APOL1 mediated kidney disease: A review and look toward the future

Authors

Vinay Srinivasan, Division of Nephrology, Cooper University Hospital and Cooper Medical School of Rowan University, Camden, NJ.
Paolo Nikolai So, Department of Internal Medicine, Piedmont Athens Regional, Athens, GA.
Edward P. Kwakyi, Department of Medicine and Therapeutics, University of Ghana Medical School, Accra, Ghana.
Edgar V. Lerma, Advocate Health - MidwestFollow
Nasim Wiegley, Division of Nephrology, University of California Davis School of Medicine, Sacramento, CA.

Recommended Citation

Srinivasan V, So PN, Kwakyi EPK, Lerma EV, Wiegley N. APOL1 Mediated Kidney Disease: A Review and Look Toward the Future. Kidney Med. 2025;7(9):101062. Published 2025 Jul 3. doi:10.1016/j.xkme.2025.101062

Affiliations

Advocate Christ Medical Center

Abstract

Individuals of recent African ancestry are disproportionately affected by kidney disease. The discovery of the Apolipoprotein L1 (APOL1) gene and, subsequently, the G1 and G2 risk alleles has helped to understand some of these disparities. The APOL1 gene does not appear to be necessary for normal kidney function, and the high-risk alleles appear to be gain of function mutations offering protection against Trypanosoma species. In the United States, ∼6 million African Americans have a high-risk genotype. However, not all patients with high-risk genotypes will develop kidney disease, leading to the idea of a second hit hypothesis by certain genetic, environmental, and inflammatory triggers. Recent clinical trials have focused on the different postulated mechanisms of cellular toxicity, and one promising candidate, inaxaplin, has advanced to a phase 3 study. This mini-review discusses the development of APOL1 risk alleles, clinical implications of a high-risk genotype, and a suggested framework for nephrologists to pursue genetic testing in countries where it is easily accessible.

Document Type

Article

PubMed ID

40837248