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SAN FRANCISCO – A host of novel clinical and serologic findings that physicians can put to good use right now in helping to distinguish early SLE from its many mimickers have been identified in a large study conducted on four continents, Marta Mosca, MD, PhD, observed at an international congress on systemic lupus erythematosus.
These useful findings aren’t incorporated into the current American College of Rheumatology (ACR) or Systemic Lupus International Collaborating Clinics (SLICC) lupus classification criteria, which have come under criticism for limited sensitivity in identifying early SLE. Some of the novel findings provide support for increased suspicion of early SLE, while others suggest a need to veer in another direction and assess a patient for a disease other than lupus. The study has served to provide input for the proposed new ACR/EULAR weighted SLE classification criteria, although that scheme is meant to be used only for research and not in clinical practice, explained Dr. Mosca of the University of Pisa (Italy).
She was lead author of the four-continent study, which included 616 patients referred to experienced academic lupus centers for possible SLE with a symptom duration of less than 1 year. During up to 3 years of follow-up, 389 patients were diagnosed as having SLE by experienced rheumatologists based upon their clinical judgment, without any requirement to meet the full ACR or SLICC classification criteria. The other 227 patients were determined to be SLE mimickers with conditions including lymphoma, Sjögren’s syndrome, systemic sclerosis, interstitial lung disease, fibromyalgia, antinuclear antibody–positive thyroiditis, and undifferentiated connective tissue disease.
Dr. Mosca also highlighted key recent work by other investigators aimed at speeding the diagnosis of SLE and shortening the duration of what she called “the gray zone” of diagnostic uncertainty, when autoantibodies and insidious symptoms are present but not yet sufficient to make the diagnosis of SLE by conventional criteria. It’s well established that 60%-70% of patients with mild undifferentiated connective tissue disease will remain stable without evolving into SLE during long years of follow-up.
The ultimate objective of all this work is to try to change the natural history of the disease through targeted early aggressive therapy aimed at minimizing the extent of active disease and preventing severe organ involvement.
Among the key takeaways from the four-continent study led by Dr. Mosca: Fever not related to infection was far more prevalent in early SLE than in mimicking conditions, by a margin of 34.5% versus 13.7%. On the other hand, Raynaud’s phenomenon was more than twice as prevalent among patients with mimicking conditions: 22.1% in early SLE, compared with 48.5% in SLE mimickers. Sicca symptoms were present in just 4.4% of early SLE patients versus 34.4% of SLE mimickers. Only 0.3% of early SLE patients complained of dysphagia; the rate was 20-fold higher in the SLE mimickers. Rashes atypical for lupus were twice as frequent in the SLE mimicking conditions (Arthritis Rheumatol. 2019 Jan;71[1]:91-8).
Turning to key differentiating serologic findings, Dr. Mosca noted that anti-double stranded DNA (anti-dsDNA) and anti-Sm antibodies were present in 71.7% and 30.2% of early SLE patients, respectively, compared with 6.9% and 2.6% of SLE mimickers. Anticardiolipin IgM, a positive Coombs test, anti-beta2 glycoprotein-I antibodies, leukopenia, autoimmune hemolytic anemia, and hypocomplementemia were all significantly more common in the early SLE cohort.
In contrast, antibodies to Ro (SS-A) and La (SS-B) were of no value in separating early SLE from its mimickers, according to Dr. Mosca.
Other tipoffs to early SLE
Two separate teams of British researchers have advanced the field in a highly practical way. One group showed in a study of 1,739 newly diagnosed SLE patients and 6,956 controls that in the 5 years prior to diagnosis, the SLE group averaged 9.2 primary care visits per year, compared with 3.8 for controls. The visits clustered around nonspecific complaints of arthritis and arthralgias, alopecia, and rash (Arthritis Care Res. 2017 Jun;69[6]:833-41).
“An accumulating number of primary care office visits and referrals over time should raise suspicion,” Dr. Mosca said.
Other investigators, working with 1,426 cases of newly diagnosed SLE in the U.K. Clinical Practice Research Database, observed that the proportion of patients with disease manifestations in three or more British Isles Lupus Activity Group (BILAG) symptom domains rose from 18.7% at 3 years prior to diagnosis to 39.7% in the year before diagnosis (Lupus Sci Med. 2017 Feb 10;4[1]:e000172. doi: 10.1136/lupus-2016-000172).
“These patients accrue clinical manifestations. It’s not just one symptom, it’s more of a state of being unwell. This is a suspicious factor for the development of lupus,” she continued.
And just as patients who will eventually be diagnosed with SLE accrue a growing number of signs and symptoms during the run up to diagnosis, they also accrue multiple autoantibodies. Moreover, as demonstrated by a multicenter group of U.S. investigators, patients also develop elevated levels of multiple soluble inflammatory markers more than 3.5 years prior to diagnosis of SLE. These include interleukins-5 and -6 and interferon-gamma. And less than 10 months prior to being classified as having SLE, patients develop significantly higher levels of B lymphocyte stimulator (BLyS) and a proliferation-inducing ligand known as APRIL. The investigators developed a predictive model incorporating IL-5, -6, and interferon-gamma levels with antinuclear antibody status that identified future SLE patients with 84% accuracy more than 3.5 years before diagnosis. This could prove useful in selecting high-risk patients for clinical prevention trials (J Autoimmun. 2016 Nov;74:182-93).
Researchers at the University of Leeds (England) have also zeroed in on interferon activity as playing a key role in progression from asymptomatic antinuclear antigen positivity, which is present in up to 25% of the general population, to symptomatic autoimmune connective tissue disease, which affects less than 1%. A multivariate logistic regression analysis identified two independent predictors of development of autoimmune connective tissue disease within the next 12 months: a family history of autoimmune rheumatic disease, which was associated with an 8.2-fold increased risk; and positivity for a pattern of interferon-stimulated gene activity they call IFN-Score-B (Ann Rheum Dis. 2018 Oct;77[10]:1432-9).
All of this work has led up to what Dr. Mosca called “a glance into the future”: the National Institutes of Health–supported Study of Anti-Malarials in Incomplete Lupus Erythematosus (SMILE), which is now recruiting patients. This randomized, double-blind, placebo-controlled multicenter U.S. trial involves patients who are antinuclear antibody positive at a titer of 1:80 or more plus one or two additional criteria from the SLICC classification scheme. Participants are being randomized to 96 weeks of hydroxychloroquine or placebo. The goal is to learn whether hydroxychloroquine can slow disease progression, with the primary endpoint being the number of SLICC criteria met at the study’s end. The trial will also scrutinize potential biomarkers that could be used to guide treatment decisions (Trials. 2018 Dec 20;19[1]:694. doi: 10.1186/s13063-018-3076-7).
Dr. Mosca reported serving as an adviser to UCB and Lilly.
SAN FRANCISCO – A host of novel clinical and serologic findings that physicians can put to good use right now in helping to distinguish early SLE from its many mimickers have been identified in a large study conducted on four continents, Marta Mosca, MD, PhD, observed at an international congress on systemic lupus erythematosus.
These useful findings aren’t incorporated into the current American College of Rheumatology (ACR) or Systemic Lupus International Collaborating Clinics (SLICC) lupus classification criteria, which have come under criticism for limited sensitivity in identifying early SLE. Some of the novel findings provide support for increased suspicion of early SLE, while others suggest a need to veer in another direction and assess a patient for a disease other than lupus. The study has served to provide input for the proposed new ACR/EULAR weighted SLE classification criteria, although that scheme is meant to be used only for research and not in clinical practice, explained Dr. Mosca of the University of Pisa (Italy).
She was lead author of the four-continent study, which included 616 patients referred to experienced academic lupus centers for possible SLE with a symptom duration of less than 1 year. During up to 3 years of follow-up, 389 patients were diagnosed as having SLE by experienced rheumatologists based upon their clinical judgment, without any requirement to meet the full ACR or SLICC classification criteria. The other 227 patients were determined to be SLE mimickers with conditions including lymphoma, Sjögren’s syndrome, systemic sclerosis, interstitial lung disease, fibromyalgia, antinuclear antibody–positive thyroiditis, and undifferentiated connective tissue disease.
Dr. Mosca also highlighted key recent work by other investigators aimed at speeding the diagnosis of SLE and shortening the duration of what she called “the gray zone” of diagnostic uncertainty, when autoantibodies and insidious symptoms are present but not yet sufficient to make the diagnosis of SLE by conventional criteria. It’s well established that 60%-70% of patients with mild undifferentiated connective tissue disease will remain stable without evolving into SLE during long years of follow-up.
The ultimate objective of all this work is to try to change the natural history of the disease through targeted early aggressive therapy aimed at minimizing the extent of active disease and preventing severe organ involvement.
Among the key takeaways from the four-continent study led by Dr. Mosca: Fever not related to infection was far more prevalent in early SLE than in mimicking conditions, by a margin of 34.5% versus 13.7%. On the other hand, Raynaud’s phenomenon was more than twice as prevalent among patients with mimicking conditions: 22.1% in early SLE, compared with 48.5% in SLE mimickers. Sicca symptoms were present in just 4.4% of early SLE patients versus 34.4% of SLE mimickers. Only 0.3% of early SLE patients complained of dysphagia; the rate was 20-fold higher in the SLE mimickers. Rashes atypical for lupus were twice as frequent in the SLE mimicking conditions (Arthritis Rheumatol. 2019 Jan;71[1]:91-8).
Turning to key differentiating serologic findings, Dr. Mosca noted that anti-double stranded DNA (anti-dsDNA) and anti-Sm antibodies were present in 71.7% and 30.2% of early SLE patients, respectively, compared with 6.9% and 2.6% of SLE mimickers. Anticardiolipin IgM, a positive Coombs test, anti-beta2 glycoprotein-I antibodies, leukopenia, autoimmune hemolytic anemia, and hypocomplementemia were all significantly more common in the early SLE cohort.
In contrast, antibodies to Ro (SS-A) and La (SS-B) were of no value in separating early SLE from its mimickers, according to Dr. Mosca.
Other tipoffs to early SLE
Two separate teams of British researchers have advanced the field in a highly practical way. One group showed in a study of 1,739 newly diagnosed SLE patients and 6,956 controls that in the 5 years prior to diagnosis, the SLE group averaged 9.2 primary care visits per year, compared with 3.8 for controls. The visits clustered around nonspecific complaints of arthritis and arthralgias, alopecia, and rash (Arthritis Care Res. 2017 Jun;69[6]:833-41).
“An accumulating number of primary care office visits and referrals over time should raise suspicion,” Dr. Mosca said.
Other investigators, working with 1,426 cases of newly diagnosed SLE in the U.K. Clinical Practice Research Database, observed that the proportion of patients with disease manifestations in three or more British Isles Lupus Activity Group (BILAG) symptom domains rose from 18.7% at 3 years prior to diagnosis to 39.7% in the year before diagnosis (Lupus Sci Med. 2017 Feb 10;4[1]:e000172. doi: 10.1136/lupus-2016-000172).
“These patients accrue clinical manifestations. It’s not just one symptom, it’s more of a state of being unwell. This is a suspicious factor for the development of lupus,” she continued.
And just as patients who will eventually be diagnosed with SLE accrue a growing number of signs and symptoms during the run up to diagnosis, they also accrue multiple autoantibodies. Moreover, as demonstrated by a multicenter group of U.S. investigators, patients also develop elevated levels of multiple soluble inflammatory markers more than 3.5 years prior to diagnosis of SLE. These include interleukins-5 and -6 and interferon-gamma. And less than 10 months prior to being classified as having SLE, patients develop significantly higher levels of B lymphocyte stimulator (BLyS) and a proliferation-inducing ligand known as APRIL. The investigators developed a predictive model incorporating IL-5, -6, and interferon-gamma levels with antinuclear antibody status that identified future SLE patients with 84% accuracy more than 3.5 years before diagnosis. This could prove useful in selecting high-risk patients for clinical prevention trials (J Autoimmun. 2016 Nov;74:182-93).
Researchers at the University of Leeds (England) have also zeroed in on interferon activity as playing a key role in progression from asymptomatic antinuclear antigen positivity, which is present in up to 25% of the general population, to symptomatic autoimmune connective tissue disease, which affects less than 1%. A multivariate logistic regression analysis identified two independent predictors of development of autoimmune connective tissue disease within the next 12 months: a family history of autoimmune rheumatic disease, which was associated with an 8.2-fold increased risk; and positivity for a pattern of interferon-stimulated gene activity they call IFN-Score-B (Ann Rheum Dis. 2018 Oct;77[10]:1432-9).
All of this work has led up to what Dr. Mosca called “a glance into the future”: the National Institutes of Health–supported Study of Anti-Malarials in Incomplete Lupus Erythematosus (SMILE), which is now recruiting patients. This randomized, double-blind, placebo-controlled multicenter U.S. trial involves patients who are antinuclear antibody positive at a titer of 1:80 or more plus one or two additional criteria from the SLICC classification scheme. Participants are being randomized to 96 weeks of hydroxychloroquine or placebo. The goal is to learn whether hydroxychloroquine can slow disease progression, with the primary endpoint being the number of SLICC criteria met at the study’s end. The trial will also scrutinize potential biomarkers that could be used to guide treatment decisions (Trials. 2018 Dec 20;19[1]:694. doi: 10.1186/s13063-018-3076-7).
Dr. Mosca reported serving as an adviser to UCB and Lilly.
SAN FRANCISCO – A host of novel clinical and serologic findings that physicians can put to good use right now in helping to distinguish early SLE from its many mimickers have been identified in a large study conducted on four continents, Marta Mosca, MD, PhD, observed at an international congress on systemic lupus erythematosus.
These useful findings aren’t incorporated into the current American College of Rheumatology (ACR) or Systemic Lupus International Collaborating Clinics (SLICC) lupus classification criteria, which have come under criticism for limited sensitivity in identifying early SLE. Some of the novel findings provide support for increased suspicion of early SLE, while others suggest a need to veer in another direction and assess a patient for a disease other than lupus. The study has served to provide input for the proposed new ACR/EULAR weighted SLE classification criteria, although that scheme is meant to be used only for research and not in clinical practice, explained Dr. Mosca of the University of Pisa (Italy).
She was lead author of the four-continent study, which included 616 patients referred to experienced academic lupus centers for possible SLE with a symptom duration of less than 1 year. During up to 3 years of follow-up, 389 patients were diagnosed as having SLE by experienced rheumatologists based upon their clinical judgment, without any requirement to meet the full ACR or SLICC classification criteria. The other 227 patients were determined to be SLE mimickers with conditions including lymphoma, Sjögren’s syndrome, systemic sclerosis, interstitial lung disease, fibromyalgia, antinuclear antibody–positive thyroiditis, and undifferentiated connective tissue disease.
Dr. Mosca also highlighted key recent work by other investigators aimed at speeding the diagnosis of SLE and shortening the duration of what she called “the gray zone” of diagnostic uncertainty, when autoantibodies and insidious symptoms are present but not yet sufficient to make the diagnosis of SLE by conventional criteria. It’s well established that 60%-70% of patients with mild undifferentiated connective tissue disease will remain stable without evolving into SLE during long years of follow-up.
The ultimate objective of all this work is to try to change the natural history of the disease through targeted early aggressive therapy aimed at minimizing the extent of active disease and preventing severe organ involvement.
Among the key takeaways from the four-continent study led by Dr. Mosca: Fever not related to infection was far more prevalent in early SLE than in mimicking conditions, by a margin of 34.5% versus 13.7%. On the other hand, Raynaud’s phenomenon was more than twice as prevalent among patients with mimicking conditions: 22.1% in early SLE, compared with 48.5% in SLE mimickers. Sicca symptoms were present in just 4.4% of early SLE patients versus 34.4% of SLE mimickers. Only 0.3% of early SLE patients complained of dysphagia; the rate was 20-fold higher in the SLE mimickers. Rashes atypical for lupus were twice as frequent in the SLE mimicking conditions (Arthritis Rheumatol. 2019 Jan;71[1]:91-8).
Turning to key differentiating serologic findings, Dr. Mosca noted that anti-double stranded DNA (anti-dsDNA) and anti-Sm antibodies were present in 71.7% and 30.2% of early SLE patients, respectively, compared with 6.9% and 2.6% of SLE mimickers. Anticardiolipin IgM, a positive Coombs test, anti-beta2 glycoprotein-I antibodies, leukopenia, autoimmune hemolytic anemia, and hypocomplementemia were all significantly more common in the early SLE cohort.
In contrast, antibodies to Ro (SS-A) and La (SS-B) were of no value in separating early SLE from its mimickers, according to Dr. Mosca.
Other tipoffs to early SLE
Two separate teams of British researchers have advanced the field in a highly practical way. One group showed in a study of 1,739 newly diagnosed SLE patients and 6,956 controls that in the 5 years prior to diagnosis, the SLE group averaged 9.2 primary care visits per year, compared with 3.8 for controls. The visits clustered around nonspecific complaints of arthritis and arthralgias, alopecia, and rash (Arthritis Care Res. 2017 Jun;69[6]:833-41).
“An accumulating number of primary care office visits and referrals over time should raise suspicion,” Dr. Mosca said.
Other investigators, working with 1,426 cases of newly diagnosed SLE in the U.K. Clinical Practice Research Database, observed that the proportion of patients with disease manifestations in three or more British Isles Lupus Activity Group (BILAG) symptom domains rose from 18.7% at 3 years prior to diagnosis to 39.7% in the year before diagnosis (Lupus Sci Med. 2017 Feb 10;4[1]:e000172. doi: 10.1136/lupus-2016-000172).
“These patients accrue clinical manifestations. It’s not just one symptom, it’s more of a state of being unwell. This is a suspicious factor for the development of lupus,” she continued.
And just as patients who will eventually be diagnosed with SLE accrue a growing number of signs and symptoms during the run up to diagnosis, they also accrue multiple autoantibodies. Moreover, as demonstrated by a multicenter group of U.S. investigators, patients also develop elevated levels of multiple soluble inflammatory markers more than 3.5 years prior to diagnosis of SLE. These include interleukins-5 and -6 and interferon-gamma. And less than 10 months prior to being classified as having SLE, patients develop significantly higher levels of B lymphocyte stimulator (BLyS) and a proliferation-inducing ligand known as APRIL. The investigators developed a predictive model incorporating IL-5, -6, and interferon-gamma levels with antinuclear antibody status that identified future SLE patients with 84% accuracy more than 3.5 years before diagnosis. This could prove useful in selecting high-risk patients for clinical prevention trials (J Autoimmun. 2016 Nov;74:182-93).
Researchers at the University of Leeds (England) have also zeroed in on interferon activity as playing a key role in progression from asymptomatic antinuclear antigen positivity, which is present in up to 25% of the general population, to symptomatic autoimmune connective tissue disease, which affects less than 1%. A multivariate logistic regression analysis identified two independent predictors of development of autoimmune connective tissue disease within the next 12 months: a family history of autoimmune rheumatic disease, which was associated with an 8.2-fold increased risk; and positivity for a pattern of interferon-stimulated gene activity they call IFN-Score-B (Ann Rheum Dis. 2018 Oct;77[10]:1432-9).
All of this work has led up to what Dr. Mosca called “a glance into the future”: the National Institutes of Health–supported Study of Anti-Malarials in Incomplete Lupus Erythematosus (SMILE), which is now recruiting patients. This randomized, double-blind, placebo-controlled multicenter U.S. trial involves patients who are antinuclear antibody positive at a titer of 1:80 or more plus one or two additional criteria from the SLICC classification scheme. Participants are being randomized to 96 weeks of hydroxychloroquine or placebo. The goal is to learn whether hydroxychloroquine can slow disease progression, with the primary endpoint being the number of SLICC criteria met at the study’s end. The trial will also scrutinize potential biomarkers that could be used to guide treatment decisions (Trials. 2018 Dec 20;19[1]:694. doi: 10.1186/s13063-018-3076-7).
Dr. Mosca reported serving as an adviser to UCB and Lilly.
REPORTING FROM LUPUS 2019