Association of APOL1 Risk Alleles With Cardiovascular Disease in Blacks in the Million Veteran Program

Alexander G Bick; Elvis Akwo; Cassianne Robinson-Cohen; Kyung Lee; Julie Lynch; Themistocles L Assimes; Scott DuVall; Todd Edwards; Huaying Fang; S Matthew Freiberg; Ayush Giri; Jennifer E Huffman; Jie Huang; Leland Hull; Rachel L Kember; Derek Klarin; Jennifer S Lee; Michael Levin; Donald R Miller; Pradeep Natarajan; Danish Saleheen; Qing Shao; Yan V Sun; Hua Tang; Otis Wilson; Kyong-Mi Chang; Kelly Cho; John Concato; J Michael Gaziano; Sekar Kathiresan; Christopher J O'Donnell; Daniel J Rader; Philip S Tsao; Peter W Wilson; Adriana M Hung; Scott M Damrauer; VA Million Veteran Program

doi:10.1161/CIRCULATIONAHA.118.036589

Association of APOL1 Risk Alleles With Cardiovascular Disease in Blacks in the Million Veteran Program

Circulation. 2019 Sep 17;140(12):1031-1040. doi: 10.1161/CIRCULATIONAHA.118.036589. Epub 2019 Jul 24.

Authors

Alexander G Bick^{1

2

3}, Elvis Akwo^{4

5}, Cassianne Robinson-Cohen^{4

5}, Kyung Lee⁶, Julie Lynch^{6

7

8}, Themistocles L Assimes^{9

10}, Scott DuVall⁸, Todd Edwards^{4

5}, Huaying Fang^{9

10}, S Matthew Freiberg^{4

5}, Ayush Giri^{4

5}, Jennifer E Huffman¹, Jie Huang¹, Leland Hull^{1

6}, Rachel L Kember^{11

12}, Derek Klarin^{1

2

3}, Jennifer S Lee^{9

10}, Michael Levin^{11

12}, Donald R Miller^{6

13}, Pradeep Natarajan^{2

3}, Danish Saleheen^{11

12}, Qing Shao⁶, Yan V Sun^{14

15}, Hua Tang^{9

10}, Otis Wilson⁴, Kyong-Mi Chang^{11

12}, Kelly Cho¹, John Concato¹⁶, J Michael Gaziano^{1

17}, Sekar Kathiresan^{2

3

17}, Christopher J O'Donnell^{1

17}, Daniel J Rader¹¹, Philip S Tsao^{9

10}, Peter W Wilson^{14

15}, Adriana M Hung^{4

5}, Scott M Damrauer^{11

12}; VA Million Veteran Program

Affiliations

¹ Boston VA Healthcare System, MA (A.G.B., J.E.H., J.H., L.H., D.K., K.C., J.M.G., C.J.O.).
² Massachusetts General Hospital, Boston (A.G.B., D.K., P.N., S.K.).
³ Broad Institute of MIT and Harvard, Cambridge, MA (A.G.B., D.K., P.N., S.K.).
⁴ Nashville VA Medical Center, TN (E.A., C.R.-C., T.E., S.M.F., A.G., O.W., A.M.H.).
⁵ Vanderbilt University Medical Center, Nashville, TN (E.A., C.R.-C., T.E., S.M.F., A.G., A.M.H.).
⁶ Edith Norse Rogers Memorial VA Medical Center, Bedford, MA (K.L., J.L., L.H., D.R.M., Q.S.).
⁷ University of Massachusetts College of Nursing & Health Sciences, Boston (J.L.).
⁸ VA Informatics and Computing Infrastructure, Salt Lake City, UT (J.L., S.D.).
⁹ Palo Alto VA Health Care, CA (T.L.A., H.F., J.S.L., H.T., P.S.T.).
¹⁰ Stanford University School of Medicine, CA (T.L.A., H.F., J.S.L., H.T., P.S.T.).
¹¹ Corporal Michael Crescenz VA Medical Center, Philadelphia, PA (R.L.K., M.L., D.S., K.-M.C., D.J.R., S.M.D.).
¹² Perelman School of Medicine, University of Pennsylvania, Philadelphia (R.L.K., M.L., D.S., K.-M.C., S.M.D.).
¹³ Boston University, MA (D.R.M.).
¹⁴ Atlanta VA Medical Center, GA (Y.V.S., P.W.W.).
¹⁵ Emory University, Atlanta, GA (Y.V.S., P.W.W.).
¹⁶ VA Connecticut HealthCare System, New Haven (J.C.).
¹⁷ Harvard Medical School, Boston, MA (J.M.G., S.K., C.J.O.).

Abstract

Background: Approximately 13% of black individuals carry 2 copies of the apolipoprotein L1 (APOL1) risk alleles G1 or G2, which are associated with 1.5- to 2.5-fold increased risk of chronic kidney disease. There have been conflicting reports as to whether an association exists between APOL1 risk alleles and cardiovascular disease (CVD) that is independent of the effects of APOL1 on kidney disease. We sought to test the association of APOL1 G1/G2 alleles with coronary artery disease, peripheral artery disease, and stroke among black individuals in the Million Veteran Program.

Methods: We performed a time-to-event analysis of retrospective electronic health record data using Cox proportional hazard and competing-risks Fine and Gray subdistribution hazard models. The primary exposure was APOL1 risk allele status. The primary outcome was incident coronary artery disease among individuals without chronic kidney disease during the 12.5-year follow-up period. We separately analyzed the cross-sectional association of APOL1 risk allele status with lipid traits and 115 cardiovascular diseases using phenome-wide association.

Results: Among 30 903 black Million Veteran Program participants, 3941 (13%) carried the 2 APOL1 risk allele high-risk genotype. Individuals with normal kidney function at baseline with 2 risk alleles had slightly higher risk of developing coronary artery disease compared with those with no risk alleles (hazard ratio, 1.11 [95% CI, 1.01-1.21]; P=0.039). Similarly, modest associations were identified with incident stroke (hazard ratio, 1.20 [95% CI, 1.05-1.36; P=0.007) and peripheral artery disease (hazard ratio, 1.15 [95% CI, 1.01-1.29l; P=0.031). When both cardiovascular and renal outcomes were modeled, APOL1 was strongly associated with incident renal disease, whereas no significant association with the CVD end points could be detected. Cardiovascular phenome-wide association analyses did not identify additional significant associations with CVD subsets.

Conclusions: APOL1 risk variants display a modest association with CVD, and this association is likely mediated by the known APOL1 association with chronic kidney disease.

Keywords: apolipoprotein L1; cardiovascular diseases; genetics; renal insufficiency, chronic.

Publication types

Research Support, U.S. Gov't, P.H.S.

MeSH terms

Adult
Alleles
Apolipoprotein L1 / genetics*
Black or African American*
Coronary Artery Disease / epidemiology
Coronary Artery Disease / genetics*
Electronic Health Records
Female
Genetic Predisposition to Disease
Genotype*
Humans
Incidence
Male
Middle Aged
Myocardial Infarction / epidemiology
Myocardial Infarction / genetics*
Peripheral Arterial Disease / epidemiology
Peripheral Arterial Disease / genetics*
Polymorphism, Genetic
Retrospective Studies
Risk
United States / epidemiology
Veterans

Substances

APOL1 protein, human
Apolipoprotein L1

Abstract

Publication types

MeSH terms

Substances

Grants and funding