Apolipoprotein L1 risk variants associate with prevalent atherosclerotic disease in African American systemic lupus erythematosus patients.

Ashira Blazer Binhuan Wang Danny Simpson Tomas Kirchhoff Sean Heffron Robert M Clancy Adriana Heguy Karina Ray Matija Snuderl Jill P Buyon

PLoS One

Department of Medicine, Division of Rheumatology, New York University School of Medicine, New York, New York, United States of America.

Published: October 2017

A study was conducted to explore the relationship between common risk alleles of Apolipoprotein L1 (APOL1) and atherosclerotic cardiovascular disease (CVD) in African American patients with systemic lupus erythematosus (SLE), revealing an increased risk in this population compared to White patients.
The research involved 113 African American SLE patients, who were genotyped for APOL1 and assessed for various cardiovascular problems; results showed a significant association between carrying risk alleles and higher rates of atherosclerotic CVD.
Findings indicated that patients with more APOL1 risk alleles had a greater prevalence of symptomatic CVD, suggesting that these genetic factors contribute to the heightened cardiovascular

Objective: Atherosclerosis is exaggerated in African American (AA) systemic lupus erythematosus (SLE) patients, with doubled cardiovascular disease (CVD) risk compared to White patients. The extent to which common Apolipoprotein L1 (APOL1) risk alleles (RA) contribute to this trend is unknown. This retrospective cohort study assessed prevalent atherosclerotic disease across APOL1 genotypes in AA SLE patients.

Methods: One hundred thirteen AA SLE subjects were APOL1-genotyped and stratified as having: zero risk alleles, one risk allele, or two risk alleles. Chart review assessed CVD manifestations including abdominal aortic aneurysm, angina, carotid artery disease, coronary artery disease, myocardial infarction, peripheral vascular disease, stroke, and vascular calcifications. Associations between the genotypes and a composite endpoint defined as one or more CVD manifestations were calculated using logistic regression. Symptomatic atherosclerotic disease, excluding incidental vascular calcifications, was also assessed.

Results: The 0-risk-allele, 1-risk-allele and 2-risk-allele groups, respectively, comprised 34%, 53%, and 13% of the cohort. Respectively, 13.2%, 41.7%, and 60.0% of the 0-risk allele, 1-risk-allele, and 2-risk-allele groups met the composite endpoint of atherosclerotic CVD (p = 0.001). Adjusting for risk factors-including smoking, ESRD, BMI >25 and hypertension-we observed an association between carrying one or more RA and atherosclerotic CVD (OR = 7.1; p = 0.002). For symptomatic disease, the OR was 3.5 (p = 0.02). In a time-to-event analysis, the proportion of subjects free from the composite primary endpoint, symptomatic atherosclerotic CVD, was higher in the 0-risk-allele group compared to the 1-risk-allele and 2-risk-allele groups (χ2 = 6.5; p = 0.04).

Conclusions: Taken together, the APOL1 RAs associate with prevalent atherosclerotic CVD in this cohort of AA SLE patients, perhaps reflecting a potentiating effect of SLE on APOL1-related cardiovascular phenotypes.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5574561	PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0182483	PLOS

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