APOL1 nephropathy – a population genetics success story

OBJECTIVES (1) To examine 'race' in acute and chronic kidney disease under similar conditions, and (2) to encourage further study of implied cofactors and an international approach to end misuse of 'race'. METHODS We re-analyzed data from United States veterans, (1) comparing outcomes after removing 'race correction' from legacy estimated glomerular filtration rates and (2) graphing data to explore more subtle relationships. We hypothesized factors confounding the link between kidney disease and apolipoprotein L1 gene variants, including cofactors implied and controlled by veteran status. RESULTS Studies of veterans minimized 'racial' disparity in chronic kidney disease, suggesting an effect of starting conditions, including Armed Services entry requirements and equitable access to healthcare. Apolipoprotein L1 "high-risk" and N264K+ gene variants may be proxies for 'race', with gradients of effect due to colorism. CONCLUSIONS Under equitable conditions, comparable kidney disease outcomes should be the expected norm for all, regardless of 'race', ethnicity, or nationality. Discouraging misuse of 'race' in medical research and healthcare is an actionable population health initiative with potentially high impact but low effort and cost. ABBREVIATIONS AKI = acute kidney injury, APOL1 = apolipoprotein L1, BS = bad science, CKD = chronic kidney disease, COVID = coronavirus disease, eGFR = estimated GFR, FSGS = focal segmental glomerulosclerosis, GFR = glomerular filtration rate, HR = high risk, LR = low risk, IRB = institutional review board, KF = kidney failure, MDRD = Modification of Diet in Renal Disease, NASEM = National Academies of Science Engineering and Medicine, OR = odds ratio, RR = relative risk, RV = risk variant, SDOH = social determinants of health, VA = Veterans Administration.

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De novo rates of aTrypanosoma-resistant mutation in two human populations

Melamed,

Shemer,

Bolotin

et al. 2024

Preprint

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Until recently, mutation rates have only been measured as averages across many genomic positions. Recently, a method to measure mutation rates at the single-mutation resolution was applied to a narrow region in the human hemoglobin subunit beta (HBB) gene containing the site of the hemoglobin S (HbS) mutation as well as to a paralogous hemoglobin subunit delta (HBD) region, in sperm samples from sub-Saharan African and northern European donors. The HbS mutation, which protects against malaria while causing sickle-cell anemia in homozygotes originated de novo significantly more frequently in theHBBgene in Africans compared to the other three test cases combined (the EuropeanHBBgene and the European and AfricanHBDgene). Here, we apply this approach to the human apolipopro-tein L1 (APOL1) gene containing the site of the G1 1024A→G mutation, which protects against African sleeping sickness caused byTrypanosoma brucei gambiensewhile causing a substantially increased risk of chronic kidney disease (CKD) in homozygotes. We find that the 1024A→G mutation is the mutation of highest de novo origination rate and deviates most from the genome-wide average rate for its type (A→G) compared to all other observable mutations in the region, and that it originates de novo significantly more frequently in Africans than in Europeans—i.e., in the population where it is of adaptive significance. The results are inconsistent with the notion that the probability of a specific mutational event is independent of its value to the organism and underscore the importance of studying mutation rates at the single-mutation resolution.

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APOL1 nephropathy – a population genetics success story

Cited by 3 publications

References 101 publications

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Focal Segmental Glomerulosclerosis With Superimposed Infection‐Related Glomerulonephritis in a Diabetic Patient: A Case of Rapid Renal Decline

Re-analyzed APOL1 kidney data support new ethics of ‘race’

De novo rates of aTrypanosoma-resistant mutation in two human populations

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