4.8 Article

Intersection of population variation and autoimmunity genetics in human T cell activation

Journal

SCIENCE
Volume 345, Issue 6202, Pages 1311-+

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.1254665

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Funding

  1. U.S. National Institute of General Medical Sciences [RC2 GM093080]
  2. NIH [F32 AG043267]
  3. National Multiple Sclerosis Society [JF2138A1]

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T lymphocyte activation by antigen conditions adaptive immune responses and immunopathologies, but we know little about its variation in humans and its genetic or environmental roots. We analyzed gene expression in CD4(+) T cells during unbiased activation or in T helper 17 (T(H)17) conditions from 348 healthy participants representing European, Asian, and African ancestries. We observed interindividual variability, most marked for cytokine transcripts, with clear biases on the basis of ancestry, and following patterns more complex than simple T(H)1/2/17 partitions. We identified 39 genetic loci specifically associated in cis with activated gene expression. We further fine-mapped and validated a single-base variant that modulates YY1 binding and the activity of an enhancer element controlling the autoimmune-associated IL2RA gene, affecting its activity in activated but not regulatory T cells. Thus, interindividual variability affects the fundamental immunologic process of T helper activation, with important connections to autoimmune disease.

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