transport in cardiac cells, and may contribute to cardiac fibrosis and inflammation, leading to faster progression to heart failure following damage to cardiac muscle.

The new VINDICATE study randomized 223 patients with CHF due to LVSD and vitamin D deficiency to 1 year’s treatment with 4,000 IU of 25(OH) vitamin D3 daily, or placebo, Dr. Witte and associates concluded at the annual meeting of the American College of Cardiology. The results were published online April 4 in JACC (doi: 10.1016/j.jacc.2016.03.508).

Of these patients, 163 completed follow-up at 12 months, and 6-minute walk distance (MWT) and echocardiography findings were recorded at baseline and follow-up.

Dr. Witte and colleagues found significant evidence of improved function in the vitamin D–treated patients as measured by left ventricular ejection fraction +6.07% (95% confidence interval 3.20, 8.95; P less than .0001); and a reversal of left ventricular remodeling (left ventricular end diastolic diameter –2.49 mm (95% CI –4.09, –0.90; P equal to .002) and left ventricular end systolic diameter –2.09 mm (95% CI –4.11; –0.06; P equal to .043).

The researchers also drew blood at 3-month intervals to check for serum calcium concentration, renal function, and vitamin D levels. Treatment was well tolerated, and no patients suffered hypervitaminosis or required a dose adjustment.

“There was no effect of vitamin D supplementation on the primary endpoint of 6 MWT distance but there were statistically significant, and prognostically and clinically relevant improvements in the secondary outcomes of left ventricular ejection fraction, dimensions, and volumes, suggesting that vitamin D is leading to beneficial reverse remodeling,” the investigators wrote in their analysis.

The study’s failure to meet its primary endpoint despite significant results from its secondary endpoints led Dr. Witte and colleagues to say that its design led to underpowering.

“Variability in the walk distance measure at baseline was much greater than predicted from our pilot study such that our sample size only had 7% post hoc power to detect a difference between the groups,” meaning it was underpowered to detect a clinically relevant change in walk distance. The findings “have implications for future studies using 6-minute walk distance as an outcome measure,” they wrote.

The investigators championed the addition of vitamin D3 to CHF treatment regimens.

As new therapies for CHF are “often expensive, increasingly technical, and frequently fail to meet the rigorous demands of large phase III clinical trials,” Dr. Witte and colleagues wrote, vitamin D “might be a cheap and safe additional option for CHF patients and may have beneficial effects on multiple features of the syndrome.”

The U.K.’s National Institute for Health Research supported the study, and none of its authors declared conflicts of interest.

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High-dose oral vitamin D supplements taken for 1 year significantly improved cardiac structure and function in patients with chronic heart failure secondary to left ventricular systolic dysfunction, according to results from a new study.

However, the same study. led by Dr. Klaus Witte of the University of Leeds (England), found that 6-minute walk distance – the study’s primary outcome measure – was not improved after a year’s supplementation with vitamin D.

©Joss/Fotolia.com

It is unclear why vitamin D deficiency co-occurs in a majority of people with chronic heart failure (CHF) due to left ventricular systolic dysfunction (LVSD) or to what degree reversing it can improve outcomes. However, vitamin D deficiency is thought to interfere with calcium transport in cardiac cells, and may contribute to cardiac fibrosis and inflammation, leading to faster progression to heart failure following damage to cardiac muscle.

The new VINDICATE study randomized 223 patients with CHF due to LVSD and vitamin D deficiency to 1 year’s treatment with 4,000 IU of 25(OH) vitamin D3 daily, or placebo, Dr. Witte and associates concluded at the annual meeting of the American College of Cardiology. The results were published online April 4 in JACC (doi: 10.1016/j.jacc.2016.03.508).

Of these patients, 163 completed follow-up at 12 months, and 6-minute walk distance (MWT) and echocardiography findings were recorded at baseline and follow-up.

Dr. Witte and colleagues found significant evidence of improved function in the vitamin D–treated patients as measured by left ventricular ejection fraction +6.07% (95% confidence interval 3.20, 8.95; P less than .0001); and a reversal of left ventricular remodeling (left ventricular end diastolic diameter –2.49 mm (95% CI –4.09, –0.90; P equal to .002) and left ventricular end systolic diameter –2.09 mm (95% CI –4.11; –0.06; P equal to .043).

The researchers also drew blood at 3-month intervals to check for serum calcium concentration, renal function, and vitamin D levels. Treatment was well tolerated, and no patients suffered hypervitaminosis or required a dose adjustment.

“There was no effect of vitamin D supplementation on the primary endpoint of 6 MWT distance but there were statistically significant, and prognostically and clinically relevant improvements in the secondary outcomes of left ventricular ejection fraction, dimensions, and volumes, suggesting that vitamin D is leading to beneficial reverse remodeling,” the investigators wrote in their analysis.

The study’s failure to meet its primary endpoint despite significant results from its secondary endpoints led Dr. Witte and colleagues to say that its design led to underpowering.

“Variability in the walk distance measure at baseline was much greater than predicted from our pilot study such that our sample size only had 7% post hoc power to detect a difference between the groups,” meaning it was underpowered to detect a clinically relevant change in walk distance. The findings “have implications for future studies using 6-minute walk distance as an outcome measure,” they wrote.

The investigators championed the addition of vitamin D3 to CHF treatment regimens.

As new therapies for CHF are “often expensive, increasingly technical, and frequently fail to meet the rigorous demands of large phase III clinical trials,” Dr. Witte and colleagues wrote, vitamin D “might be a cheap and safe additional option for CHF patients and may have beneficial effects on multiple features of the syndrome.”

The U.K.’s National Institute for Health Research supported the study, and none of its authors declared conflicts of interest.

High-dose oral vitamin D supplements taken for 1 year significantly improved cardiac structure and function in patients with chronic heart failure secondary to left ventricular systolic dysfunction, according to results from a new study.

However, the same study. led by Dr. Klaus Witte of the University of Leeds (England), found that 6-minute walk distance – the study’s primary outcome measure – was not improved after a year’s supplementation with vitamin D.

©Joss/Fotolia.com

It is unclear why vitamin D deficiency co-occurs in a majority of people with chronic heart failure (CHF) due to left ventricular systolic dysfunction (LVSD) or to what degree reversing it can improve outcomes. However, vitamin D deficiency is thought to interfere with calcium transport in cardiac cells, and may contribute to cardiac fibrosis and inflammation, leading to faster progression to heart failure following damage to cardiac muscle.

The new VINDICATE study randomized 223 patients with CHF due to LVSD and vitamin D deficiency to 1 year’s treatment with 4,000 IU of 25(OH) vitamin D3 daily, or placebo, Dr. Witte and associates concluded at the annual meeting of the American College of Cardiology. The results were published online April 4 in JACC (doi: 10.1016/j.jacc.2016.03.508).

Of these patients, 163 completed follow-up at 12 months, and 6-minute walk distance (MWT) and echocardiography findings were recorded at baseline and follow-up.

Dr. Witte and colleagues found significant evidence of improved function in the vitamin D–treated patients as measured by left ventricular ejection fraction +6.07% (95% confidence interval 3.20, 8.95; P less than .0001); and a reversal of left ventricular remodeling (left ventricular end diastolic diameter –2.49 mm (95% CI –4.09, –0.90; P equal to .002) and left ventricular end systolic diameter –2.09 mm (95% CI –4.11; –0.06; P equal to .043).

The researchers also drew blood at 3-month intervals to check for serum calcium concentration, renal function, and vitamin D levels. Treatment was well tolerated, and no patients suffered hypervitaminosis or required a dose adjustment.

“There was no effect of vitamin D supplementation on the primary endpoint of 6 MWT distance but there were statistically significant, and prognostically and clinically relevant improvements in the secondary outcomes of left ventricular ejection fraction, dimensions, and volumes, suggesting that vitamin D is leading to beneficial reverse remodeling,” the investigators wrote in their analysis.

The study’s failure to meet its primary endpoint despite significant results from its secondary endpoints led Dr. Witte and colleagues to say that its design led to underpowering.

“Variability in the walk distance measure at baseline was much greater than predicted from our pilot study such that our sample size only had 7% post hoc power to detect a difference between the groups,” meaning it was underpowered to detect a clinically relevant change in walk distance. The findings “have implications for future studies using 6-minute walk distance as an outcome measure,” they wrote.

The investigators championed the addition of vitamin D3 to CHF treatment regimens.

As new therapies for CHF are “often expensive, increasingly technical, and frequently fail to meet the rigorous demands of large phase III clinical trials,” Dr. Witte and colleagues wrote, vitamin D “might be a cheap and safe additional option for CHF patients and may have beneficial effects on multiple features of the syndrome.”

The U.K.’s National Institute for Health Research supported the study, and none of its authors declared conflicts of interest.

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High-dose vitamin D improves heart structure, function in chronic heart failure
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Key clinical point: Oral supplementation of high-dose vitamin D3 led to significantly improved left ventricular function and structure in a cohort of vitamin-deficient patients.

Major finding: Treated patients had significantly improved left ventricular ejection fraction of +6.07% vs. nontreated patients at 1 year, and significant reversal of left ventricular remodeling (left ventricular end diastolic diameter –2.49 mm and left ventricular end systolic diameter –2.09 mm).

Data source: A single-site randomized trial in which 229 patients with LV CHF received high-dose vitamin D or placebo for 12 months.

Disclosures: The U.K.’s National Institute for Health Research supported the study, and none of its authors declared conflicts of interest.

PCSK9 inhibitor overcomes muscle-related statin intolerance

Findings clarify muscle-related statin intolerance
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PCSK9 inhibitor overcomes muscle-related statin intolerance

CHICAGO – Statin-associated muscle symptoms are real for roughly 40% of patients with a history of this adverse effect, and for such patients who are truly unable to tolerate a statin treatment, a PCSK9 inhibitor provided an effective and well-tolerated alternative in a randomized trial with more than 500 patients.

“Controversy has surrounded the issue of statin-associated muscle symptoms because of large differences in the incidence of this disorder in randomized trials and observational studies. The GAUSS-3 study results demonstrate that muscle-related intolerance is reproducible during blinded statin rechallenge in a substantial fraction, about 40%, of patients with a history of symptoms,” Dr. Steven E. Nissen said at the annual meeting of the American College of Cardiology. “Alternative approaches to reducing low-density lipoprotein cholesterol in these patients represents an important medical priority.”

Mitchel L. Zoler/Frontline Medical News
Dr. Steven E. Nissen

Statin intolerance has been a challenging diagnosis for physicians to confirm because no biomarker exists to definitively document it, which led to this study to test a more systematic and objective approach to confirm the diagnosis, explained Dr. Nissen, chairman of the department of cardiology at the Cleveland Clinic. GAUSS-3 (Goal Achievement After Utilizing an Anti-PCSK9 Antibody in Statin Intolerant Subjects 3), run at 53 centers worldwide, included two distinct phases.

In the first phase, researchers enrolled 511 patients with elevated LDL cholesterol levels who had a history of an inability to tolerate treatment with atorvastatin plus at least one other statin or at least three statins of any type. Following a 4-week washout period with no lipid-lowering treatments, they randomized patients to 10 weeks of 20 mg atorvastatin daily or placebo, followed by crossover to the alternative treatment for an additional 10 weeks. The patients averaged 61 years old, with an average LDL cholesterol level of 212 mg/dL.

During this phase, 43% of the patients reported having intolerable muscle symptoms while on atorvastatin, but not on placebo. In addition, 27% reported intolerable muscle symptoms while on placebo but not on atorvastatin, demonstrating the high incidence of psychosomatic muscle symptoms experienced by many patients with this history, Dr. Nissen noted. This placebo-controlled statin rechallenge provides a model for how clinicians can reliably confirm which patients experience statin-specific muscle symptoms.

“This gives physicians a strategy for managing these patients. This was the best strategy we could use to find out who really has intolerance,” Dr. Nissen said.

The second phase included 218 patients who had their muscle symptoms confirmed in the first phase plus a small number of patients with a history of muscle-related statin intolerance who skipped the first phase because their serum creatinine kinase level was greater than 10-times above the upper limit of normal. The researchers randomized these patients to treatment with either a monthly subcutaneous injection with 420 mg of evolocumab (Repatha) or 10 mg of oral ezetimibe (Zetia) given daily. To maintain blinding, all patients received simultaneous placebo treatment that mimicked the drug they were not assigned to receive. The patients enrolled in the second phase had an average entry LDL cholesterol level of about 220 mg/dL.

After 24 weeks on treatment, patients on ezetimibe had an average 17% reduction in their LDL cholesterol level, while those on evolocumab had an average reduction of 53%. An LDL cholesterol level of less than 100 mg/dL was achieved in 2% of the ezetimibe patients and in 64% of those on evolocumab. Muscle-related symptoms occurred in 29% of the ezetimibe patients and in 21% of those on evolocumab, but discontinuations because of muscle symptoms were limited to 1 patient on evolocumab and 5 patients on ezetimibe, Dr. Nissen reported. Concurrent with his report at the meeting, an article with the results appeared online (JAMA. 2016 Apr 3. doi: 10.1001/jama.2016.3608).

Dr. Frederick A. Masoudi

“These findings show that it pays to be patient” when dealing with patients who report statin-associated muscle symptoms as more than half of them were able to tolerate the daily 20 mg atorvastatin challenge for 10 weeks, commented Dr. Frederick A. Masoudi, a cardiologist and professor of medicine at the University of Colorado at Denver, Aurora. The report also “gives us a better approach for dealing with patients who have this nonspecific reaction to statin treatment, which remains the mainstay of cholesterol-lowering treatment.”

Dr. Nissen stressed that in his opinion, it is appropriate to use a PCSK9 inhibitor in this off-label way despite the controversial high cost for these drugs. “We have to do something for these patients who say that they cannot take a statin, but have multiple coronary disease risk factors and LDL cholesterol levels above 200 mg/dL. They are an accident waiting to happen. I am unwilling to leave patients with an LDL cholesterol of 200 mg/dL who can’t take statins and just walk away.”

 

 

GAUSS-3 was sponsored by Amgen, which markets evolocumab. Dr. Nissen has received research grants from Amgen and several other drug companies. Dr. Masoudi had no disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

References

Body

Dr. Nissen and his associates did a great job in this study of bringing much more clarity to the issue of muscle-related statin intolerance. Results from observational studies have suggested that this occurs in roughly 10%-20% of patients who start treatment on a statin. The rate has often been much lower in randomized statin trials because statin-intolerant patients are often identified and excluded from participation during a run-in phase before the randomized phase begins.

The first phase of GAUSS-3 showed that significant and treatment-limiting myalgia in response to statin treatment is real, and affects about 40% of patients who have a history of reporting muscle pain while taking statins. This part of the study provides clinicians with an important message about how to determine whether a patient really has muscle-related statin intolerance, and also showed that controlled rechallenge with a statin can identify many patients who can tolerate a statin despite a history of intolerance.

Dr. Roger Blumenthal

The second phase of GAUSS-3 showed that most patients with a history of muscle-related statin intolerance could nicely tolerate treatment with an effective regimen of either ezetimibe or the PCSK9 inhibitor evolocumab. Evolocumab was especially effective, reducing patient levels of LDL cholesterol by more than 50%.

Currently, the Food and Drug Administration–approved indications for treatment with PCSK9 inhibitors are limited to patients with familial hypercholesterolemia or with poorly-controlled LDL cholesterol levels and clinical atherosclerotic cardiovascular disease. That’s because we still await reports of longer-term follow-up of studies designed to confirm the clinical benefits of lowering LDL cholesterol using a PCSK9 inhibitor. Results from these studies should be available within the next year.

Dr. Roger Blumenthal is professor of medicine and director of the Ciccarone Center for the Prevention of Heart Disease at Johns Hopkins University in Baltimore. He had no disclosures. He made these comments in an interview.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
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Dr. Nissen and his associates did a great job in this study of bringing much more clarity to the issue of muscle-related statin intolerance. Results from observational studies have suggested that this occurs in roughly 10%-20% of patients who start treatment on a statin. The rate has often been much lower in randomized statin trials because statin-intolerant patients are often identified and excluded from participation during a run-in phase before the randomized phase begins.

The first phase of GAUSS-3 showed that significant and treatment-limiting myalgia in response to statin treatment is real, and affects about 40% of patients who have a history of reporting muscle pain while taking statins. This part of the study provides clinicians with an important message about how to determine whether a patient really has muscle-related statin intolerance, and also showed that controlled rechallenge with a statin can identify many patients who can tolerate a statin despite a history of intolerance.

Dr. Roger Blumenthal

The second phase of GAUSS-3 showed that most patients with a history of muscle-related statin intolerance could nicely tolerate treatment with an effective regimen of either ezetimibe or the PCSK9 inhibitor evolocumab. Evolocumab was especially effective, reducing patient levels of LDL cholesterol by more than 50%.

Currently, the Food and Drug Administration–approved indications for treatment with PCSK9 inhibitors are limited to patients with familial hypercholesterolemia or with poorly-controlled LDL cholesterol levels and clinical atherosclerotic cardiovascular disease. That’s because we still await reports of longer-term follow-up of studies designed to confirm the clinical benefits of lowering LDL cholesterol using a PCSK9 inhibitor. Results from these studies should be available within the next year.

Dr. Roger Blumenthal is professor of medicine and director of the Ciccarone Center for the Prevention of Heart Disease at Johns Hopkins University in Baltimore. He had no disclosures. He made these comments in an interview.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
Body

Dr. Nissen and his associates did a great job in this study of bringing much more clarity to the issue of muscle-related statin intolerance. Results from observational studies have suggested that this occurs in roughly 10%-20% of patients who start treatment on a statin. The rate has often been much lower in randomized statin trials because statin-intolerant patients are often identified and excluded from participation during a run-in phase before the randomized phase begins.

The first phase of GAUSS-3 showed that significant and treatment-limiting myalgia in response to statin treatment is real, and affects about 40% of patients who have a history of reporting muscle pain while taking statins. This part of the study provides clinicians with an important message about how to determine whether a patient really has muscle-related statin intolerance, and also showed that controlled rechallenge with a statin can identify many patients who can tolerate a statin despite a history of intolerance.

Dr. Roger Blumenthal

The second phase of GAUSS-3 showed that most patients with a history of muscle-related statin intolerance could nicely tolerate treatment with an effective regimen of either ezetimibe or the PCSK9 inhibitor evolocumab. Evolocumab was especially effective, reducing patient levels of LDL cholesterol by more than 50%.

Currently, the Food and Drug Administration–approved indications for treatment with PCSK9 inhibitors are limited to patients with familial hypercholesterolemia or with poorly-controlled LDL cholesterol levels and clinical atherosclerotic cardiovascular disease. That’s because we still await reports of longer-term follow-up of studies designed to confirm the clinical benefits of lowering LDL cholesterol using a PCSK9 inhibitor. Results from these studies should be available within the next year.

Dr. Roger Blumenthal is professor of medicine and director of the Ciccarone Center for the Prevention of Heart Disease at Johns Hopkins University in Baltimore. He had no disclosures. He made these comments in an interview.

The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
Title
Findings clarify muscle-related statin intolerance
Findings clarify muscle-related statin intolerance

CHICAGO – Statin-associated muscle symptoms are real for roughly 40% of patients with a history of this adverse effect, and for such patients who are truly unable to tolerate a statin treatment, a PCSK9 inhibitor provided an effective and well-tolerated alternative in a randomized trial with more than 500 patients.

“Controversy has surrounded the issue of statin-associated muscle symptoms because of large differences in the incidence of this disorder in randomized trials and observational studies. The GAUSS-3 study results demonstrate that muscle-related intolerance is reproducible during blinded statin rechallenge in a substantial fraction, about 40%, of patients with a history of symptoms,” Dr. Steven E. Nissen said at the annual meeting of the American College of Cardiology. “Alternative approaches to reducing low-density lipoprotein cholesterol in these patients represents an important medical priority.”

Mitchel L. Zoler/Frontline Medical News
Dr. Steven E. Nissen

Statin intolerance has been a challenging diagnosis for physicians to confirm because no biomarker exists to definitively document it, which led to this study to test a more systematic and objective approach to confirm the diagnosis, explained Dr. Nissen, chairman of the department of cardiology at the Cleveland Clinic. GAUSS-3 (Goal Achievement After Utilizing an Anti-PCSK9 Antibody in Statin Intolerant Subjects 3), run at 53 centers worldwide, included two distinct phases.

In the first phase, researchers enrolled 511 patients with elevated LDL cholesterol levels who had a history of an inability to tolerate treatment with atorvastatin plus at least one other statin or at least three statins of any type. Following a 4-week washout period with no lipid-lowering treatments, they randomized patients to 10 weeks of 20 mg atorvastatin daily or placebo, followed by crossover to the alternative treatment for an additional 10 weeks. The patients averaged 61 years old, with an average LDL cholesterol level of 212 mg/dL.

During this phase, 43% of the patients reported having intolerable muscle symptoms while on atorvastatin, but not on placebo. In addition, 27% reported intolerable muscle symptoms while on placebo but not on atorvastatin, demonstrating the high incidence of psychosomatic muscle symptoms experienced by many patients with this history, Dr. Nissen noted. This placebo-controlled statin rechallenge provides a model for how clinicians can reliably confirm which patients experience statin-specific muscle symptoms.

“This gives physicians a strategy for managing these patients. This was the best strategy we could use to find out who really has intolerance,” Dr. Nissen said.

The second phase included 218 patients who had their muscle symptoms confirmed in the first phase plus a small number of patients with a history of muscle-related statin intolerance who skipped the first phase because their serum creatinine kinase level was greater than 10-times above the upper limit of normal. The researchers randomized these patients to treatment with either a monthly subcutaneous injection with 420 mg of evolocumab (Repatha) or 10 mg of oral ezetimibe (Zetia) given daily. To maintain blinding, all patients received simultaneous placebo treatment that mimicked the drug they were not assigned to receive. The patients enrolled in the second phase had an average entry LDL cholesterol level of about 220 mg/dL.

After 24 weeks on treatment, patients on ezetimibe had an average 17% reduction in their LDL cholesterol level, while those on evolocumab had an average reduction of 53%. An LDL cholesterol level of less than 100 mg/dL was achieved in 2% of the ezetimibe patients and in 64% of those on evolocumab. Muscle-related symptoms occurred in 29% of the ezetimibe patients and in 21% of those on evolocumab, but discontinuations because of muscle symptoms were limited to 1 patient on evolocumab and 5 patients on ezetimibe, Dr. Nissen reported. Concurrent with his report at the meeting, an article with the results appeared online (JAMA. 2016 Apr 3. doi: 10.1001/jama.2016.3608).

Dr. Frederick A. Masoudi

“These findings show that it pays to be patient” when dealing with patients who report statin-associated muscle symptoms as more than half of them were able to tolerate the daily 20 mg atorvastatin challenge for 10 weeks, commented Dr. Frederick A. Masoudi, a cardiologist and professor of medicine at the University of Colorado at Denver, Aurora. The report also “gives us a better approach for dealing with patients who have this nonspecific reaction to statin treatment, which remains the mainstay of cholesterol-lowering treatment.”

Dr. Nissen stressed that in his opinion, it is appropriate to use a PCSK9 inhibitor in this off-label way despite the controversial high cost for these drugs. “We have to do something for these patients who say that they cannot take a statin, but have multiple coronary disease risk factors and LDL cholesterol levels above 200 mg/dL. They are an accident waiting to happen. I am unwilling to leave patients with an LDL cholesterol of 200 mg/dL who can’t take statins and just walk away.”

 

 

GAUSS-3 was sponsored by Amgen, which markets evolocumab. Dr. Nissen has received research grants from Amgen and several other drug companies. Dr. Masoudi had no disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

CHICAGO – Statin-associated muscle symptoms are real for roughly 40% of patients with a history of this adverse effect, and for such patients who are truly unable to tolerate a statin treatment, a PCSK9 inhibitor provided an effective and well-tolerated alternative in a randomized trial with more than 500 patients.

“Controversy has surrounded the issue of statin-associated muscle symptoms because of large differences in the incidence of this disorder in randomized trials and observational studies. The GAUSS-3 study results demonstrate that muscle-related intolerance is reproducible during blinded statin rechallenge in a substantial fraction, about 40%, of patients with a history of symptoms,” Dr. Steven E. Nissen said at the annual meeting of the American College of Cardiology. “Alternative approaches to reducing low-density lipoprotein cholesterol in these patients represents an important medical priority.”

Mitchel L. Zoler/Frontline Medical News
Dr. Steven E. Nissen

Statin intolerance has been a challenging diagnosis for physicians to confirm because no biomarker exists to definitively document it, which led to this study to test a more systematic and objective approach to confirm the diagnosis, explained Dr. Nissen, chairman of the department of cardiology at the Cleveland Clinic. GAUSS-3 (Goal Achievement After Utilizing an Anti-PCSK9 Antibody in Statin Intolerant Subjects 3), run at 53 centers worldwide, included two distinct phases.

In the first phase, researchers enrolled 511 patients with elevated LDL cholesterol levels who had a history of an inability to tolerate treatment with atorvastatin plus at least one other statin or at least three statins of any type. Following a 4-week washout period with no lipid-lowering treatments, they randomized patients to 10 weeks of 20 mg atorvastatin daily or placebo, followed by crossover to the alternative treatment for an additional 10 weeks. The patients averaged 61 years old, with an average LDL cholesterol level of 212 mg/dL.

During this phase, 43% of the patients reported having intolerable muscle symptoms while on atorvastatin, but not on placebo. In addition, 27% reported intolerable muscle symptoms while on placebo but not on atorvastatin, demonstrating the high incidence of psychosomatic muscle symptoms experienced by many patients with this history, Dr. Nissen noted. This placebo-controlled statin rechallenge provides a model for how clinicians can reliably confirm which patients experience statin-specific muscle symptoms.

“This gives physicians a strategy for managing these patients. This was the best strategy we could use to find out who really has intolerance,” Dr. Nissen said.

The second phase included 218 patients who had their muscle symptoms confirmed in the first phase plus a small number of patients with a history of muscle-related statin intolerance who skipped the first phase because their serum creatinine kinase level was greater than 10-times above the upper limit of normal. The researchers randomized these patients to treatment with either a monthly subcutaneous injection with 420 mg of evolocumab (Repatha) or 10 mg of oral ezetimibe (Zetia) given daily. To maintain blinding, all patients received simultaneous placebo treatment that mimicked the drug they were not assigned to receive. The patients enrolled in the second phase had an average entry LDL cholesterol level of about 220 mg/dL.

After 24 weeks on treatment, patients on ezetimibe had an average 17% reduction in their LDL cholesterol level, while those on evolocumab had an average reduction of 53%. An LDL cholesterol level of less than 100 mg/dL was achieved in 2% of the ezetimibe patients and in 64% of those on evolocumab. Muscle-related symptoms occurred in 29% of the ezetimibe patients and in 21% of those on evolocumab, but discontinuations because of muscle symptoms were limited to 1 patient on evolocumab and 5 patients on ezetimibe, Dr. Nissen reported. Concurrent with his report at the meeting, an article with the results appeared online (JAMA. 2016 Apr 3. doi: 10.1001/jama.2016.3608).

Dr. Frederick A. Masoudi

“These findings show that it pays to be patient” when dealing with patients who report statin-associated muscle symptoms as more than half of them were able to tolerate the daily 20 mg atorvastatin challenge for 10 weeks, commented Dr. Frederick A. Masoudi, a cardiologist and professor of medicine at the University of Colorado at Denver, Aurora. The report also “gives us a better approach for dealing with patients who have this nonspecific reaction to statin treatment, which remains the mainstay of cholesterol-lowering treatment.”

Dr. Nissen stressed that in his opinion, it is appropriate to use a PCSK9 inhibitor in this off-label way despite the controversial high cost for these drugs. “We have to do something for these patients who say that they cannot take a statin, but have multiple coronary disease risk factors and LDL cholesterol levels above 200 mg/dL. They are an accident waiting to happen. I am unwilling to leave patients with an LDL cholesterol of 200 mg/dL who can’t take statins and just walk away.”

 

 

GAUSS-3 was sponsored by Amgen, which markets evolocumab. Dr. Nissen has received research grants from Amgen and several other drug companies. Dr. Masoudi had no disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PCSK9 inhibitor overcomes muscle-related statin intolerance
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Key clinical point: Muscle-related statin intolerance was reproducible in many patients, but most could tolerate and respond robustly to a PCSK9 inhibitor.

Major finding: In patients with a history of muscle-related statin intolerance, 43% were intolerant of blinded atorvastatin challenge, but not blinded placebo.

Data source: GAUSS-3, a multicenter, two-phase randomized controlled trial with 511 patients.

Disclosures: GAUSS-3 was sponsored by Amgen, which markets evolocumab. Dr. Nissen has received research grants from Amgen and several other drug companies. Dr. Masoudi had no disclosures.