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VIDEO: Did the PROMISE trial keep its promise?
SAN DIEGO – Patients with new-onset, stable chest pain account for millions of stress tests annually in the United States, but randomized data are limited on which test is best and the impact of testing on clinical outcomes.
Results from the prospective PROMISE trial, presented at the annual meeting of the American College of Cardiology, show there is no Holy Grail testing strategy. First-line testing with CT angiography did not reduce hard clinical events compared with functional testing, but did cut the number of patients undergoing an invasive catheterization showing no obstructive coronary artery disease.
Listen here for our interview with ACC president Dr. Patrick O’Gara on how these results will impact patient care and potentially influence current guideline recommendations.
Dr. O’Gara reported no relevant financial conflicts.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
SAN DIEGO – Patients with new-onset, stable chest pain account for millions of stress tests annually in the United States, but randomized data are limited on which test is best and the impact of testing on clinical outcomes.
Results from the prospective PROMISE trial, presented at the annual meeting of the American College of Cardiology, show there is no Holy Grail testing strategy. First-line testing with CT angiography did not reduce hard clinical events compared with functional testing, but did cut the number of patients undergoing an invasive catheterization showing no obstructive coronary artery disease.
Listen here for our interview with ACC president Dr. Patrick O’Gara on how these results will impact patient care and potentially influence current guideline recommendations.
Dr. O’Gara reported no relevant financial conflicts.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
SAN DIEGO – Patients with new-onset, stable chest pain account for millions of stress tests annually in the United States, but randomized data are limited on which test is best and the impact of testing on clinical outcomes.
Results from the prospective PROMISE trial, presented at the annual meeting of the American College of Cardiology, show there is no Holy Grail testing strategy. First-line testing with CT angiography did not reduce hard clinical events compared with functional testing, but did cut the number of patients undergoing an invasive catheterization showing no obstructive coronary artery disease.
Listen here for our interview with ACC president Dr. Patrick O’Gara on how these results will impact patient care and potentially influence current guideline recommendations.
Dr. O’Gara reported no relevant financial conflicts.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
AT ACC 15
PCI linked to higher rate of cardiovascular events than CABG
SAN DIEGO– Percutaneous coronary intervention with everolimus-eluting stents is associated with significantly higher major adverse cardiovascular events than is coronary artery bypass grafting in patients with multivessel coronary artery disease, according to results of the BEST trial.
In the randomized noninferiority trial of 880 patients, there was a 47% higher rate of the primary endpoint of death, myocardial infarction, or target vessel revascularization among patients randomized to percutaneous coronary intervention (PCI) with the new-generation drug-eluting stent than among those randomized to coronary artery bypass grafting (CABG), after a median of 4.6 years follow-up.
However, the differences in primary endpoint were not significant for noninferiority between the two groups at the 2-year follow-up mark, Dr. Seung-Jung Park said at the annual meeting of the American College of Cardiology.
The Xience everolimus-eluting stent used in BEST (Randomized Comparison of Coronary Artery Bypass Surgery and Everolimus-Eluting Stent Implantation in the Treatment of Patients with Multivessel Coronary Artery Disease) is one of several bioabsorbable vascular scaffolds that have caught on in recent years. The working hypothesis behind the device is that by dissolving during a period of 12-24 months, the scaffold provides temporary bracing against restenosis but then disappears, allowing improved endovascular healing.
Patients were randomized after diagnostic coronary angiography to PCI (438 patients) or to CABG (442).
The study, which was terminated early because of slow enrollment, also found a significantly greater rate of the composite secondary endpoint of death, myocardial infarction, stroke, or repeat revascularization in the PCI group compared to the CABG group (19.9% vs. 13.3%, P = .01).
There were no significant differences between the two groups in the rate of the other secondary safety endpoint: a composite of death, MI, and stroke.
In total, 29 patients assigned to PCI died, compared with 22 assigned to CABG (6.6% vs. 5%, P = .30).
The rate of spontaneous myocardial infarction was significantly higher in the PCI group (4.3% vs. 1.6%, P = .02), as was the rate of repeat revascularization (11% vs. 5.4%, P = .003).
There were fewer incidences of major bleeding in the PCI group compared to the CABG group, although the rate of fatal major bleeding was similar for both arms of the study.
Diabetes status had a major negative impact on outcome for patients undergoing PCI, increasing the rate of the primary endpoint to 19.2%, compared to 9.1% in patients undergoing CABG (P = .007).
“In the BEST trial, PCI with everolimus-eluting stents was not shown to be noninferior to CABG with respect to the primary endpoint of death, myocardial infarction, or target vessel revascularization at 2 years,” wrote Dr. Park of the University of Ulsan College of Medicine, and his coauthors. The article was published online simultaneously with his presentation (N. Engl. J. Med. 2015 March 15 [doi:10.1056/NEJMoa1415447]).
“At longer-term follow-up (median 4.6 years), PCI was associated with a significant increase in the incidence of the primary endpoint, as compared to the incidence with CABG.”
The authors suggested this difference was largely attributable to the higher rate of repeat target-vessel revascularization in patients who had undergone PCI, as well as the spontaneous myocardial infarction and new lesion revascularization.
In contrast to previous studies, the researchers did not find a significant difference in the rate of stroke between the two groups.
“The reason for this discrepancy is not clear, but the use of off-pump CABG can avoid excessive manipulation of the aorta, and may have contributed to a reduced rate of stroke in the CABG group in our study,” the authors noted.
The researchers acknowledged that the trial was not powered to detect differences in individual endpoints and that they did experience enrollment difficulties.
The CardioVascular Research Foundation, Abbott Vascular, and the Korea Healthcare Technology Research and Development Project supported the study. Dr. Park disclosed ties with Abbott, Cordis, Boston Scientific, and Medtronic, and has an ownership interest in the Cardiovascular Research Foundation.
SAN DIEGO– Percutaneous coronary intervention with everolimus-eluting stents is associated with significantly higher major adverse cardiovascular events than is coronary artery bypass grafting in patients with multivessel coronary artery disease, according to results of the BEST trial.
In the randomized noninferiority trial of 880 patients, there was a 47% higher rate of the primary endpoint of death, myocardial infarction, or target vessel revascularization among patients randomized to percutaneous coronary intervention (PCI) with the new-generation drug-eluting stent than among those randomized to coronary artery bypass grafting (CABG), after a median of 4.6 years follow-up.
However, the differences in primary endpoint were not significant for noninferiority between the two groups at the 2-year follow-up mark, Dr. Seung-Jung Park said at the annual meeting of the American College of Cardiology.
The Xience everolimus-eluting stent used in BEST (Randomized Comparison of Coronary Artery Bypass Surgery and Everolimus-Eluting Stent Implantation in the Treatment of Patients with Multivessel Coronary Artery Disease) is one of several bioabsorbable vascular scaffolds that have caught on in recent years. The working hypothesis behind the device is that by dissolving during a period of 12-24 months, the scaffold provides temporary bracing against restenosis but then disappears, allowing improved endovascular healing.
Patients were randomized after diagnostic coronary angiography to PCI (438 patients) or to CABG (442).
The study, which was terminated early because of slow enrollment, also found a significantly greater rate of the composite secondary endpoint of death, myocardial infarction, stroke, or repeat revascularization in the PCI group compared to the CABG group (19.9% vs. 13.3%, P = .01).
There were no significant differences between the two groups in the rate of the other secondary safety endpoint: a composite of death, MI, and stroke.
In total, 29 patients assigned to PCI died, compared with 22 assigned to CABG (6.6% vs. 5%, P = .30).
The rate of spontaneous myocardial infarction was significantly higher in the PCI group (4.3% vs. 1.6%, P = .02), as was the rate of repeat revascularization (11% vs. 5.4%, P = .003).
There were fewer incidences of major bleeding in the PCI group compared to the CABG group, although the rate of fatal major bleeding was similar for both arms of the study.
Diabetes status had a major negative impact on outcome for patients undergoing PCI, increasing the rate of the primary endpoint to 19.2%, compared to 9.1% in patients undergoing CABG (P = .007).
“In the BEST trial, PCI with everolimus-eluting stents was not shown to be noninferior to CABG with respect to the primary endpoint of death, myocardial infarction, or target vessel revascularization at 2 years,” wrote Dr. Park of the University of Ulsan College of Medicine, and his coauthors. The article was published online simultaneously with his presentation (N. Engl. J. Med. 2015 March 15 [doi:10.1056/NEJMoa1415447]).
“At longer-term follow-up (median 4.6 years), PCI was associated with a significant increase in the incidence of the primary endpoint, as compared to the incidence with CABG.”
The authors suggested this difference was largely attributable to the higher rate of repeat target-vessel revascularization in patients who had undergone PCI, as well as the spontaneous myocardial infarction and new lesion revascularization.
In contrast to previous studies, the researchers did not find a significant difference in the rate of stroke between the two groups.
“The reason for this discrepancy is not clear, but the use of off-pump CABG can avoid excessive manipulation of the aorta, and may have contributed to a reduced rate of stroke in the CABG group in our study,” the authors noted.
The researchers acknowledged that the trial was not powered to detect differences in individual endpoints and that they did experience enrollment difficulties.
The CardioVascular Research Foundation, Abbott Vascular, and the Korea Healthcare Technology Research and Development Project supported the study. Dr. Park disclosed ties with Abbott, Cordis, Boston Scientific, and Medtronic, and has an ownership interest in the Cardiovascular Research Foundation.
SAN DIEGO– Percutaneous coronary intervention with everolimus-eluting stents is associated with significantly higher major adverse cardiovascular events than is coronary artery bypass grafting in patients with multivessel coronary artery disease, according to results of the BEST trial.
In the randomized noninferiority trial of 880 patients, there was a 47% higher rate of the primary endpoint of death, myocardial infarction, or target vessel revascularization among patients randomized to percutaneous coronary intervention (PCI) with the new-generation drug-eluting stent than among those randomized to coronary artery bypass grafting (CABG), after a median of 4.6 years follow-up.
However, the differences in primary endpoint were not significant for noninferiority between the two groups at the 2-year follow-up mark, Dr. Seung-Jung Park said at the annual meeting of the American College of Cardiology.
The Xience everolimus-eluting stent used in BEST (Randomized Comparison of Coronary Artery Bypass Surgery and Everolimus-Eluting Stent Implantation in the Treatment of Patients with Multivessel Coronary Artery Disease) is one of several bioabsorbable vascular scaffolds that have caught on in recent years. The working hypothesis behind the device is that by dissolving during a period of 12-24 months, the scaffold provides temporary bracing against restenosis but then disappears, allowing improved endovascular healing.
Patients were randomized after diagnostic coronary angiography to PCI (438 patients) or to CABG (442).
The study, which was terminated early because of slow enrollment, also found a significantly greater rate of the composite secondary endpoint of death, myocardial infarction, stroke, or repeat revascularization in the PCI group compared to the CABG group (19.9% vs. 13.3%, P = .01).
There were no significant differences between the two groups in the rate of the other secondary safety endpoint: a composite of death, MI, and stroke.
In total, 29 patients assigned to PCI died, compared with 22 assigned to CABG (6.6% vs. 5%, P = .30).
The rate of spontaneous myocardial infarction was significantly higher in the PCI group (4.3% vs. 1.6%, P = .02), as was the rate of repeat revascularization (11% vs. 5.4%, P = .003).
There were fewer incidences of major bleeding in the PCI group compared to the CABG group, although the rate of fatal major bleeding was similar for both arms of the study.
Diabetes status had a major negative impact on outcome for patients undergoing PCI, increasing the rate of the primary endpoint to 19.2%, compared to 9.1% in patients undergoing CABG (P = .007).
“In the BEST trial, PCI with everolimus-eluting stents was not shown to be noninferior to CABG with respect to the primary endpoint of death, myocardial infarction, or target vessel revascularization at 2 years,” wrote Dr. Park of the University of Ulsan College of Medicine, and his coauthors. The article was published online simultaneously with his presentation (N. Engl. J. Med. 2015 March 15 [doi:10.1056/NEJMoa1415447]).
“At longer-term follow-up (median 4.6 years), PCI was associated with a significant increase in the incidence of the primary endpoint, as compared to the incidence with CABG.”
The authors suggested this difference was largely attributable to the higher rate of repeat target-vessel revascularization in patients who had undergone PCI, as well as the spontaneous myocardial infarction and new lesion revascularization.
In contrast to previous studies, the researchers did not find a significant difference in the rate of stroke between the two groups.
“The reason for this discrepancy is not clear, but the use of off-pump CABG can avoid excessive manipulation of the aorta, and may have contributed to a reduced rate of stroke in the CABG group in our study,” the authors noted.
The researchers acknowledged that the trial was not powered to detect differences in individual endpoints and that they did experience enrollment difficulties.
The CardioVascular Research Foundation, Abbott Vascular, and the Korea Healthcare Technology Research and Development Project supported the study. Dr. Park disclosed ties with Abbott, Cordis, Boston Scientific, and Medtronic, and has an ownership interest in the Cardiovascular Research Foundation.
AT ACC 15
Key clinical point: PCI with everolimus-eluting stents is associated with significantly higher major adverse cardiovascular events than is CABG in patients with multivessel coronary artery disease.
Major finding: Patients undergoing PCI had a 47% higher rate of the primary endpoint of death, myocardial infarction, or target vessel revascularization among patients compared to those undergoing CABG.
Data source: BEST, a randomized noninferiority trial of 880 patients.
Disclosures: The CardioVascular Research Foundation, Abbott Vascular, and the Korea Healthcare Technology Research and Development Project supported the study. Dr. Park disclosed ties with Abbott, Cordis, Boston Scientific, and Medtronic, and has an ownership interest in the Cardiovascular Research Foundation.
Cardiovascular event rates similar in PCI and CABG after 5 years
Percutaneous coronary intervention with a sirolimus-eluting stent showed comparable rates of death, myocardial infarction and stroke to coronary artery bypass grafting in patients with coronary artery stenosis after 5 years in a randomized trial.
The PRECOMBAT (Premier of Randomized Comparison of Bypass Surgery versus Angioplasty Using Sirolimus-Eluting Stent in Patients with Left Main Coronary Artery Disease) study randomized trial in 600 patients with unprotected left main coronary artery stenosis – 300 of whom were randomized to PCI and the rest to CABG – showed no significant difference in major adverse cardiac or cerebrovascular events (hazard ratio, 1.27; 95% confidence interval, 0.84-1.90; P = 0.26), according to a presentation at the American College of Cardiology meeting in San Diego.
However, the study did observe a twofold increase in the rate of ischemia-driven target vessel revascularization among patients treated with PCI, compared to those who underwent CABG (HR, 2.11; 95% CI, 1.16-3.84; P = 0.012), although the authors pointed out that this did not appear to impact the study’s harder endpoints.
“Given a higher rate of repeat revascularization even after the use of second-generation drug-eluting stents for unprotected left main coronary artery stenosis, frequent repeat revascularization could be an inherent weakness of stent-related treatments,” wrote Dr. Jung-Min Ahn, from the Asan Medical Center, Seoul, and coauthors (J. Am. Coll. Cardiol. 2015; March 15 [doi:10.1016/j.jacc.2015.03.033]).
The study was supported by the CardioVascular Research Foundation, Cordis, Johnson and Johnson, and the Korean Ministry of Health & Welfare. No conflicts of interest were disclosed.
Percutaneous coronary intervention with a sirolimus-eluting stent showed comparable rates of death, myocardial infarction and stroke to coronary artery bypass grafting in patients with coronary artery stenosis after 5 years in a randomized trial.
The PRECOMBAT (Premier of Randomized Comparison of Bypass Surgery versus Angioplasty Using Sirolimus-Eluting Stent in Patients with Left Main Coronary Artery Disease) study randomized trial in 600 patients with unprotected left main coronary artery stenosis – 300 of whom were randomized to PCI and the rest to CABG – showed no significant difference in major adverse cardiac or cerebrovascular events (hazard ratio, 1.27; 95% confidence interval, 0.84-1.90; P = 0.26), according to a presentation at the American College of Cardiology meeting in San Diego.
However, the study did observe a twofold increase in the rate of ischemia-driven target vessel revascularization among patients treated with PCI, compared to those who underwent CABG (HR, 2.11; 95% CI, 1.16-3.84; P = 0.012), although the authors pointed out that this did not appear to impact the study’s harder endpoints.
“Given a higher rate of repeat revascularization even after the use of second-generation drug-eluting stents for unprotected left main coronary artery stenosis, frequent repeat revascularization could be an inherent weakness of stent-related treatments,” wrote Dr. Jung-Min Ahn, from the Asan Medical Center, Seoul, and coauthors (J. Am. Coll. Cardiol. 2015; March 15 [doi:10.1016/j.jacc.2015.03.033]).
The study was supported by the CardioVascular Research Foundation, Cordis, Johnson and Johnson, and the Korean Ministry of Health & Welfare. No conflicts of interest were disclosed.
Percutaneous coronary intervention with a sirolimus-eluting stent showed comparable rates of death, myocardial infarction and stroke to coronary artery bypass grafting in patients with coronary artery stenosis after 5 years in a randomized trial.
The PRECOMBAT (Premier of Randomized Comparison of Bypass Surgery versus Angioplasty Using Sirolimus-Eluting Stent in Patients with Left Main Coronary Artery Disease) study randomized trial in 600 patients with unprotected left main coronary artery stenosis – 300 of whom were randomized to PCI and the rest to CABG – showed no significant difference in major adverse cardiac or cerebrovascular events (hazard ratio, 1.27; 95% confidence interval, 0.84-1.90; P = 0.26), according to a presentation at the American College of Cardiology meeting in San Diego.
However, the study did observe a twofold increase in the rate of ischemia-driven target vessel revascularization among patients treated with PCI, compared to those who underwent CABG (HR, 2.11; 95% CI, 1.16-3.84; P = 0.012), although the authors pointed out that this did not appear to impact the study’s harder endpoints.
“Given a higher rate of repeat revascularization even after the use of second-generation drug-eluting stents for unprotected left main coronary artery stenosis, frequent repeat revascularization could be an inherent weakness of stent-related treatments,” wrote Dr. Jung-Min Ahn, from the Asan Medical Center, Seoul, and coauthors (J. Am. Coll. Cardiol. 2015; March 15 [doi:10.1016/j.jacc.2015.03.033]).
The study was supported by the CardioVascular Research Foundation, Cordis, Johnson and Johnson, and the Korean Ministry of Health & Welfare. No conflicts of interest were disclosed.
FROM ACC 2015
Key clinical point: Percutaneous coronary intervention with sirolimus-eluting stents shows comparable rates of death, myocardial infarction and stroke to coronary artery bypass grafting after 5 years.
Major finding: There were no significant differences in major adverse cardiac or cerebrovascular events between PCI and CABG in patients with unprotected left main coronary artery stenosis.
Data source: PRECOMBAT, A randomized trial in 600 patients with unprotected left main coronary artery stenosis.
Disclosures: The study was supported by the CardioVascular Research Foundation, Cordis, Johnson&Johnson, and the Korean Ministry of Health & Welfare. No conflicts of interest were disclosed.
SCOT-HEART: CT angiography scores big in stable chest pain
SAN DIEGO – The addition of CT angiography to standard care changed the diagnosis and treatment of one in four patients with stable chest pain in the prospective, randomized SCOT-HEART trial.
CT angiography (CTA) also reduced coronary heart disease deaths or myocardial infarctions by 38% after a median follow-up of 1.7 years, although the finding was of borderline significance (hazard ratio, 0.62; P = .053).
A post-hoc, landmark analysis, however, that accounted for the roughly 6-week delay between the clinic visit and implementation or alteration of therapy based on CTA findings, showed a halving of these outcomes (HR, 0.50; P = .015), chief investigator Dr. David Newby reported at the annual meeting of the American College of Cardiology.
SCOT-HEART (Scottish COmputed Tomography of the Heart trial) involved 4,146 patients referred from chest pain clinics across Scotland for assessment of suspected angina due to coronary artery disease, of whom 47% were diagnosed in the clinic with coronary heart disease and 36% with angina due to coronary heart disease. Patients were then evenly randomized to standard care involving cardiovascular risk assessment with the ASSIGN Score alone or with CTA.
When attending clinicians reviewed the cases at 6 weeks, the diagnosis of coronary heart disease (CHD) changed in 25% of patients assigned CTA vs. only 1% assigned standard care alone and the diagnosis of angina due to CHD changed in 23% vs. 1% (P value < .001 for both), Dr. Newby, from the University of Edinburgh, said.
Clinicians reported that CTA significantly increased the certainty (Relative risk, 2.56; P < .0001) and frequency (RR, 1.09; P = .017) of the diagnosis of CHD and increased the certainty of a diagnosis of angina due to CHD (RR, 1.79; P < .0001), but had no effect on its frequency (RR, 0.93; P = .12).
Overall, 63% of patients had evidence of CHD on CTA, with 25% having obstructive disease.
CTA altered subsequent testing in 15% of patients vs. only 1% with standard care (P < .001). CTA use was associated with the cancellation of 121 functional stress tests and 29 invasive coronary angiography exams. CTA also prompted 94 new angiograms vs. just 8 with standard care, but this was mainly the result of the exclusion or discovery of obstructive coronary heart disease, including triple vessel disease, Dr. Newby observed. CT was associated with a nonsignificant increase in coronary revascularizations (11.2% vs. 9.7%; HR, 1.19; P .06).
The changes in diagnosis and testing were associated with changes in subsequent treatment in 23% of CTA patients vs. 5% of standard care patients overall (P < .001), including recommendations and cancellations for preventive and anti-anginal therapies. The results were also simultaneously published online (Lancet 2015 [doi:10.19016/S0140-6736(15)060291-4]).
The most impressive aspect of SCOT-HEART was the strong trend for improved outcomes in patients for which therapeutic alterations were made, Dr. Eric Peterson, with the Duke University in Durham, N.C., commented.
“This sets the standard for how we perform and evaluate whether CT can improve outcomes for patients,” he said.
In an editorial accompanying the report,, Dr. Pamela Douglas, from the Duke Clinical Research Institute in Durham, N.C., called the finding of reduced death and MI “intriguing,” but urged caution in its interpretation because it was one of 22 secondary end points and the absolute difference between groups was only 16 events (Lancet 2015; [doi: 10.1016/S0140-6736(15)60463-9]). Earlier in the meeting, she reported that the PROMISE trial found no difference in its primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications among chest pain patients evaluated with CTA or functional testing.
Finally, it was noted that radiation exposure in SCOT-HEART (median 4.1 mSv) was substantially lower than that reported in PROMISE, a finding Dr. Newby said he could not explain.
SAN DIEGO – The addition of CT angiography to standard care changed the diagnosis and treatment of one in four patients with stable chest pain in the prospective, randomized SCOT-HEART trial.
CT angiography (CTA) also reduced coronary heart disease deaths or myocardial infarctions by 38% after a median follow-up of 1.7 years, although the finding was of borderline significance (hazard ratio, 0.62; P = .053).
A post-hoc, landmark analysis, however, that accounted for the roughly 6-week delay between the clinic visit and implementation or alteration of therapy based on CTA findings, showed a halving of these outcomes (HR, 0.50; P = .015), chief investigator Dr. David Newby reported at the annual meeting of the American College of Cardiology.
SCOT-HEART (Scottish COmputed Tomography of the Heart trial) involved 4,146 patients referred from chest pain clinics across Scotland for assessment of suspected angina due to coronary artery disease, of whom 47% were diagnosed in the clinic with coronary heart disease and 36% with angina due to coronary heart disease. Patients were then evenly randomized to standard care involving cardiovascular risk assessment with the ASSIGN Score alone or with CTA.
When attending clinicians reviewed the cases at 6 weeks, the diagnosis of coronary heart disease (CHD) changed in 25% of patients assigned CTA vs. only 1% assigned standard care alone and the diagnosis of angina due to CHD changed in 23% vs. 1% (P value < .001 for both), Dr. Newby, from the University of Edinburgh, said.
Clinicians reported that CTA significantly increased the certainty (Relative risk, 2.56; P < .0001) and frequency (RR, 1.09; P = .017) of the diagnosis of CHD and increased the certainty of a diagnosis of angina due to CHD (RR, 1.79; P < .0001), but had no effect on its frequency (RR, 0.93; P = .12).
Overall, 63% of patients had evidence of CHD on CTA, with 25% having obstructive disease.
CTA altered subsequent testing in 15% of patients vs. only 1% with standard care (P < .001). CTA use was associated with the cancellation of 121 functional stress tests and 29 invasive coronary angiography exams. CTA also prompted 94 new angiograms vs. just 8 with standard care, but this was mainly the result of the exclusion or discovery of obstructive coronary heart disease, including triple vessel disease, Dr. Newby observed. CT was associated with a nonsignificant increase in coronary revascularizations (11.2% vs. 9.7%; HR, 1.19; P .06).
The changes in diagnosis and testing were associated with changes in subsequent treatment in 23% of CTA patients vs. 5% of standard care patients overall (P < .001), including recommendations and cancellations for preventive and anti-anginal therapies. The results were also simultaneously published online (Lancet 2015 [doi:10.19016/S0140-6736(15)060291-4]).
The most impressive aspect of SCOT-HEART was the strong trend for improved outcomes in patients for which therapeutic alterations were made, Dr. Eric Peterson, with the Duke University in Durham, N.C., commented.
“This sets the standard for how we perform and evaluate whether CT can improve outcomes for patients,” he said.
In an editorial accompanying the report,, Dr. Pamela Douglas, from the Duke Clinical Research Institute in Durham, N.C., called the finding of reduced death and MI “intriguing,” but urged caution in its interpretation because it was one of 22 secondary end points and the absolute difference between groups was only 16 events (Lancet 2015; [doi: 10.1016/S0140-6736(15)60463-9]). Earlier in the meeting, she reported that the PROMISE trial found no difference in its primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications among chest pain patients evaluated with CTA or functional testing.
Finally, it was noted that radiation exposure in SCOT-HEART (median 4.1 mSv) was substantially lower than that reported in PROMISE, a finding Dr. Newby said he could not explain.
SAN DIEGO – The addition of CT angiography to standard care changed the diagnosis and treatment of one in four patients with stable chest pain in the prospective, randomized SCOT-HEART trial.
CT angiography (CTA) also reduced coronary heart disease deaths or myocardial infarctions by 38% after a median follow-up of 1.7 years, although the finding was of borderline significance (hazard ratio, 0.62; P = .053).
A post-hoc, landmark analysis, however, that accounted for the roughly 6-week delay between the clinic visit and implementation or alteration of therapy based on CTA findings, showed a halving of these outcomes (HR, 0.50; P = .015), chief investigator Dr. David Newby reported at the annual meeting of the American College of Cardiology.
SCOT-HEART (Scottish COmputed Tomography of the Heart trial) involved 4,146 patients referred from chest pain clinics across Scotland for assessment of suspected angina due to coronary artery disease, of whom 47% were diagnosed in the clinic with coronary heart disease and 36% with angina due to coronary heart disease. Patients were then evenly randomized to standard care involving cardiovascular risk assessment with the ASSIGN Score alone or with CTA.
When attending clinicians reviewed the cases at 6 weeks, the diagnosis of coronary heart disease (CHD) changed in 25% of patients assigned CTA vs. only 1% assigned standard care alone and the diagnosis of angina due to CHD changed in 23% vs. 1% (P value < .001 for both), Dr. Newby, from the University of Edinburgh, said.
Clinicians reported that CTA significantly increased the certainty (Relative risk, 2.56; P < .0001) and frequency (RR, 1.09; P = .017) of the diagnosis of CHD and increased the certainty of a diagnosis of angina due to CHD (RR, 1.79; P < .0001), but had no effect on its frequency (RR, 0.93; P = .12).
Overall, 63% of patients had evidence of CHD on CTA, with 25% having obstructive disease.
CTA altered subsequent testing in 15% of patients vs. only 1% with standard care (P < .001). CTA use was associated with the cancellation of 121 functional stress tests and 29 invasive coronary angiography exams. CTA also prompted 94 new angiograms vs. just 8 with standard care, but this was mainly the result of the exclusion or discovery of obstructive coronary heart disease, including triple vessel disease, Dr. Newby observed. CT was associated with a nonsignificant increase in coronary revascularizations (11.2% vs. 9.7%; HR, 1.19; P .06).
The changes in diagnosis and testing were associated with changes in subsequent treatment in 23% of CTA patients vs. 5% of standard care patients overall (P < .001), including recommendations and cancellations for preventive and anti-anginal therapies. The results were also simultaneously published online (Lancet 2015 [doi:10.19016/S0140-6736(15)060291-4]).
The most impressive aspect of SCOT-HEART was the strong trend for improved outcomes in patients for which therapeutic alterations were made, Dr. Eric Peterson, with the Duke University in Durham, N.C., commented.
“This sets the standard for how we perform and evaluate whether CT can improve outcomes for patients,” he said.
In an editorial accompanying the report,, Dr. Pamela Douglas, from the Duke Clinical Research Institute in Durham, N.C., called the finding of reduced death and MI “intriguing,” but urged caution in its interpretation because it was one of 22 secondary end points and the absolute difference between groups was only 16 events (Lancet 2015; [doi: 10.1016/S0140-6736(15)60463-9]). Earlier in the meeting, she reported that the PROMISE trial found no difference in its primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications among chest pain patients evaluated with CTA or functional testing.
Finally, it was noted that radiation exposure in SCOT-HEART (median 4.1 mSv) was substantially lower than that reported in PROMISE, a finding Dr. Newby said he could not explain.
AT ACC 2015
Key clinical point:CTA clarifies the diagnosis and leads to major alterations in testing and treatments in patients with suspected angina due to coronary heart disease.
Major finding:The addition of CT angiography changed the diagnosis and treatment of one in four patients with stable chest pain.
Data source: SCOT-HEART, a prospective, randomized study in 4,146 patients with new-onset, stable chest pain.
Disclosures: The study was funded by the Chief Scientist Office of the Scottish Government Health and Social Care Directorates, with supplementary awards from Edinburgh and Lothian’s Health Foundation Trust and the Heart Diseases Research Fund. Dr. Newby reported consultant fees and honoraria from Eli-Lilly, Roche, Toshiba, Pfizer, AstraZeneca, MSD, BMS, Boeringer Ingelheim, GlaxoSmithKline.
Evolocumab halved cardiovascular events in OSLER study
SAN DIEGO– The investigational PCSK9 inhibitor evolucumab dramatically reduced the 1-year cardiovascular event rate, by 53%, compared with standard statin-based lipid-lowering in the randomized OSLER study.
This reduction in adverse cardiovascular events was accompanied by a robust 61% reduction in LDL compared with standard therapy. The LDL level in evolocumab-treated patients dropped from 120 mg/dL to an average of 48 mg/dL, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The safety profile of patients on evolocumab plus standard, statin-based lipid lowering was essentially the same as in controls on standard therapy alone. Moreover, no gradient was seen for any adverse events on the basis of the extent of LDL lowering. For example, the types and incidence of adverse events and laboratory abnormalities in the 773 evolocumab-treated OSLER participants with an achieved LDL less than 25 mg/dL were closely similar to those seen with an LDL above 40 mg/dL, according to Dr. Sabatine, chairman of the Thrombolysis In Myocardial Infarction Study Group at Brigham and Women’s Hospital in Boston.
“These data, in conjuction with epidemiological and genetic data, offer further support for the potential for PCSK9 inhibition as a safe and effective means to reduce major adverse cardiovascular outcomes through particularly robust LDL cholesterol lowering,” he added.
OSLER (Open-Label Study of Long-Term Evaluation against LDL Cholesterol) included 4,465 patients who had completed one of a dozen earlier phase II or III studies of evolucumab, a monoclonal antibody that inhibits proprotein convertase subtilisin kexin type 9 (PCSK9), and were then randomized 2:1 to 1 year of open-label evolucumab administered subcutaneously at either 140 mg every 2 weeks or 420 mg once monthly plus standard lipid-lowering, or to standard lipid-lowering alone, generally with moderate- or high-dose statins.
The PCSK9 inhibitor reduced LDL cholesterol by 73 mg/dL compared to the control arm. In addition, the evolocumab group experienced a 26% decrease in Lp(a), a 47% drop in ApoB, a 13% reduction in triglycerides, and a 7% rise in HDL relative to standard care.
The 1-year composite cardiovascular event rate was just 0.95% in the evolucumab group, a 53% reduction relative to the 2.18% rate in the control arm. The composite outcome was comprised of death, MI, stroke or TIA, hospitalization for heart failure, coronary revascularization, or hospitalization for unstable angina. The reduction in events seen with evolocumab was consistent across all the components of the composite outcome.
Rates of most adverse events were closely similar in the two study arms. The exception was self-reported neurocognitive events such as forgetfulness or confusion, where the 0.9% incidence in the evolucumab group, while quite low in an absolute sense, was nonetheless threefold higher than in controls.
While the OSLER findings are highly encouraging in terms of both efficacy and safety, the study was too small and too brief at 1 year to be considered definitive, especially in terms of cardiovascular event rates, of which there only 60 in total. All eyes are now on the ongoing 27,500-patient, randomized, placebo-controlled FOURIER (Further Cardiovascular Outcomes Research with PCSK9 Inhibition in Subjects with Elevated Risk) study. Participants in FOURIER must have a history of MI, stroke, or peripheral artery disease plus at least one additional high-risk feature. Results are expected in 2017.
Similar massive pivotal phase III studies of two other highly promising PCSK9 inhibitors – alirocumab and bococizumab – are ongoing. The PCSK9 inhibitors were the talk of ACC 2015 in light of the mounting impressive safety and efficacy data. The Food and Drug Administration is now considering whether to approve PCSK9 inhibition for patients with familial hypercholesterolemia whose LDL is not adequately controlled by statins, with a decision expected later this year.
Discussant Dr. Christopher P. Cannon called OSLER “a terrific study.”
The OSLER findings, coupled with a previously reported preliminary analysis suggesting reduced cardiovascular events in clinical trials of alirocumab, provide strong support for the notion that the lower the achieved LDL – whether accomplished by statins or other agents – the greater the cardiovascular benefit.
“This is so exciting. Lowering cholesterol is definitely a passion of mine,” said Dr. Cannon, professor of medicine at Harvard Medical School, Boston.
Discussant Dr. Judith S. Hochman was equally enthusiastic about the OSLER outcomes.
“This is really impressive and very encouraging for this class of cholesterol-lowering agents. And I want to congratulate you for enrolling 50% women. But we need more study about the potential for neurocognitive events,” commented Dr. Hochman, professor of cardiology and senior associate dean for clinical sciences at New York University.
Dr. Sabatine agreed. While neurocognitive events in OSLER were self-reported by patients, FOURIER includes a substudy featuring formal neurocognitive testing using validated instruments. And while that should provide definitive answers, he said he’s not too concerned about the neurocognitive issue.
“Biologically, LDL cholesterol is not used as a source of cholesterol for cells, and that’s especially true for cells in the CNS because of the blood-brain barrier. And very low LDL levels don’t appear to have any effect on the CNS in animal models,” he said.
A more comprehensive picture of evolucumab’s safety was provided elsewhere at ACC 15 by Dr. Peter P. Toth. His safety analysis incorporated more than 6,000 evolucumab-treated patients and 3,569 controls who participated in a dozen phase II and III trials as well as OSLER.
The short version: This pooled analysis demonstrated no increase in any clinical adverse events or laboratory abnormalities with evolocumab, compared with controls. That includes muscle-related adverse events, liver or renal toxicity, impairment in glucose metabolism, infections, injection-site reactions, and neurocognitive events, said Dr. Toth of the University of Illinois, Peoria.
Simultaneous with Dr. Sabatine’s presentation at ACC 15, the OSLER results were published online (N. Engl. J. Med. 2015 [doi: 10.1056/NEJMoa1500858]).
Both OSLER and Dr. Toth’s broader safety analysis were funded by Amgen. Dr. Sabatine and Dr. Toth reported having received research grant support from and serving as consultants to Amgen and numerous other pharmaceutical companies. Dr. Hochman is a consultant to GlaxoSmithKline. Dr. Cannon has received research grant support from and served as a consultant or advisor to many pharmaceutical companies.
SAN DIEGO– The investigational PCSK9 inhibitor evolucumab dramatically reduced the 1-year cardiovascular event rate, by 53%, compared with standard statin-based lipid-lowering in the randomized OSLER study.
This reduction in adverse cardiovascular events was accompanied by a robust 61% reduction in LDL compared with standard therapy. The LDL level in evolocumab-treated patients dropped from 120 mg/dL to an average of 48 mg/dL, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The safety profile of patients on evolocumab plus standard, statin-based lipid lowering was essentially the same as in controls on standard therapy alone. Moreover, no gradient was seen for any adverse events on the basis of the extent of LDL lowering. For example, the types and incidence of adverse events and laboratory abnormalities in the 773 evolocumab-treated OSLER participants with an achieved LDL less than 25 mg/dL were closely similar to those seen with an LDL above 40 mg/dL, according to Dr. Sabatine, chairman of the Thrombolysis In Myocardial Infarction Study Group at Brigham and Women’s Hospital in Boston.
“These data, in conjuction with epidemiological and genetic data, offer further support for the potential for PCSK9 inhibition as a safe and effective means to reduce major adverse cardiovascular outcomes through particularly robust LDL cholesterol lowering,” he added.
OSLER (Open-Label Study of Long-Term Evaluation against LDL Cholesterol) included 4,465 patients who had completed one of a dozen earlier phase II or III studies of evolucumab, a monoclonal antibody that inhibits proprotein convertase subtilisin kexin type 9 (PCSK9), and were then randomized 2:1 to 1 year of open-label evolucumab administered subcutaneously at either 140 mg every 2 weeks or 420 mg once monthly plus standard lipid-lowering, or to standard lipid-lowering alone, generally with moderate- or high-dose statins.
The PCSK9 inhibitor reduced LDL cholesterol by 73 mg/dL compared to the control arm. In addition, the evolocumab group experienced a 26% decrease in Lp(a), a 47% drop in ApoB, a 13% reduction in triglycerides, and a 7% rise in HDL relative to standard care.
The 1-year composite cardiovascular event rate was just 0.95% in the evolucumab group, a 53% reduction relative to the 2.18% rate in the control arm. The composite outcome was comprised of death, MI, stroke or TIA, hospitalization for heart failure, coronary revascularization, or hospitalization for unstable angina. The reduction in events seen with evolocumab was consistent across all the components of the composite outcome.
Rates of most adverse events were closely similar in the two study arms. The exception was self-reported neurocognitive events such as forgetfulness or confusion, where the 0.9% incidence in the evolucumab group, while quite low in an absolute sense, was nonetheless threefold higher than in controls.
While the OSLER findings are highly encouraging in terms of both efficacy and safety, the study was too small and too brief at 1 year to be considered definitive, especially in terms of cardiovascular event rates, of which there only 60 in total. All eyes are now on the ongoing 27,500-patient, randomized, placebo-controlled FOURIER (Further Cardiovascular Outcomes Research with PCSK9 Inhibition in Subjects with Elevated Risk) study. Participants in FOURIER must have a history of MI, stroke, or peripheral artery disease plus at least one additional high-risk feature. Results are expected in 2017.
Similar massive pivotal phase III studies of two other highly promising PCSK9 inhibitors – alirocumab and bococizumab – are ongoing. The PCSK9 inhibitors were the talk of ACC 2015 in light of the mounting impressive safety and efficacy data. The Food and Drug Administration is now considering whether to approve PCSK9 inhibition for patients with familial hypercholesterolemia whose LDL is not adequately controlled by statins, with a decision expected later this year.
Discussant Dr. Christopher P. Cannon called OSLER “a terrific study.”
The OSLER findings, coupled with a previously reported preliminary analysis suggesting reduced cardiovascular events in clinical trials of alirocumab, provide strong support for the notion that the lower the achieved LDL – whether accomplished by statins or other agents – the greater the cardiovascular benefit.
“This is so exciting. Lowering cholesterol is definitely a passion of mine,” said Dr. Cannon, professor of medicine at Harvard Medical School, Boston.
Discussant Dr. Judith S. Hochman was equally enthusiastic about the OSLER outcomes.
“This is really impressive and very encouraging for this class of cholesterol-lowering agents. And I want to congratulate you for enrolling 50% women. But we need more study about the potential for neurocognitive events,” commented Dr. Hochman, professor of cardiology and senior associate dean for clinical sciences at New York University.
Dr. Sabatine agreed. While neurocognitive events in OSLER were self-reported by patients, FOURIER includes a substudy featuring formal neurocognitive testing using validated instruments. And while that should provide definitive answers, he said he’s not too concerned about the neurocognitive issue.
“Biologically, LDL cholesterol is not used as a source of cholesterol for cells, and that’s especially true for cells in the CNS because of the blood-brain barrier. And very low LDL levels don’t appear to have any effect on the CNS in animal models,” he said.
A more comprehensive picture of evolucumab’s safety was provided elsewhere at ACC 15 by Dr. Peter P. Toth. His safety analysis incorporated more than 6,000 evolucumab-treated patients and 3,569 controls who participated in a dozen phase II and III trials as well as OSLER.
The short version: This pooled analysis demonstrated no increase in any clinical adverse events or laboratory abnormalities with evolocumab, compared with controls. That includes muscle-related adverse events, liver or renal toxicity, impairment in glucose metabolism, infections, injection-site reactions, and neurocognitive events, said Dr. Toth of the University of Illinois, Peoria.
Simultaneous with Dr. Sabatine’s presentation at ACC 15, the OSLER results were published online (N. Engl. J. Med. 2015 [doi: 10.1056/NEJMoa1500858]).
Both OSLER and Dr. Toth’s broader safety analysis were funded by Amgen. Dr. Sabatine and Dr. Toth reported having received research grant support from and serving as consultants to Amgen and numerous other pharmaceutical companies. Dr. Hochman is a consultant to GlaxoSmithKline. Dr. Cannon has received research grant support from and served as a consultant or advisor to many pharmaceutical companies.
SAN DIEGO– The investigational PCSK9 inhibitor evolucumab dramatically reduced the 1-year cardiovascular event rate, by 53%, compared with standard statin-based lipid-lowering in the randomized OSLER study.
This reduction in adverse cardiovascular events was accompanied by a robust 61% reduction in LDL compared with standard therapy. The LDL level in evolocumab-treated patients dropped from 120 mg/dL to an average of 48 mg/dL, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The safety profile of patients on evolocumab plus standard, statin-based lipid lowering was essentially the same as in controls on standard therapy alone. Moreover, no gradient was seen for any adverse events on the basis of the extent of LDL lowering. For example, the types and incidence of adverse events and laboratory abnormalities in the 773 evolocumab-treated OSLER participants with an achieved LDL less than 25 mg/dL were closely similar to those seen with an LDL above 40 mg/dL, according to Dr. Sabatine, chairman of the Thrombolysis In Myocardial Infarction Study Group at Brigham and Women’s Hospital in Boston.
“These data, in conjuction with epidemiological and genetic data, offer further support for the potential for PCSK9 inhibition as a safe and effective means to reduce major adverse cardiovascular outcomes through particularly robust LDL cholesterol lowering,” he added.
OSLER (Open-Label Study of Long-Term Evaluation against LDL Cholesterol) included 4,465 patients who had completed one of a dozen earlier phase II or III studies of evolucumab, a monoclonal antibody that inhibits proprotein convertase subtilisin kexin type 9 (PCSK9), and were then randomized 2:1 to 1 year of open-label evolucumab administered subcutaneously at either 140 mg every 2 weeks or 420 mg once monthly plus standard lipid-lowering, or to standard lipid-lowering alone, generally with moderate- or high-dose statins.
The PCSK9 inhibitor reduced LDL cholesterol by 73 mg/dL compared to the control arm. In addition, the evolocumab group experienced a 26% decrease in Lp(a), a 47% drop in ApoB, a 13% reduction in triglycerides, and a 7% rise in HDL relative to standard care.
The 1-year composite cardiovascular event rate was just 0.95% in the evolucumab group, a 53% reduction relative to the 2.18% rate in the control arm. The composite outcome was comprised of death, MI, stroke or TIA, hospitalization for heart failure, coronary revascularization, or hospitalization for unstable angina. The reduction in events seen with evolocumab was consistent across all the components of the composite outcome.
Rates of most adverse events were closely similar in the two study arms. The exception was self-reported neurocognitive events such as forgetfulness or confusion, where the 0.9% incidence in the evolucumab group, while quite low in an absolute sense, was nonetheless threefold higher than in controls.
While the OSLER findings are highly encouraging in terms of both efficacy and safety, the study was too small and too brief at 1 year to be considered definitive, especially in terms of cardiovascular event rates, of which there only 60 in total. All eyes are now on the ongoing 27,500-patient, randomized, placebo-controlled FOURIER (Further Cardiovascular Outcomes Research with PCSK9 Inhibition in Subjects with Elevated Risk) study. Participants in FOURIER must have a history of MI, stroke, or peripheral artery disease plus at least one additional high-risk feature. Results are expected in 2017.
Similar massive pivotal phase III studies of two other highly promising PCSK9 inhibitors – alirocumab and bococizumab – are ongoing. The PCSK9 inhibitors were the talk of ACC 2015 in light of the mounting impressive safety and efficacy data. The Food and Drug Administration is now considering whether to approve PCSK9 inhibition for patients with familial hypercholesterolemia whose LDL is not adequately controlled by statins, with a decision expected later this year.
Discussant Dr. Christopher P. Cannon called OSLER “a terrific study.”
The OSLER findings, coupled with a previously reported preliminary analysis suggesting reduced cardiovascular events in clinical trials of alirocumab, provide strong support for the notion that the lower the achieved LDL – whether accomplished by statins or other agents – the greater the cardiovascular benefit.
“This is so exciting. Lowering cholesterol is definitely a passion of mine,” said Dr. Cannon, professor of medicine at Harvard Medical School, Boston.
Discussant Dr. Judith S. Hochman was equally enthusiastic about the OSLER outcomes.
“This is really impressive and very encouraging for this class of cholesterol-lowering agents. And I want to congratulate you for enrolling 50% women. But we need more study about the potential for neurocognitive events,” commented Dr. Hochman, professor of cardiology and senior associate dean for clinical sciences at New York University.
Dr. Sabatine agreed. While neurocognitive events in OSLER were self-reported by patients, FOURIER includes a substudy featuring formal neurocognitive testing using validated instruments. And while that should provide definitive answers, he said he’s not too concerned about the neurocognitive issue.
“Biologically, LDL cholesterol is not used as a source of cholesterol for cells, and that’s especially true for cells in the CNS because of the blood-brain barrier. And very low LDL levels don’t appear to have any effect on the CNS in animal models,” he said.
A more comprehensive picture of evolucumab’s safety was provided elsewhere at ACC 15 by Dr. Peter P. Toth. His safety analysis incorporated more than 6,000 evolucumab-treated patients and 3,569 controls who participated in a dozen phase II and III trials as well as OSLER.
The short version: This pooled analysis demonstrated no increase in any clinical adverse events or laboratory abnormalities with evolocumab, compared with controls. That includes muscle-related adverse events, liver or renal toxicity, impairment in glucose metabolism, infections, injection-site reactions, and neurocognitive events, said Dr. Toth of the University of Illinois, Peoria.
Simultaneous with Dr. Sabatine’s presentation at ACC 15, the OSLER results were published online (N. Engl. J. Med. 2015 [doi: 10.1056/NEJMoa1500858]).
Both OSLER and Dr. Toth’s broader safety analysis were funded by Amgen. Dr. Sabatine and Dr. Toth reported having received research grant support from and serving as consultants to Amgen and numerous other pharmaceutical companies. Dr. Hochman is a consultant to GlaxoSmithKline. Dr. Cannon has received research grant support from and served as a consultant or advisor to many pharmaceutical companies.
AT ACC 15
Key clinical point: Evolocumab shows impressive LDL lowering and slashes cardiovascular events.
Major finding: The PCSK9 inhibitor lowered LDL by an average of 73 mg/dL more than standard lipid-lowering therapy alone while reducing the 1-year rate of composite cardiovascular events by 53%.
Data source: The OSLER study included 4,465 patients who were randomized to 1 year of open-label evolocumab plus standard statin-based lipid-lowering or to standard lipid-lowering alone.
Disclosures: OSLER was funded by Amgen. The presenter reported receiving research grant support from and serving as a consultant to Amgen and numerous other pharmaceutical companies.
Long-term DAPT offers ongoing post-MI benefit
SAN DIEGO – The idea that patients with established coronary disease can derive important, secondary-prevention benefit from prolonged dual-antiplatelet therapy received a major boost with the results of a major, international, controlled trial with more than 21,000 patients.
Results from the PEGASUS-TIMI 54 (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction 54) showed putting post-myocardial infarction patients on dual-antiplatelet therapy (DAPT) with aspirin and the thienopyridine ticagrelor (Brilinta) for a median of 33 months cut the combined incidence of cardiovascular death, MI, or stroke by a relative 15%, compared with patients on aspirin alone as well as the other standard treatments used for post-MI patients, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The findings added to the growing body of evidence that long-term – and possibly lifelong – DAPT is a key part of secondary prevention. Last year, results from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66) supplied evidence for this in acute coronary syndrome patients who had undergone percutaneous coronary intervention (PCI). The PEGASUS-TIMI 54 trial did not require that enrolled post-MI patients had undergone PCI, but the reality is that this is the way most MI patients get managed, and in PEGASUS-TIMI 54 roughly 83% of the patients had a PCI history.
The new findings also highlighted the risk-benefit trade-off that DAPT means for patients. In PEGASUS-TIMI 54 the increased incidence of major bleeding events roughly matched the decreased rate of major cardiovascular events prevented. But while the incidence of bleeds categorized as TIMI major bleeds more than doubled in the patients randomized to DAPT compared with those on aspirin only, the prolonged treatment with ticagrelor did not result in an increase in fatal bleeds or in intracranial hemorrhages, the two most feared types of TIMI major bleeds.
“I’d much rather prevent cardiovascular deaths, MIs, and strokes even at the expense of causing reversible, nonfatal bleeding events,” said Dr. Sabatine, professor of medicine at Harvard Medical School in Boston and chairman of the TIMI Study Group at Brigham and Women’s Hospital.
Another notable adverse effect from ticagrelor treatment was a roughly threefold increased incidence of dyspnea, which led to drug discontinuation in 5%-7% of patients, depending on whether they received ticagrelor at 60 mg b.i.d. or 90 mg b.i.d. The study results showed a reduced rate of both bleeding and dyspnea in patients randomized to receive the 60-mg b.i.d. dosage, compared with those who received the 90-mg b.i.d. dosage, which is the standard ticagrelor dosage and the formulation now sold. At the same time, the efficacy of the 60-mg b.i.d. dosage for preventing ischemic events equaled that of the higher dosage. But as of today, it is impossible for a physician to prescribe a 60-mg formulation of ticagrelor because the manufacturer does not sell it.
Several cardiologists PEGASUS-TIMI 54 at the meeting said that they agreed with Dr. Sabatine and felt that the benefits from prolonged DAPT with ticagrelor outweighed the downside of an increased bleeding risk.
“I think that the benefit is greater than the risk. None of us wants to see patients experience bleeding, but I was encouraged that fatal bleeds and intracranial hemorrhages were no different,” commented Dr. Elliott M. Antman, a professor of medicine at Harvard.
“The benefits outweigh the bleeding risk, but I wouldn’t trivialize the bleeding risk. Assessing a patient’s bleeding risk is really important,” commented Dr. Robert Harrington, professor of medicine at Stanford (Calif.) University.
But others at the meeting said that the elevated bleeding risk gave them pause. “There clearly is a price to be paid even if extended-duration DAPT reduces MI and stent thrombosis. I believe only the highest risk patients – those with acute coronary syndrome and ST-elevation MI – are the ones for whom I’d even consider it. Unless we can reduce bleeding risk, maybe with even lower doses [of ticagrelor], stopping aspirin, or using a reversal agent, we will be causing bleeds that are very relevant to patients,” commented Dr. Ajay J. Kirtane, an interventional cardiologist at Columbia University in New York.
Dr. Kirtane also questioned whether TIMI major bleeds was the appropriate measure of bleeding risk in the context of a study like PEGASUS-TIMI 54. “Historically, TIMI major bleeding was derived from studies of acute heart attack patients getting fibrinolytic therapy. That is a very different population from this one. In my mind, the combination of TIMI major and minor bleeding would be more encompassing, and for patients the bleeding risks of these therapies are real and have been associated with bad sequelae,” he said in an interview.
When placed in the context of prior reports the new findings also raise the possibility that the generic, and hence much cheaper, thienopyridine clopidogrel might provide roughly the same long-term benefit as more expensive ticagrelor, especially for patients without a genetic profile that makes them poor clopidogrel metabolizers. This may be an attractive option for patients who have a problem paying for ticagrelor long term.
“I’d rather prescribe a patient a cheaper medication that might be a bit less effective than create an economic hardship,” Dr. Harrington said in an interview. The results from the DAPT trial, which included some post-PCI patients who received long-term DAPT with clopidogrel plus aspirin “give you a certain comfort” with the idea of substituting clopidogrel for ticagrelor when affordability is a major concern, Dr. Harrington noted.
PEGASUS-TIMI 54 enrolled 21, 162 patients who were 1-3 years out from a prior myocardial infarction at 1,161 sites in 31 countries. Enrolled patients also had to be at least 50 years old, and have at least one additional risk factor for ischemic events such as age 65 years or older, diabetes, multivessel coronary artery disease, or chronic renal dysfunction. The enrolled patients averaged 1.7 years out from their index MI. Randomization assigned patients to treatment with 90 mg ticagrelor b.i.d., 60 mg ticagrelor b.i.d., or placebo, and all patients also received daily treatment with 75-150 mg aspirin.
After a median follow-up of 33 months on treatment, the combined rate of cardiovascular death, myocardial infarction, or stroke – the study’s primary endpoint – occurred in 7.85% of patients on the 90-mg ticagrelor dosage, 7.77% of those on the 60-mg dosage, and in 9.04% of patients on placebo receiving aspirin only, statistically significant differences for the study’s primary endpoint for each of the two ticagrelor dosages. Concurrent with the report at the meeting the results also appeared online (N. Engl. J. Med. 2015; [doi:10.1056/nejmoa1500857]). This translated into hazard ratios of 0.85 for the 90 mg dosage and 0.84 for the 60 mg dosage compared with placebo.
The study’s primary safety outcome was the incidence of TIMI major bleeding events, which occurred in 2.60% of patients on the higher ticagrelor dosage, 2.30% of those on the 60 mg dosage, and in 1.06% of those on placebo, which converted into hazard ratios of 2.69 for the 90-mg dosage and 2.32 for the lower dosage for TIMI major bleeds compared with aspirin alone.
On Twitter @mitchelzoler
The results from PEGASUS-TIMI 54 provide a powerful message for secondary prevention: Patients who have had a prior myocardial infarction remain at an increased risk for subsequent ischemic events, even when maintained on what is currently standard therapy and even when they are several years out from their event.
Dr. Richard C. Becker |
We have no perfect antiplatelet drugs. Treating patients like those enrolled in the trial with an agent like ticagrelor further reduced their risk for ischemic events, but at the price of increasing their risk for major bleeds. The good news was that the rates of fatal bleeds and intracranial hemorrhages did not increase with ticagrelor treatment. Selecting the right patients to treat with prolonged dual antiplatelet therapy (DAPT) requires good judgment as well as understanding the patient’s values and preferences. From the clinician’s perspective it is the fatal bleeds or intracranial hemorrhages that are most comparable to cardiovascular deaths, myocardial infarctions or strokes. Although I do not want to minimize the impact of other major or minor bleeds that might require transfusions, these are not considered as important for patient well being as the ischemic events that ticagrelor treatment reduced.
I believe that the findings from PEGASUS-TIMI 54 will work their way into everyday practice with clinicians increasingly keeping patients on prolonged DAPT following percutaneous coronary interventions or a myocardial infarction. Problems with bleeding or dyspnea usually appear relatively early for patients on DAPT. The new findings give us increased confidence that once these patients get to a year out from the onset of treatment they can safely continue treatment and derive ongoing benefit from it, especially higher-risk patients, even though the 60-mg formulation of ticagrelor is not currently available. The new results complement those reported last year from the DAPT trial, which also addressed the safety and incremental value of more prolonged DAPT for higher-risk MI and acute coronary syndrome patients.
Richard C. Becker, M.D. is professor and director of the University of Cincinnati Heart, Lung and Vascular Institute. He has been a consultant to and received research grants from AstraZeneca, the company that sponsored PEGASUS-TIMI 54 and that markets ticagrelor (Brilinta). He made these comments in an interview.
The results from PEGASUS-TIMI 54 provide a powerful message for secondary prevention: Patients who have had a prior myocardial infarction remain at an increased risk for subsequent ischemic events, even when maintained on what is currently standard therapy and even when they are several years out from their event.
Dr. Richard C. Becker |
We have no perfect antiplatelet drugs. Treating patients like those enrolled in the trial with an agent like ticagrelor further reduced their risk for ischemic events, but at the price of increasing their risk for major bleeds. The good news was that the rates of fatal bleeds and intracranial hemorrhages did not increase with ticagrelor treatment. Selecting the right patients to treat with prolonged dual antiplatelet therapy (DAPT) requires good judgment as well as understanding the patient’s values and preferences. From the clinician’s perspective it is the fatal bleeds or intracranial hemorrhages that are most comparable to cardiovascular deaths, myocardial infarctions or strokes. Although I do not want to minimize the impact of other major or minor bleeds that might require transfusions, these are not considered as important for patient well being as the ischemic events that ticagrelor treatment reduced.
I believe that the findings from PEGASUS-TIMI 54 will work their way into everyday practice with clinicians increasingly keeping patients on prolonged DAPT following percutaneous coronary interventions or a myocardial infarction. Problems with bleeding or dyspnea usually appear relatively early for patients on DAPT. The new findings give us increased confidence that once these patients get to a year out from the onset of treatment they can safely continue treatment and derive ongoing benefit from it, especially higher-risk patients, even though the 60-mg formulation of ticagrelor is not currently available. The new results complement those reported last year from the DAPT trial, which also addressed the safety and incremental value of more prolonged DAPT for higher-risk MI and acute coronary syndrome patients.
Richard C. Becker, M.D. is professor and director of the University of Cincinnati Heart, Lung and Vascular Institute. He has been a consultant to and received research grants from AstraZeneca, the company that sponsored PEGASUS-TIMI 54 and that markets ticagrelor (Brilinta). He made these comments in an interview.
The results from PEGASUS-TIMI 54 provide a powerful message for secondary prevention: Patients who have had a prior myocardial infarction remain at an increased risk for subsequent ischemic events, even when maintained on what is currently standard therapy and even when they are several years out from their event.
Dr. Richard C. Becker |
We have no perfect antiplatelet drugs. Treating patients like those enrolled in the trial with an agent like ticagrelor further reduced their risk for ischemic events, but at the price of increasing their risk for major bleeds. The good news was that the rates of fatal bleeds and intracranial hemorrhages did not increase with ticagrelor treatment. Selecting the right patients to treat with prolonged dual antiplatelet therapy (DAPT) requires good judgment as well as understanding the patient’s values and preferences. From the clinician’s perspective it is the fatal bleeds or intracranial hemorrhages that are most comparable to cardiovascular deaths, myocardial infarctions or strokes. Although I do not want to minimize the impact of other major or minor bleeds that might require transfusions, these are not considered as important for patient well being as the ischemic events that ticagrelor treatment reduced.
I believe that the findings from PEGASUS-TIMI 54 will work their way into everyday practice with clinicians increasingly keeping patients on prolonged DAPT following percutaneous coronary interventions or a myocardial infarction. Problems with bleeding or dyspnea usually appear relatively early for patients on DAPT. The new findings give us increased confidence that once these patients get to a year out from the onset of treatment they can safely continue treatment and derive ongoing benefit from it, especially higher-risk patients, even though the 60-mg formulation of ticagrelor is not currently available. The new results complement those reported last year from the DAPT trial, which also addressed the safety and incremental value of more prolonged DAPT for higher-risk MI and acute coronary syndrome patients.
Richard C. Becker, M.D. is professor and director of the University of Cincinnati Heart, Lung and Vascular Institute. He has been a consultant to and received research grants from AstraZeneca, the company that sponsored PEGASUS-TIMI 54 and that markets ticagrelor (Brilinta). He made these comments in an interview.
SAN DIEGO – The idea that patients with established coronary disease can derive important, secondary-prevention benefit from prolonged dual-antiplatelet therapy received a major boost with the results of a major, international, controlled trial with more than 21,000 patients.
Results from the PEGASUS-TIMI 54 (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction 54) showed putting post-myocardial infarction patients on dual-antiplatelet therapy (DAPT) with aspirin and the thienopyridine ticagrelor (Brilinta) for a median of 33 months cut the combined incidence of cardiovascular death, MI, or stroke by a relative 15%, compared with patients on aspirin alone as well as the other standard treatments used for post-MI patients, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The findings added to the growing body of evidence that long-term – and possibly lifelong – DAPT is a key part of secondary prevention. Last year, results from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66) supplied evidence for this in acute coronary syndrome patients who had undergone percutaneous coronary intervention (PCI). The PEGASUS-TIMI 54 trial did not require that enrolled post-MI patients had undergone PCI, but the reality is that this is the way most MI patients get managed, and in PEGASUS-TIMI 54 roughly 83% of the patients had a PCI history.
The new findings also highlighted the risk-benefit trade-off that DAPT means for patients. In PEGASUS-TIMI 54 the increased incidence of major bleeding events roughly matched the decreased rate of major cardiovascular events prevented. But while the incidence of bleeds categorized as TIMI major bleeds more than doubled in the patients randomized to DAPT compared with those on aspirin only, the prolonged treatment with ticagrelor did not result in an increase in fatal bleeds or in intracranial hemorrhages, the two most feared types of TIMI major bleeds.
“I’d much rather prevent cardiovascular deaths, MIs, and strokes even at the expense of causing reversible, nonfatal bleeding events,” said Dr. Sabatine, professor of medicine at Harvard Medical School in Boston and chairman of the TIMI Study Group at Brigham and Women’s Hospital.
Another notable adverse effect from ticagrelor treatment was a roughly threefold increased incidence of dyspnea, which led to drug discontinuation in 5%-7% of patients, depending on whether they received ticagrelor at 60 mg b.i.d. or 90 mg b.i.d. The study results showed a reduced rate of both bleeding and dyspnea in patients randomized to receive the 60-mg b.i.d. dosage, compared with those who received the 90-mg b.i.d. dosage, which is the standard ticagrelor dosage and the formulation now sold. At the same time, the efficacy of the 60-mg b.i.d. dosage for preventing ischemic events equaled that of the higher dosage. But as of today, it is impossible for a physician to prescribe a 60-mg formulation of ticagrelor because the manufacturer does not sell it.
Several cardiologists PEGASUS-TIMI 54 at the meeting said that they agreed with Dr. Sabatine and felt that the benefits from prolonged DAPT with ticagrelor outweighed the downside of an increased bleeding risk.
“I think that the benefit is greater than the risk. None of us wants to see patients experience bleeding, but I was encouraged that fatal bleeds and intracranial hemorrhages were no different,” commented Dr. Elliott M. Antman, a professor of medicine at Harvard.
“The benefits outweigh the bleeding risk, but I wouldn’t trivialize the bleeding risk. Assessing a patient’s bleeding risk is really important,” commented Dr. Robert Harrington, professor of medicine at Stanford (Calif.) University.
But others at the meeting said that the elevated bleeding risk gave them pause. “There clearly is a price to be paid even if extended-duration DAPT reduces MI and stent thrombosis. I believe only the highest risk patients – those with acute coronary syndrome and ST-elevation MI – are the ones for whom I’d even consider it. Unless we can reduce bleeding risk, maybe with even lower doses [of ticagrelor], stopping aspirin, or using a reversal agent, we will be causing bleeds that are very relevant to patients,” commented Dr. Ajay J. Kirtane, an interventional cardiologist at Columbia University in New York.
Dr. Kirtane also questioned whether TIMI major bleeds was the appropriate measure of bleeding risk in the context of a study like PEGASUS-TIMI 54. “Historically, TIMI major bleeding was derived from studies of acute heart attack patients getting fibrinolytic therapy. That is a very different population from this one. In my mind, the combination of TIMI major and minor bleeding would be more encompassing, and for patients the bleeding risks of these therapies are real and have been associated with bad sequelae,” he said in an interview.
When placed in the context of prior reports the new findings also raise the possibility that the generic, and hence much cheaper, thienopyridine clopidogrel might provide roughly the same long-term benefit as more expensive ticagrelor, especially for patients without a genetic profile that makes them poor clopidogrel metabolizers. This may be an attractive option for patients who have a problem paying for ticagrelor long term.
“I’d rather prescribe a patient a cheaper medication that might be a bit less effective than create an economic hardship,” Dr. Harrington said in an interview. The results from the DAPT trial, which included some post-PCI patients who received long-term DAPT with clopidogrel plus aspirin “give you a certain comfort” with the idea of substituting clopidogrel for ticagrelor when affordability is a major concern, Dr. Harrington noted.
PEGASUS-TIMI 54 enrolled 21, 162 patients who were 1-3 years out from a prior myocardial infarction at 1,161 sites in 31 countries. Enrolled patients also had to be at least 50 years old, and have at least one additional risk factor for ischemic events such as age 65 years or older, diabetes, multivessel coronary artery disease, or chronic renal dysfunction. The enrolled patients averaged 1.7 years out from their index MI. Randomization assigned patients to treatment with 90 mg ticagrelor b.i.d., 60 mg ticagrelor b.i.d., or placebo, and all patients also received daily treatment with 75-150 mg aspirin.
After a median follow-up of 33 months on treatment, the combined rate of cardiovascular death, myocardial infarction, or stroke – the study’s primary endpoint – occurred in 7.85% of patients on the 90-mg ticagrelor dosage, 7.77% of those on the 60-mg dosage, and in 9.04% of patients on placebo receiving aspirin only, statistically significant differences for the study’s primary endpoint for each of the two ticagrelor dosages. Concurrent with the report at the meeting the results also appeared online (N. Engl. J. Med. 2015; [doi:10.1056/nejmoa1500857]). This translated into hazard ratios of 0.85 for the 90 mg dosage and 0.84 for the 60 mg dosage compared with placebo.
The study’s primary safety outcome was the incidence of TIMI major bleeding events, which occurred in 2.60% of patients on the higher ticagrelor dosage, 2.30% of those on the 60 mg dosage, and in 1.06% of those on placebo, which converted into hazard ratios of 2.69 for the 90-mg dosage and 2.32 for the lower dosage for TIMI major bleeds compared with aspirin alone.
On Twitter @mitchelzoler
SAN DIEGO – The idea that patients with established coronary disease can derive important, secondary-prevention benefit from prolonged dual-antiplatelet therapy received a major boost with the results of a major, international, controlled trial with more than 21,000 patients.
Results from the PEGASUS-TIMI 54 (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction 54) showed putting post-myocardial infarction patients on dual-antiplatelet therapy (DAPT) with aspirin and the thienopyridine ticagrelor (Brilinta) for a median of 33 months cut the combined incidence of cardiovascular death, MI, or stroke by a relative 15%, compared with patients on aspirin alone as well as the other standard treatments used for post-MI patients, Dr. Marc S. Sabatine reported at the annual meeting of the American College of Cardiology.
The findings added to the growing body of evidence that long-term – and possibly lifelong – DAPT is a key part of secondary prevention. Last year, results from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66) supplied evidence for this in acute coronary syndrome patients who had undergone percutaneous coronary intervention (PCI). The PEGASUS-TIMI 54 trial did not require that enrolled post-MI patients had undergone PCI, but the reality is that this is the way most MI patients get managed, and in PEGASUS-TIMI 54 roughly 83% of the patients had a PCI history.
The new findings also highlighted the risk-benefit trade-off that DAPT means for patients. In PEGASUS-TIMI 54 the increased incidence of major bleeding events roughly matched the decreased rate of major cardiovascular events prevented. But while the incidence of bleeds categorized as TIMI major bleeds more than doubled in the patients randomized to DAPT compared with those on aspirin only, the prolonged treatment with ticagrelor did not result in an increase in fatal bleeds or in intracranial hemorrhages, the two most feared types of TIMI major bleeds.
“I’d much rather prevent cardiovascular deaths, MIs, and strokes even at the expense of causing reversible, nonfatal bleeding events,” said Dr. Sabatine, professor of medicine at Harvard Medical School in Boston and chairman of the TIMI Study Group at Brigham and Women’s Hospital.
Another notable adverse effect from ticagrelor treatment was a roughly threefold increased incidence of dyspnea, which led to drug discontinuation in 5%-7% of patients, depending on whether they received ticagrelor at 60 mg b.i.d. or 90 mg b.i.d. The study results showed a reduced rate of both bleeding and dyspnea in patients randomized to receive the 60-mg b.i.d. dosage, compared with those who received the 90-mg b.i.d. dosage, which is the standard ticagrelor dosage and the formulation now sold. At the same time, the efficacy of the 60-mg b.i.d. dosage for preventing ischemic events equaled that of the higher dosage. But as of today, it is impossible for a physician to prescribe a 60-mg formulation of ticagrelor because the manufacturer does not sell it.
Several cardiologists PEGASUS-TIMI 54 at the meeting said that they agreed with Dr. Sabatine and felt that the benefits from prolonged DAPT with ticagrelor outweighed the downside of an increased bleeding risk.
“I think that the benefit is greater than the risk. None of us wants to see patients experience bleeding, but I was encouraged that fatal bleeds and intracranial hemorrhages were no different,” commented Dr. Elliott M. Antman, a professor of medicine at Harvard.
“The benefits outweigh the bleeding risk, but I wouldn’t trivialize the bleeding risk. Assessing a patient’s bleeding risk is really important,” commented Dr. Robert Harrington, professor of medicine at Stanford (Calif.) University.
But others at the meeting said that the elevated bleeding risk gave them pause. “There clearly is a price to be paid even if extended-duration DAPT reduces MI and stent thrombosis. I believe only the highest risk patients – those with acute coronary syndrome and ST-elevation MI – are the ones for whom I’d even consider it. Unless we can reduce bleeding risk, maybe with even lower doses [of ticagrelor], stopping aspirin, or using a reversal agent, we will be causing bleeds that are very relevant to patients,” commented Dr. Ajay J. Kirtane, an interventional cardiologist at Columbia University in New York.
Dr. Kirtane also questioned whether TIMI major bleeds was the appropriate measure of bleeding risk in the context of a study like PEGASUS-TIMI 54. “Historically, TIMI major bleeding was derived from studies of acute heart attack patients getting fibrinolytic therapy. That is a very different population from this one. In my mind, the combination of TIMI major and minor bleeding would be more encompassing, and for patients the bleeding risks of these therapies are real and have been associated with bad sequelae,” he said in an interview.
When placed in the context of prior reports the new findings also raise the possibility that the generic, and hence much cheaper, thienopyridine clopidogrel might provide roughly the same long-term benefit as more expensive ticagrelor, especially for patients without a genetic profile that makes them poor clopidogrel metabolizers. This may be an attractive option for patients who have a problem paying for ticagrelor long term.
“I’d rather prescribe a patient a cheaper medication that might be a bit less effective than create an economic hardship,” Dr. Harrington said in an interview. The results from the DAPT trial, which included some post-PCI patients who received long-term DAPT with clopidogrel plus aspirin “give you a certain comfort” with the idea of substituting clopidogrel for ticagrelor when affordability is a major concern, Dr. Harrington noted.
PEGASUS-TIMI 54 enrolled 21, 162 patients who were 1-3 years out from a prior myocardial infarction at 1,161 sites in 31 countries. Enrolled patients also had to be at least 50 years old, and have at least one additional risk factor for ischemic events such as age 65 years or older, diabetes, multivessel coronary artery disease, or chronic renal dysfunction. The enrolled patients averaged 1.7 years out from their index MI. Randomization assigned patients to treatment with 90 mg ticagrelor b.i.d., 60 mg ticagrelor b.i.d., or placebo, and all patients also received daily treatment with 75-150 mg aspirin.
After a median follow-up of 33 months on treatment, the combined rate of cardiovascular death, myocardial infarction, or stroke – the study’s primary endpoint – occurred in 7.85% of patients on the 90-mg ticagrelor dosage, 7.77% of those on the 60-mg dosage, and in 9.04% of patients on placebo receiving aspirin only, statistically significant differences for the study’s primary endpoint for each of the two ticagrelor dosages. Concurrent with the report at the meeting the results also appeared online (N. Engl. J. Med. 2015; [doi:10.1056/nejmoa1500857]). This translated into hazard ratios of 0.85 for the 90 mg dosage and 0.84 for the 60 mg dosage compared with placebo.
The study’s primary safety outcome was the incidence of TIMI major bleeding events, which occurred in 2.60% of patients on the higher ticagrelor dosage, 2.30% of those on the 60 mg dosage, and in 1.06% of those on placebo, which converted into hazard ratios of 2.69 for the 90-mg dosage and 2.32 for the lower dosage for TIMI major bleeds compared with aspirin alone.
On Twitter @mitchelzoler
AT ACC 15
Key clinical point: Myocardial infarction patients 1-3 years out from their event who took long-term dual-antiplatelet therapy with aspirin and ticagrelor had significantly fewer major ischemic events but also significantly more major bleeding events.
Major finding: Treatment with ticagrelor plus aspirin for 3 years cut major ischemic events by a relative 15% compared with aspirin alone.
Data source: PEGASUS-TIMI 54, a multicenter, randomized trial with 21,162 patients.
Disclosures: PEGASUS-TIMI 54 was sponsored by AstraZeneca, the company that markets ticagrelor (Brilinta). Dr. Sabatine has received research support from AstraZeneca and from several other companies, and has been a consultant to several drug companies. Dr. Antman has received research support from AstraZeneca, Eli Lilly, and Daiichi Sankyo. Dr. Harrington was an investigator for the trial that led to ticagrelor’s marketing approval and received research support from AstraZeneca and several other companies. Dr. Kirtane has received research support from AstraZeneca and six other companies.
Five-year PARTNER 1 results held up
SAN DIEGO – Five years out, transcatheter aortic valve replacement beat standard therapy in patients with severe, inoperable aortic stenosis, and measured up to surgery in high-risk patients.
The final data from the PARTNER 1 data showed TAVR as an alternative to surgery for some high-risk surgical patients, Dr. Michael Mack reported at the annual scientific sessions of the American College of Cardiology. High-risk surgical patients had similar all-cause mortality, cardiovascular mortality, stroke, and hospital readmission rates, regardless of whether they underwent TAVR or surgical valve replacement, Dr. Mack of Baylor Scott & White Health in Plano, Texas, and his associates wrote in an article published online simultaneously with the presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60308-7]). “Functional outcomes were also similar and preservation of valve hemodynamics was equivalent in both groups,” they wrote.
The trial also showed “a sustained benefit of TAVR” for inoperable aortic stenosis, “as measured by all-cause mortality, cardiovascular mortality, repeat hospital admission, and functional status. Valves were durable, with no increase in transvalvular gradient, attrition of valve area, or worsening of aortic regurgitation,” Dr. Samir Kapadia at the Cleveland Clinic in Ohio and his associates reported in an related article that was not presented at the ACC meeting but was published at the same time as Dr. Mack’s presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60290-2]). Based on the findings, “TAVR should be strongly considered for patients who are not surgical candidates for aortic valve replacement,” the researchers added. “Appropriate selection of patients will help to maximize the benefit of TAVR and reduce mortality from coexisting severe comorbidities.”
The Placement of Aortic Transcatheter Valves (PARTNER 1) trial compared TAVR, standard nonsurgical treatment, and surgery in patients with severe, symptomatic aortic stenosis. The inoperable cohort included 358 patients who averaged 83 years of age. The high-risk cohort enrolled 699 patients whose overall average Society of Thoracic Surgeons (STS) Predicted Risk of Mortality Score was more than 11%. Inoperable patients were randomized to TAVR or standard treatment (usually including balloon aortic valvuloplasty), while high-risk patients were randomized to TAVR or surgical valve replacement.
Five years after treatment, almost 72% of TAVR patients in the inoperable cohort had died, compared with 94% of patients who received standard treatment (hazard ratio, 0.50; 95% confidence interval, 0.39-0.65; P < .0001), Dr. Kapadia and his associates reported. Notably, 86% (or 42 of 49) of surviving TAVR patients had New York Heart Association class 1 or 2 symptoms, compared with only 60% of patients who received standard treatment. Echocardiography did not reveal valve deterioration, the investigators said.
Patients in the high-risk group also faced substantial mortality – only about a third were alive 5 years after TAVR or surgery, Dr. Mack reported. Also, 14% of TAVR patients developed moderate to severe valvular regurgitation, compared with only 1% of the surgery group; P < .0001), and this complication was tied to lower survival, they wrote. “The clinical outcomes and valve performance in this trial might not reflect that of subsequent generations of balloon-expandable transcatheter valves, present operator expertise and experience, and more rigorous patient selection for TAVR,” he cautioned. “The patients selected for treatment in this trial, which started in 2007, are also representative of clinical practice at that time; clinicians have since refined patient selection, at least partly on the basis of early outcomes from this trial.”
Edwards Lifesciences funded the study. Several authors reported receiving travel reimbursements from Edwards Lifesciences and financial or consulting relationships with Abbott Vascular, Edwards Lifesciences, Medtronic, Thubrikar Aortic Valve, St Jude Medical, Philips Healthcare, Sorin Medical, DirectFlow, Boston Scientific, Cardiosolutions, ValvXchange, and Posthorax.
The PARTNER trial was perhaps unique in showing that the first generation of a medical device resulted in a substantial mortality benefit compared with standard treatment. However, some uncertainties remain. The conclusions apply only to appropriately selected patients because many more patients were screened than were enrolled. Other patient populations that might ultimately benefit most from treatment with these new technologies should become better defined over the coming years.
In patients with aortic stenosis who were unsuitable for surgery, transcatheter aortic valve replacement provided a survival benefit of almost 22% [compared with standard treatment]... and a 28% lower cardiovascular mortality. Even more important for elderly patients is quality of life, and 86% of the 49 survivors who received TAVR had New York Heart Association (NYHA) functional class 1 or 2. A benefit of this size is remarkable for inoperable old patients treated with a first-generation medical device. However, a concern is that 48% of the patients undergoing TAVR were readmitted to hospital … and 34% of deaths were noncardiovascular. To treat one disease process, only for another to take its place, is not the objective of an invasive and expensive treatment with complications.
For high-risk patients, the clinical results of TAVR equaled those of SAVR, and the valve showed itself to be durable. The findings challenge whether surgery can still be considered the gold standard for patients at high surgical risk. In 2008, Dr. Mack predicted that the benefits of new, less invasive procedures for percutaneous heart valve treatment would equal or surpass those of their open-surgery predecessors, and concluded that patients will choose a less invasive approach over a more invasive one even if there is uncertainty. With more than 150,000 implantations worldwide and the indication shifting towards intermediate-risk patients, this prediction has been met.
Arie P. Kappetein, M.D., Ph.D., is a cardiothoracic surgeon at Erasmus University in Rotterdam, the Netherlands. These comments were excerpted from his accompanying editorial (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60448-2]).
The PARTNER trial was perhaps unique in showing that the first generation of a medical device resulted in a substantial mortality benefit compared with standard treatment. However, some uncertainties remain. The conclusions apply only to appropriately selected patients because many more patients were screened than were enrolled. Other patient populations that might ultimately benefit most from treatment with these new technologies should become better defined over the coming years.
In patients with aortic stenosis who were unsuitable for surgery, transcatheter aortic valve replacement provided a survival benefit of almost 22% [compared with standard treatment]... and a 28% lower cardiovascular mortality. Even more important for elderly patients is quality of life, and 86% of the 49 survivors who received TAVR had New York Heart Association (NYHA) functional class 1 or 2. A benefit of this size is remarkable for inoperable old patients treated with a first-generation medical device. However, a concern is that 48% of the patients undergoing TAVR were readmitted to hospital … and 34% of deaths were noncardiovascular. To treat one disease process, only for another to take its place, is not the objective of an invasive and expensive treatment with complications.
For high-risk patients, the clinical results of TAVR equaled those of SAVR, and the valve showed itself to be durable. The findings challenge whether surgery can still be considered the gold standard for patients at high surgical risk. In 2008, Dr. Mack predicted that the benefits of new, less invasive procedures for percutaneous heart valve treatment would equal or surpass those of their open-surgery predecessors, and concluded that patients will choose a less invasive approach over a more invasive one even if there is uncertainty. With more than 150,000 implantations worldwide and the indication shifting towards intermediate-risk patients, this prediction has been met.
Arie P. Kappetein, M.D., Ph.D., is a cardiothoracic surgeon at Erasmus University in Rotterdam, the Netherlands. These comments were excerpted from his accompanying editorial (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60448-2]).
The PARTNER trial was perhaps unique in showing that the first generation of a medical device resulted in a substantial mortality benefit compared with standard treatment. However, some uncertainties remain. The conclusions apply only to appropriately selected patients because many more patients were screened than were enrolled. Other patient populations that might ultimately benefit most from treatment with these new technologies should become better defined over the coming years.
In patients with aortic stenosis who were unsuitable for surgery, transcatheter aortic valve replacement provided a survival benefit of almost 22% [compared with standard treatment]... and a 28% lower cardiovascular mortality. Even more important for elderly patients is quality of life, and 86% of the 49 survivors who received TAVR had New York Heart Association (NYHA) functional class 1 or 2. A benefit of this size is remarkable for inoperable old patients treated with a first-generation medical device. However, a concern is that 48% of the patients undergoing TAVR were readmitted to hospital … and 34% of deaths were noncardiovascular. To treat one disease process, only for another to take its place, is not the objective of an invasive and expensive treatment with complications.
For high-risk patients, the clinical results of TAVR equaled those of SAVR, and the valve showed itself to be durable. The findings challenge whether surgery can still be considered the gold standard for patients at high surgical risk. In 2008, Dr. Mack predicted that the benefits of new, less invasive procedures for percutaneous heart valve treatment would equal or surpass those of their open-surgery predecessors, and concluded that patients will choose a less invasive approach over a more invasive one even if there is uncertainty. With more than 150,000 implantations worldwide and the indication shifting towards intermediate-risk patients, this prediction has been met.
Arie P. Kappetein, M.D., Ph.D., is a cardiothoracic surgeon at Erasmus University in Rotterdam, the Netherlands. These comments were excerpted from his accompanying editorial (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60448-2]).
SAN DIEGO – Five years out, transcatheter aortic valve replacement beat standard therapy in patients with severe, inoperable aortic stenosis, and measured up to surgery in high-risk patients.
The final data from the PARTNER 1 data showed TAVR as an alternative to surgery for some high-risk surgical patients, Dr. Michael Mack reported at the annual scientific sessions of the American College of Cardiology. High-risk surgical patients had similar all-cause mortality, cardiovascular mortality, stroke, and hospital readmission rates, regardless of whether they underwent TAVR or surgical valve replacement, Dr. Mack of Baylor Scott & White Health in Plano, Texas, and his associates wrote in an article published online simultaneously with the presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60308-7]). “Functional outcomes were also similar and preservation of valve hemodynamics was equivalent in both groups,” they wrote.
The trial also showed “a sustained benefit of TAVR” for inoperable aortic stenosis, “as measured by all-cause mortality, cardiovascular mortality, repeat hospital admission, and functional status. Valves were durable, with no increase in transvalvular gradient, attrition of valve area, or worsening of aortic regurgitation,” Dr. Samir Kapadia at the Cleveland Clinic in Ohio and his associates reported in an related article that was not presented at the ACC meeting but was published at the same time as Dr. Mack’s presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60290-2]). Based on the findings, “TAVR should be strongly considered for patients who are not surgical candidates for aortic valve replacement,” the researchers added. “Appropriate selection of patients will help to maximize the benefit of TAVR and reduce mortality from coexisting severe comorbidities.”
The Placement of Aortic Transcatheter Valves (PARTNER 1) trial compared TAVR, standard nonsurgical treatment, and surgery in patients with severe, symptomatic aortic stenosis. The inoperable cohort included 358 patients who averaged 83 years of age. The high-risk cohort enrolled 699 patients whose overall average Society of Thoracic Surgeons (STS) Predicted Risk of Mortality Score was more than 11%. Inoperable patients were randomized to TAVR or standard treatment (usually including balloon aortic valvuloplasty), while high-risk patients were randomized to TAVR or surgical valve replacement.
Five years after treatment, almost 72% of TAVR patients in the inoperable cohort had died, compared with 94% of patients who received standard treatment (hazard ratio, 0.50; 95% confidence interval, 0.39-0.65; P < .0001), Dr. Kapadia and his associates reported. Notably, 86% (or 42 of 49) of surviving TAVR patients had New York Heart Association class 1 or 2 symptoms, compared with only 60% of patients who received standard treatment. Echocardiography did not reveal valve deterioration, the investigators said.
Patients in the high-risk group also faced substantial mortality – only about a third were alive 5 years after TAVR or surgery, Dr. Mack reported. Also, 14% of TAVR patients developed moderate to severe valvular regurgitation, compared with only 1% of the surgery group; P < .0001), and this complication was tied to lower survival, they wrote. “The clinical outcomes and valve performance in this trial might not reflect that of subsequent generations of balloon-expandable transcatheter valves, present operator expertise and experience, and more rigorous patient selection for TAVR,” he cautioned. “The patients selected for treatment in this trial, which started in 2007, are also representative of clinical practice at that time; clinicians have since refined patient selection, at least partly on the basis of early outcomes from this trial.”
Edwards Lifesciences funded the study. Several authors reported receiving travel reimbursements from Edwards Lifesciences and financial or consulting relationships with Abbott Vascular, Edwards Lifesciences, Medtronic, Thubrikar Aortic Valve, St Jude Medical, Philips Healthcare, Sorin Medical, DirectFlow, Boston Scientific, Cardiosolutions, ValvXchange, and Posthorax.
SAN DIEGO – Five years out, transcatheter aortic valve replacement beat standard therapy in patients with severe, inoperable aortic stenosis, and measured up to surgery in high-risk patients.
The final data from the PARTNER 1 data showed TAVR as an alternative to surgery for some high-risk surgical patients, Dr. Michael Mack reported at the annual scientific sessions of the American College of Cardiology. High-risk surgical patients had similar all-cause mortality, cardiovascular mortality, stroke, and hospital readmission rates, regardless of whether they underwent TAVR or surgical valve replacement, Dr. Mack of Baylor Scott & White Health in Plano, Texas, and his associates wrote in an article published online simultaneously with the presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60308-7]). “Functional outcomes were also similar and preservation of valve hemodynamics was equivalent in both groups,” they wrote.
The trial also showed “a sustained benefit of TAVR” for inoperable aortic stenosis, “as measured by all-cause mortality, cardiovascular mortality, repeat hospital admission, and functional status. Valves were durable, with no increase in transvalvular gradient, attrition of valve area, or worsening of aortic regurgitation,” Dr. Samir Kapadia at the Cleveland Clinic in Ohio and his associates reported in an related article that was not presented at the ACC meeting but was published at the same time as Dr. Mack’s presentation (Lancet 2015 Mar. 15 [doi: 10.1016/ S0140-6736(15)60290-2]). Based on the findings, “TAVR should be strongly considered for patients who are not surgical candidates for aortic valve replacement,” the researchers added. “Appropriate selection of patients will help to maximize the benefit of TAVR and reduce mortality from coexisting severe comorbidities.”
The Placement of Aortic Transcatheter Valves (PARTNER 1) trial compared TAVR, standard nonsurgical treatment, and surgery in patients with severe, symptomatic aortic stenosis. The inoperable cohort included 358 patients who averaged 83 years of age. The high-risk cohort enrolled 699 patients whose overall average Society of Thoracic Surgeons (STS) Predicted Risk of Mortality Score was more than 11%. Inoperable patients were randomized to TAVR or standard treatment (usually including balloon aortic valvuloplasty), while high-risk patients were randomized to TAVR or surgical valve replacement.
Five years after treatment, almost 72% of TAVR patients in the inoperable cohort had died, compared with 94% of patients who received standard treatment (hazard ratio, 0.50; 95% confidence interval, 0.39-0.65; P < .0001), Dr. Kapadia and his associates reported. Notably, 86% (or 42 of 49) of surviving TAVR patients had New York Heart Association class 1 or 2 symptoms, compared with only 60% of patients who received standard treatment. Echocardiography did not reveal valve deterioration, the investigators said.
Patients in the high-risk group also faced substantial mortality – only about a third were alive 5 years after TAVR or surgery, Dr. Mack reported. Also, 14% of TAVR patients developed moderate to severe valvular regurgitation, compared with only 1% of the surgery group; P < .0001), and this complication was tied to lower survival, they wrote. “The clinical outcomes and valve performance in this trial might not reflect that of subsequent generations of balloon-expandable transcatheter valves, present operator expertise and experience, and more rigorous patient selection for TAVR,” he cautioned. “The patients selected for treatment in this trial, which started in 2007, are also representative of clinical practice at that time; clinicians have since refined patient selection, at least partly on the basis of early outcomes from this trial.”
Edwards Lifesciences funded the study. Several authors reported receiving travel reimbursements from Edwards Lifesciences and financial or consulting relationships with Abbott Vascular, Edwards Lifesciences, Medtronic, Thubrikar Aortic Valve, St Jude Medical, Philips Healthcare, Sorin Medical, DirectFlow, Boston Scientific, Cardiosolutions, ValvXchange, and Posthorax.
Key clinical point:Transcatheter aortic valve replacement is an acceptable alternative to standard treatment in some patients with aortic stenosis.
Major finding:For inoperable patients, TAVR had lower five-year mortality than did standard therapy (P < .0001). For high-risk patients, TAVR and surgical mortality rates were similar.
Data source: Five-year data from the randomized Placement of Aortic Transcatheter Valves (PARTNER 1) trial.
Disclosures: Edwards Lifesciences funded the study. Several authors reported receiving travel reimbursements from Edwards Lifesciences and financial or consulting relationships with Abbott Vascular, Edwards Lifesciences, Medtronic, Thubrikar Aortic Valve, St Jude Medical, Philips Healthcare, Sorin Medical, DirectFlow, Boston Scientific, Cardiosolutions, ValvXchange, and Posthorax.
MI survivors face higher cancer risk
SAN DIEGO– The risk of developing cancer is significantly higher in survivors of an acute MI compared to the general population, according to a large Danish national registry study.
“Greater focus on long-term cancer risk is warranted in MI survivors. This could potentially have implications on future patient care for MI patients, outpatient follow-up strategies, and distribution of health care resources,” Morten Winther Malmborg said at the annual meeting of the American College of Cardiology.
He presented a nationwide cohort study including 3,005,734 Danish adults with no baseline history of MI or cancer who were followed for up to 17 years in the comprehensive Danish National Patient Registry. During the study period, 125,926 of these individuals had a nonfatal MI.
The subsequent incidence of cancer in the MI survivors was 167 cases per 10,000 person-years compared with 95 per 10,000 person-years in the control group, reported Mr. Malmborg, a fourth-year medical student at the University of Copenhagen.
Cancer diagnoses of all types were highest by far in the first 6 months post-MI, which he attributed to surveillance bias, since that was a period of increased medical contact. However, after he and his coinvestigators excluded the cancers diagnosed during that initial 6-month period, the post-MI group still had a highly significant 11% increased relative risk for cancer overall during the period from 6 months through 17 years post-MI.
The younger a patient was when the MI occurred, the greater the subsequent cancer risk. Individuals who had a nonfatal MI at age 30-54 had a 44% greater risk of cancer overall at 6 months–17 years post-MI compared, with the control group. Those who had an MI at age 55-69 had a 19% increased cancer risk compared to controls, while those whose MI occurred at age 70-99 had a modest but still statistically significant 5% increase in cancer risk.
Particularly striking, according to Mr. Malmborg, was the MI survivors’ 44% increased relative risk for lung cancer and 31% increase in bladder cancer during the period from 6 months–17 years post-MI compared with the general population. In contrast, rates of breast, prostate, and colon cancer weren’t significantly different between MI survivors and the general population with no history of MI.
This observational study didn’t address the mechanisms involved in MI survivors’ increased cancer risk. Although the Danish registry didn’t include information of smoking status, Mr. Malmborg speculated that smoking may figure prominently, since it is a major shared risk factor for cardiovascular disease as well as lung and bladder cancer in particular. Other shared risk factors for cardiovascular disease and cancer include obesity, sedentary lifestyle, and excessive alcohol use.
This is the first large-scale study to look at cancer risk post-MI. It’s an increasingly relevant issue because the advances in cardiac care that have brought improved long-term survival following acute MI means more patients with a history of MI are likely to die from noncardiac causes, Mr. Malmborg observed.
He and his coinvestigators are now performing a number-needed-to-screen analysis to help them determine whether structured, formal creening for cancer following an MI should be done routinely.
The study was supported by Danish national medical research funds. The presenter reported having no financial conflicts.
SAN DIEGO– The risk of developing cancer is significantly higher in survivors of an acute MI compared to the general population, according to a large Danish national registry study.
“Greater focus on long-term cancer risk is warranted in MI survivors. This could potentially have implications on future patient care for MI patients, outpatient follow-up strategies, and distribution of health care resources,” Morten Winther Malmborg said at the annual meeting of the American College of Cardiology.
He presented a nationwide cohort study including 3,005,734 Danish adults with no baseline history of MI or cancer who were followed for up to 17 years in the comprehensive Danish National Patient Registry. During the study period, 125,926 of these individuals had a nonfatal MI.
The subsequent incidence of cancer in the MI survivors was 167 cases per 10,000 person-years compared with 95 per 10,000 person-years in the control group, reported Mr. Malmborg, a fourth-year medical student at the University of Copenhagen.
Cancer diagnoses of all types were highest by far in the first 6 months post-MI, which he attributed to surveillance bias, since that was a period of increased medical contact. However, after he and his coinvestigators excluded the cancers diagnosed during that initial 6-month period, the post-MI group still had a highly significant 11% increased relative risk for cancer overall during the period from 6 months through 17 years post-MI.
The younger a patient was when the MI occurred, the greater the subsequent cancer risk. Individuals who had a nonfatal MI at age 30-54 had a 44% greater risk of cancer overall at 6 months–17 years post-MI compared, with the control group. Those who had an MI at age 55-69 had a 19% increased cancer risk compared to controls, while those whose MI occurred at age 70-99 had a modest but still statistically significant 5% increase in cancer risk.
Particularly striking, according to Mr. Malmborg, was the MI survivors’ 44% increased relative risk for lung cancer and 31% increase in bladder cancer during the period from 6 months–17 years post-MI compared with the general population. In contrast, rates of breast, prostate, and colon cancer weren’t significantly different between MI survivors and the general population with no history of MI.
This observational study didn’t address the mechanisms involved in MI survivors’ increased cancer risk. Although the Danish registry didn’t include information of smoking status, Mr. Malmborg speculated that smoking may figure prominently, since it is a major shared risk factor for cardiovascular disease as well as lung and bladder cancer in particular. Other shared risk factors for cardiovascular disease and cancer include obesity, sedentary lifestyle, and excessive alcohol use.
This is the first large-scale study to look at cancer risk post-MI. It’s an increasingly relevant issue because the advances in cardiac care that have brought improved long-term survival following acute MI means more patients with a history of MI are likely to die from noncardiac causes, Mr. Malmborg observed.
He and his coinvestigators are now performing a number-needed-to-screen analysis to help them determine whether structured, formal creening for cancer following an MI should be done routinely.
The study was supported by Danish national medical research funds. The presenter reported having no financial conflicts.
SAN DIEGO– The risk of developing cancer is significantly higher in survivors of an acute MI compared to the general population, according to a large Danish national registry study.
“Greater focus on long-term cancer risk is warranted in MI survivors. This could potentially have implications on future patient care for MI patients, outpatient follow-up strategies, and distribution of health care resources,” Morten Winther Malmborg said at the annual meeting of the American College of Cardiology.
He presented a nationwide cohort study including 3,005,734 Danish adults with no baseline history of MI or cancer who were followed for up to 17 years in the comprehensive Danish National Patient Registry. During the study period, 125,926 of these individuals had a nonfatal MI.
The subsequent incidence of cancer in the MI survivors was 167 cases per 10,000 person-years compared with 95 per 10,000 person-years in the control group, reported Mr. Malmborg, a fourth-year medical student at the University of Copenhagen.
Cancer diagnoses of all types were highest by far in the first 6 months post-MI, which he attributed to surveillance bias, since that was a period of increased medical contact. However, after he and his coinvestigators excluded the cancers diagnosed during that initial 6-month period, the post-MI group still had a highly significant 11% increased relative risk for cancer overall during the period from 6 months through 17 years post-MI.
The younger a patient was when the MI occurred, the greater the subsequent cancer risk. Individuals who had a nonfatal MI at age 30-54 had a 44% greater risk of cancer overall at 6 months–17 years post-MI compared, with the control group. Those who had an MI at age 55-69 had a 19% increased cancer risk compared to controls, while those whose MI occurred at age 70-99 had a modest but still statistically significant 5% increase in cancer risk.
Particularly striking, according to Mr. Malmborg, was the MI survivors’ 44% increased relative risk for lung cancer and 31% increase in bladder cancer during the period from 6 months–17 years post-MI compared with the general population. In contrast, rates of breast, prostate, and colon cancer weren’t significantly different between MI survivors and the general population with no history of MI.
This observational study didn’t address the mechanisms involved in MI survivors’ increased cancer risk. Although the Danish registry didn’t include information of smoking status, Mr. Malmborg speculated that smoking may figure prominently, since it is a major shared risk factor for cardiovascular disease as well as lung and bladder cancer in particular. Other shared risk factors for cardiovascular disease and cancer include obesity, sedentary lifestyle, and excessive alcohol use.
This is the first large-scale study to look at cancer risk post-MI. It’s an increasingly relevant issue because the advances in cardiac care that have brought improved long-term survival following acute MI means more patients with a history of MI are likely to die from noncardiac causes, Mr. Malmborg observed.
He and his coinvestigators are now performing a number-needed-to-screen analysis to help them determine whether structured, formal creening for cancer following an MI should be done routinely.
The study was supported by Danish national medical research funds. The presenter reported having no financial conflicts.
AT ACC 15
Key clinical point: Closer monitoring for development of cancer in MI survivors may be warranted.
Major finding: The incidence of cancer overall was 167 cases per 10,000 person-years in acute MI survivors, compared with 95 per 10,000 person-years in the general population without a history of MI or prior cancer.
Data source: An observational study of more than 3 million adults enrolled in the Danish National Patient Registry, roughly 126,000 of whom were diagnosed with a first nonfatal MI during the study period.
Disclosures: The study was supported by Danish national medical research funds. The presenter reported having no financial conflicts.
VIDEO: Growing evidence supports prolonged DAPT for ACS
SAN DIEGO – Current guidelines call for treating acute coronary syndrome patients with dual antiplatelet therapy (aspirin plus a thienopyridine) for at least 1 year following their event, but results from recent large, randomized trials suggest that many patients continue to benefit from treatment that extends beyond the first year, Dr. Richard C. Becker said during an interview at the annual meeting of the American College of Cardiology.
New results reported at the meeting from the PEGASUS-TIMI (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction) 54 trial highlight the long-term risk for ischemic events faced by patients following an acute coronary syndrome (N. Engl. J. Med. 2025;[doi: 10.1056/NEJMoa0904327]. The results also underscore the importance of risk assessment, and the importance of tailoring treatment to ACS patients based not only on their long-term risk from their cardiovascular disease but also their risk for adverse bleeding events secondary to prolonged, aggressive antiplatelet therapy. The PEGASUS-TIMI 54 results complement the findings reported last year from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66), he said.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
Based on the accumulated evidence, ACS patients who have done well clinically on DAPT after 1 year and are deemed at low risk for bleeding and other complications are good candidates for more prolonged DAPT treatment, said Dr. Becker, professor and director of the University of Cincinnati Heart, Lung & Vascular Institute.
PEGASUS-TIMI 54 ws sponsored by AstraZeneca, which markets ticagrelor (Brilinta). Dr. Becker has been a consultant to and received research support from AstraZeneca.
On Twitter @mitchelzoler
SAN DIEGO – Current guidelines call for treating acute coronary syndrome patients with dual antiplatelet therapy (aspirin plus a thienopyridine) for at least 1 year following their event, but results from recent large, randomized trials suggest that many patients continue to benefit from treatment that extends beyond the first year, Dr. Richard C. Becker said during an interview at the annual meeting of the American College of Cardiology.
New results reported at the meeting from the PEGASUS-TIMI (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction) 54 trial highlight the long-term risk for ischemic events faced by patients following an acute coronary syndrome (N. Engl. J. Med. 2025;[doi: 10.1056/NEJMoa0904327]. The results also underscore the importance of risk assessment, and the importance of tailoring treatment to ACS patients based not only on their long-term risk from their cardiovascular disease but also their risk for adverse bleeding events secondary to prolonged, aggressive antiplatelet therapy. The PEGASUS-TIMI 54 results complement the findings reported last year from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66), he said.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
Based on the accumulated evidence, ACS patients who have done well clinically on DAPT after 1 year and are deemed at low risk for bleeding and other complications are good candidates for more prolonged DAPT treatment, said Dr. Becker, professor and director of the University of Cincinnati Heart, Lung & Vascular Institute.
PEGASUS-TIMI 54 ws sponsored by AstraZeneca, which markets ticagrelor (Brilinta). Dr. Becker has been a consultant to and received research support from AstraZeneca.
On Twitter @mitchelzoler
SAN DIEGO – Current guidelines call for treating acute coronary syndrome patients with dual antiplatelet therapy (aspirin plus a thienopyridine) for at least 1 year following their event, but results from recent large, randomized trials suggest that many patients continue to benefit from treatment that extends beyond the first year, Dr. Richard C. Becker said during an interview at the annual meeting of the American College of Cardiology.
New results reported at the meeting from the PEGASUS-TIMI (Prevention of Cardiovascular Events in Patients with Prior Heart Attack Using Ticagrelor Compared to Placebo on a Background of Aspirin-Thrombolysis in Myocardial Infarction) 54 trial highlight the long-term risk for ischemic events faced by patients following an acute coronary syndrome (N. Engl. J. Med. 2025;[doi: 10.1056/NEJMoa0904327]. The results also underscore the importance of risk assessment, and the importance of tailoring treatment to ACS patients based not only on their long-term risk from their cardiovascular disease but also their risk for adverse bleeding events secondary to prolonged, aggressive antiplatelet therapy. The PEGASUS-TIMI 54 results complement the findings reported last year from the DAPT (Dual Antiplatelet Therapy) trial (N. Engl. J. Med. 2014;371:2155-66), he said.
The video associated with this article is no longer available on this site. Please view all of our videos on the MDedge YouTube channel
Based on the accumulated evidence, ACS patients who have done well clinically on DAPT after 1 year and are deemed at low risk for bleeding and other complications are good candidates for more prolonged DAPT treatment, said Dr. Becker, professor and director of the University of Cincinnati Heart, Lung & Vascular Institute.
PEGASUS-TIMI 54 ws sponsored by AstraZeneca, which markets ticagrelor (Brilinta). Dr. Becker has been a consultant to and received research support from AstraZeneca.
On Twitter @mitchelzoler
AT ACC 15
CT scans comparable to functional testing for CAD
SAN DIEGO – Initial anatomic testing with CT angiography yielded similar clinical outcomes to functional testing in chest pain patients evaluated for coronary artery disease in the PROMISE study.
After an average of 25 months, the primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications occurred in 3.3% of the CTA patients and 3.0% of the functional-testing patients (adjusted hazard ratio, 1.04; P = .75).
The CTA strategy may offer a slight advantage, however, in terms of fewer invasive catheterizations without evidence of obstructive coronary artery disease (3.4% vs. 4.3%; P = .022) and a higher proportion of catheterizations with obstructive CAD (72.1% vs. 47.5%) getting revascularization (6.2% vs. 3.2%) or coronary artery bypass grafting (72 events vs. 38 events).
“Our results suggest that CTA is a viable alternative to functional testing. These real-world results should inform noninvasive testing choices in clinical care as well as provide guidance to future studies of diagnostic strategies in suspected heart disease,” lead study author Dr. Pamela Douglas reported at the annual meeting of the American College of Cardiology and simultaneously published online (N. Engl. J. Med. 2015 [DOI:10.1056/NEJoa1415516].
PROMISE (Prospective Multicenter Imaging Study for the Evaluation of Chest Pain) enrolled 10,003 symptomatic outpatients requiring nonemergent, noninvasive testing for suspected CAD who were older than 54 years for men or older than 64 years for women with no risk factors, or aged 45-54 years for men and 50-64 years for women with at least one cardiac risk factor.
Patients were randomly assigned to anatomical testing with CTA or functional testing including a nuclear stress test (67%), stress echocardiography (23%), or exercise electrocardiogram (10%). The patients had an average of 2.5 risk cardiovascular risk factors and half were women.
Radiation exposure was higher overall in the CTA group than the functional-testing group (mean 12.0 mSv vs. 10.1 mSv; P < .001), largely because 33% of the functional group had no exposure. Exposure was lower, however, in CTA patients compared with those for whom a nuclear test was specified at randomization as their first intended functional test (12.0 mSv vs. 14.1 mSv; P < .001), Dr. Douglas, from Duke Clinical Research Institute in Durham, N.C., said.
During a discussion of the results, Dr. Elliott Antman, associate dean for clinical and translational research at Harvard University, Boston, said CT angiography can’t officially be described as noninferior to functional testing because PROMISE was designed as a superiority trial with a noninferiority margin that was exceeded by the confidence intervals for the primary end point and questioned how clinicians should use the results.
“What I can say to the next patient is that they can be incredibly assured about their overall prognosis, which is a nontrivial thing to say that they have a very, very low likelihood of a bad event in the next 2 years no matter what we do,” Dr. Douglas responded. “I can offer a test choice that will have no difference in major health events like death or nonfatal MI, but I can offer a test that potentially has lower radiation and has a better triage function to the cath lab where you have less likelihood of ending up in the cath lab not needing to be there because you do not have obstructive disease.”
Though PROMISE may influence practice, it is unclear whether the noninferiority issue will impact its ability to change U.S. guidelines, which currently include a IIb recommendation that CTA be considered in the evaluation of patients with chest pain.
“Technically two randomized controlled trials are needed before you get evidence level A, but we have 10,000 patients who were well studied here, so I would anticipate a big change actually in the guidelines from a use criteria, but we shall see,” Dr. Douglas said.
SAN DIEGO – Initial anatomic testing with CT angiography yielded similar clinical outcomes to functional testing in chest pain patients evaluated for coronary artery disease in the PROMISE study.
After an average of 25 months, the primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications occurred in 3.3% of the CTA patients and 3.0% of the functional-testing patients (adjusted hazard ratio, 1.04; P = .75).
The CTA strategy may offer a slight advantage, however, in terms of fewer invasive catheterizations without evidence of obstructive coronary artery disease (3.4% vs. 4.3%; P = .022) and a higher proportion of catheterizations with obstructive CAD (72.1% vs. 47.5%) getting revascularization (6.2% vs. 3.2%) or coronary artery bypass grafting (72 events vs. 38 events).
“Our results suggest that CTA is a viable alternative to functional testing. These real-world results should inform noninvasive testing choices in clinical care as well as provide guidance to future studies of diagnostic strategies in suspected heart disease,” lead study author Dr. Pamela Douglas reported at the annual meeting of the American College of Cardiology and simultaneously published online (N. Engl. J. Med. 2015 [DOI:10.1056/NEJoa1415516].
PROMISE (Prospective Multicenter Imaging Study for the Evaluation of Chest Pain) enrolled 10,003 symptomatic outpatients requiring nonemergent, noninvasive testing for suspected CAD who were older than 54 years for men or older than 64 years for women with no risk factors, or aged 45-54 years for men and 50-64 years for women with at least one cardiac risk factor.
Patients were randomly assigned to anatomical testing with CTA or functional testing including a nuclear stress test (67%), stress echocardiography (23%), or exercise electrocardiogram (10%). The patients had an average of 2.5 risk cardiovascular risk factors and half were women.
Radiation exposure was higher overall in the CTA group than the functional-testing group (mean 12.0 mSv vs. 10.1 mSv; P < .001), largely because 33% of the functional group had no exposure. Exposure was lower, however, in CTA patients compared with those for whom a nuclear test was specified at randomization as their first intended functional test (12.0 mSv vs. 14.1 mSv; P < .001), Dr. Douglas, from Duke Clinical Research Institute in Durham, N.C., said.
During a discussion of the results, Dr. Elliott Antman, associate dean for clinical and translational research at Harvard University, Boston, said CT angiography can’t officially be described as noninferior to functional testing because PROMISE was designed as a superiority trial with a noninferiority margin that was exceeded by the confidence intervals for the primary end point and questioned how clinicians should use the results.
“What I can say to the next patient is that they can be incredibly assured about their overall prognosis, which is a nontrivial thing to say that they have a very, very low likelihood of a bad event in the next 2 years no matter what we do,” Dr. Douglas responded. “I can offer a test choice that will have no difference in major health events like death or nonfatal MI, but I can offer a test that potentially has lower radiation and has a better triage function to the cath lab where you have less likelihood of ending up in the cath lab not needing to be there because you do not have obstructive disease.”
Though PROMISE may influence practice, it is unclear whether the noninferiority issue will impact its ability to change U.S. guidelines, which currently include a IIb recommendation that CTA be considered in the evaluation of patients with chest pain.
“Technically two randomized controlled trials are needed before you get evidence level A, but we have 10,000 patients who were well studied here, so I would anticipate a big change actually in the guidelines from a use criteria, but we shall see,” Dr. Douglas said.
SAN DIEGO – Initial anatomic testing with CT angiography yielded similar clinical outcomes to functional testing in chest pain patients evaluated for coronary artery disease in the PROMISE study.
After an average of 25 months, the primary composite end point of all-cause death, nonfatal myocardial infarction, unstable angina hospitalization, and major cardiovascular procedural complications occurred in 3.3% of the CTA patients and 3.0% of the functional-testing patients (adjusted hazard ratio, 1.04; P = .75).
The CTA strategy may offer a slight advantage, however, in terms of fewer invasive catheterizations without evidence of obstructive coronary artery disease (3.4% vs. 4.3%; P = .022) and a higher proportion of catheterizations with obstructive CAD (72.1% vs. 47.5%) getting revascularization (6.2% vs. 3.2%) or coronary artery bypass grafting (72 events vs. 38 events).
“Our results suggest that CTA is a viable alternative to functional testing. These real-world results should inform noninvasive testing choices in clinical care as well as provide guidance to future studies of diagnostic strategies in suspected heart disease,” lead study author Dr. Pamela Douglas reported at the annual meeting of the American College of Cardiology and simultaneously published online (N. Engl. J. Med. 2015 [DOI:10.1056/NEJoa1415516].
PROMISE (Prospective Multicenter Imaging Study for the Evaluation of Chest Pain) enrolled 10,003 symptomatic outpatients requiring nonemergent, noninvasive testing for suspected CAD who were older than 54 years for men or older than 64 years for women with no risk factors, or aged 45-54 years for men and 50-64 years for women with at least one cardiac risk factor.
Patients were randomly assigned to anatomical testing with CTA or functional testing including a nuclear stress test (67%), stress echocardiography (23%), or exercise electrocardiogram (10%). The patients had an average of 2.5 risk cardiovascular risk factors and half were women.
Radiation exposure was higher overall in the CTA group than the functional-testing group (mean 12.0 mSv vs. 10.1 mSv; P < .001), largely because 33% of the functional group had no exposure. Exposure was lower, however, in CTA patients compared with those for whom a nuclear test was specified at randomization as their first intended functional test (12.0 mSv vs. 14.1 mSv; P < .001), Dr. Douglas, from Duke Clinical Research Institute in Durham, N.C., said.
During a discussion of the results, Dr. Elliott Antman, associate dean for clinical and translational research at Harvard University, Boston, said CT angiography can’t officially be described as noninferior to functional testing because PROMISE was designed as a superiority trial with a noninferiority margin that was exceeded by the confidence intervals for the primary end point and questioned how clinicians should use the results.
“What I can say to the next patient is that they can be incredibly assured about their overall prognosis, which is a nontrivial thing to say that they have a very, very low likelihood of a bad event in the next 2 years no matter what we do,” Dr. Douglas responded. “I can offer a test choice that will have no difference in major health events like death or nonfatal MI, but I can offer a test that potentially has lower radiation and has a better triage function to the cath lab where you have less likelihood of ending up in the cath lab not needing to be there because you do not have obstructive disease.”
Though PROMISE may influence practice, it is unclear whether the noninferiority issue will impact its ability to change U.S. guidelines, which currently include a IIb recommendation that CTA be considered in the evaluation of patients with chest pain.
“Technically two randomized controlled trials are needed before you get evidence level A, but we have 10,000 patients who were well studied here, so I would anticipate a big change actually in the guidelines from a use criteria, but we shall see,” Dr. Douglas said.
AT ACC 2015
Key clinical point: Clinical outcomes are comparable with CT angiography and functional testing for suspected coronary artery disease in symptomatic patients.
Major finding: The primary end point occurred in 3.3% of the CTA group and 3.0% of the functional testing group (HR, 1.04; P = .75).
Data source: Prospective, randomized study in 10,003 symptomatic patients with suspected coronary artery disease.
Disclosures: The study was funded by the National Heart, Lung, and Blood Institute. Dr. Douglas reported numerous conflicts. Dr. Antman reported no financial disclosures.