Race-specific association of an IRGM risk allele with cytokine expression in human subjects

Author:

Ajayi Teminioluwa,Rai Prashant,Shi Min,Gabor Kristin A.,Karmaus Peer W. F.,Meacham Julie M.,Katen Kevin,Madenspacher Jennifer H.,Schurman Shepherd H.,Fessler Michael B.

Abstract

AbstractImmunity-related GTPase family M (IRGM), located on human chromosome 5q33.1, encodes a protein that promotes autophagy and suppresses the innate immune response. The minor allele of rs13361189 (−4299T>C), a single nucleotide polymorphism in the IRGM promoter, has been associated with several diseases, including Crohn’s disease and tuberculosis. Although patterns of linkage disequilibrium and minor allele frequency for this polymorphism differ dramatically between subjects of European and African descent, studies of rs13361189 have predominantly been conducted in Europeans and the mechanism of association is poorly understood. We recruited a cohort of 68 individuals (30 White, 34 African American, 4 other race) with varying rs13361189 genotypes and assessed a panel of immune response measures including whole blood cytokine induction following ex vivo stimulation with Toll-like Receptor ligands. Minor allele carriers were found to have increased serum immunoglobulin M, C-reactive protein, and circulating CD8+ T cells. No differences in whole blood cytokines were observed between minor allele carriers and non-carriers in the overall study population; however, minor allele status was associated with increased induction of a subset of cytokines among African American subjects, and decreased induction among White subjects. These findings underline the importance of broad racial inclusion in genetic studies of immunity.

Funder

National Institute of Environmental Health Sciences

National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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1. Genomic Interactions Between Mycobacterium tuberculosis and Humans;Annual Review of Genomics and Human Genetics;2024-08-27

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