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Allele-specific expression changes dynamically during T cell activation in HLA and other autoimmune loci.

Citation
Gutierrez-Arcelus, M., et al. “Allele-Specific Expression Changes Dynamically During T Cell Activation In Hla And Other Autoimmune Loci.”. Nature Genetics, pp. 247-253.
Center UCSD-UCLA
Author Maria Gutierrez-Arcelus, Yuriy Baglaenko, Jatin Arora, Susan Hannes, Yang Luo, Tiffany Amariuta, Nikola Teslovich, Deepak A Rao, Joerg Ermann, Helena Jonsson, NHLBI Trans-Omics for Precision Medicine Consortium, Cristina Navarrete, Stephen S Rich, Kent D Taylor, Jerome I Rotter, Peter K Gregersen, Tõnu Esko, Michael B Brenner, Soumya Raychaudhuri
Abstract

Genetic studies have revealed that autoimmune susceptibility variants are over-represented in memory CD4 T cell regulatory elements. Understanding how genetic variation affects gene expression in different T cell physiological states is essential for deciphering genetic mechanisms of autoimmunity. Here, we characterized the dynamics of genetic regulatory effects at eight time points during memory CD4 T cell activation with high-depth RNA-seq in healthy individuals. We discovered widespread, dynamic allele-specific expression across the genome, where the balance of alleles changes over time. These genes were enriched fourfold within autoimmune loci. We found pervasive dynamic regulatory effects within six HLA genes. HLA-DQB1 alleles had one of three distinct transcriptional regulatory programs. Using CRISPR-Cas9 genomic editing we demonstrated that a promoter variant is causal for T cell-specific control of HLA-DQB1 expression. Our study shows that genetic variation in cis-regulatory elements affects gene expression in a manner dependent on lymphocyte activation status, contributing to the interindividual complexity of immune responses.

Year of Publication
2020
Journal
Nature genetics
Volume
52
Issue
3
Number of Pages
247-253
Date Published
12/2020
ISSN Number
1546-1718
DOI
10.1038/s41588-020-0579-4
Alternate Journal
Nat Genet
PMID
32066938
PMCID
PMC7135372
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