The incidence rates of common forms of kidney disease including that attributed to hypertension are significantly higher in African Americans, relative to Caucasians. Racial differences in the frequency of Apolipoprotein L1 gene (APOL1) variants are now known to account for these differences. APOL1 risk variants rose to high frequency in African Americans since one copy protects from the parasite that causes African sleeping sickness, a potentially fatal disease. Approximately 10% of African Americans inherit two copies of APOL1 risk variants, placing them at a ten-fold increased risk for kidney disease. The mechanism whereby APOL1 gene variants contribute to kidney disease is unknown. This application proposes to determine how APOL1 gene variants contribute to kidney disease, information likely to yield more effective therapies. Existing therapies including strict blood pressure control have had disappointing results. We propose to determine whether: (1) variation in the APOL1 gene in kidney cells directly leads to cell dysfunction with resultant kidney disease, and/or (2) abnormal circulating ApoL1 proteins (high density lipoprotein [HDL] bound or lipid-free) lead to kidney disease. To explore mechanism 1, gene expression profiles will be examined in kidney cells from African Americans with and without APOL1 risk variants to determine which genes and gene pathways are over expressed (turned up) or under expressed (turned down), based upon the APOL1- specific genetic make-up of the cells. To explore mechanism 2, the amount and binding patterns of circulating ApoL1 proteins to HDL will be examined based upon an individual's genetic make- up. Kidney cells will be exposed to normal and risk ApoL1 proteins in vitro to determine whether risk variant proteins are toxic to cells and how this toxicity manifests. Based on these studies, additional analyses may be conducted in transgenic mice expressing normal and variant APOL1 to assess renal effects and in vivo metabolism of ApoL1 proteins. We will also attempt to identify undetected kidney disease risk variants in the APOL1 gene by deeply sequencing the surrounding chromosomal region. These experiments are likely to determine the mechanisms whereby APOL1 gene variants lead to non-diabetic kidney disease and assist in finding a cure for this devastating disease disproportionately impacting the African American community.

Public Health Relevance

Relative to Caucasians, African Americans have higher rates of non-diabetic kidney disease including focal segmental glomerulosclerosis, Human Immunodeficiency Virus-associated nephropathy and hypertension-attributed (HA) end-stage renal disease;all three diseases are associated with a variant Apolipoprotein L1 gene (APOL1). Aggressive hypertension control using angiotensin converting enzyme inhibitors failed to prevent progression of kidney disease in African Americans thought to have HA kidney disease, suggesting the presence of alternative disease mechanisms and demonstrating the urgent need to develop novel treatments. This renewal of RO1 DK 070941 proposes to closely examine genetic variation in the APOL1 gene region in African Americans with clinically diagnosed HA kidney disease and attempt to determine the inciting mechanism(s) whereby APOL1 gene variants contribute to development of kidney disease, steps that are critical to finding a cure for this devastating kidney disease that disproportionately impacts the African American community.

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK070941-05
Application #
8184458
Study Section
Kidney, Nutrition, Obesity and Diabetes (KNOD)
Program Officer
Rasooly, Rebekah S
Project Start
2005-04-01
Project End
2016-04-30
Budget Start
2011-09-22
Budget End
2012-04-30
Support Year
5
Fiscal Year
2011
Total Cost
$732,862
Indirect Cost
Name
Wake Forest University Health Sciences
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
937727907
City
Winston-Salem
State
NC
Country
United States
Zip Code
27157
Langefeld, Carl D; Comeau, Mary E; Ng, Maggie C Y et al. (2018) Genome-wide association studies suggest that APOL1-environment interactions more likely trigger kidney disease in African Americans with nondiabetic nephropathy than strong APOL1-second gene interactions. Kidney Int 94:599-607
Freedman, Barry I; Julian, Bruce A (2018) Evaluation of Potential Living Kidney Donors in the APOL1 Era. J Am Soc Nephrol 29:1079-1081
Ma, Lijun; Divers, Jasmin; Freedman, Barry I (2018) Mechanisms of injury in APOL1-associated kidney disease. Transplantation :
Guan, Meijian; Keaton, Jacob M; Dimitrov, Latchezar et al. (2018) An Exome-wide Association Study for Type 2 Diabetes-Attributed End-Stage Kidney Disease in African Americans. Kidney Int Rep 3:867-878
Tucker, Bryan M; Freedman, Barry I (2018) Need to Reclassify Etiologies of ESRD on the CMS 2728 Medical Evidence Report. Clin J Am Soc Nephrol 13:477-479
Skorecki, Karl L; Lee, Jessica H; Langefeld, Carl D et al. (2018) A null variant in the apolipoprotein L3 gene is associated with non-diabetic nephropathy. Nephrol Dial Transplant 33:323-330
Keaton, Jacob M; Gao, Chuan; Guan, Meijian et al. (2018) Genome-wide interaction with the insulin secretion locus MTNR1B reveals CMIP as a novel type 2 diabetes susceptibility gene in African Americans. Genet Epidemiol 42:559-570
Santoriello, Dominick; Husain, Syed A; De Serres, Sacha A et al. (2018) Donor APOL1 high-risk genotypes are associated with increased risk and inferior prognosis of de novo collapsing glomerulopathy in renal allografts. Kidney Int 94:1189-1198
Freedman, Barry I; Limou, Sophie; Ma, Lijun et al. (2018) APOL1-Associated Nephropathy: A Key Contributor to Racial Disparities in CKD. Am J Kidney Dis 72:S8-S16
Palmer, Nicholette D; Ma, Lijun; Freedman, Barry I (2018) Have We Made ""Rapid Progress"" Understanding the Pathogenesis in Rapidly Progressive Glomerulonephritis? Am J Nephrol 48:190-192

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