Inflammation status modulates the effect of host genetic variation on intestinal gene expression in inflammatory bowel disease

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作者
Shixian Hu
Werna T. Uniken Venema
Harm-Jan Westra
Arnau Vich Vila
Ruggero Barbieri
Michiel D. Voskuil
Tjasso Blokzijl
Bernadien H. Jansen
Yanni Li
Mark J. Daly
Ramnik J. Xavier
Gerard Dijkstra
Eleonora A. Festen
Rinse K. Weersma
机构
[1] University of Groningen and University Medical Center Groningen,Department of Gastroenterology and Hepatology
[2] University of Groningen and University Medical Center Groningen,Department of Genetics
[3] Broad Institute of Harvard and Massachusetts Institute of Technology,Institute for Molecular Medicine Finland, HiLIFE
[4] University of Helsinki,Center for Microbiome Informatics and Therapeutic
[5] Massachusetts Institute of Technology,undefined
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More than 240 genetic risk loci have been associated with inflammatory bowel disease (IBD), but little is known about how they contribute to disease development in involved tissue. Here, we hypothesized that host genetic variation affects gene expression in an inflammation-dependent way, and investigated 299 snap-frozen intestinal biopsies from inflamed and non-inflamed mucosa from 171 IBD patients. RNA-sequencing was performed, and genotypes were determined using whole exome sequencing and genome wide genotyping. In total, 28,746 genes and 6,894,979 SNPs were included. Linear mixed models identified 8,881 independent intestinal cis-expression quantitative trait loci (cis-eQTLs) (FDR < 0.05) and interaction analysis revealed 190 inflammation-dependent intestinal cis-eQTLs (FDR < 0.05), including known IBD-risk genes and genes encoding immune-cell receptors and antibodies. The inflammation-dependent cis-eQTL SNPs (eSNPs) mainly interact with prevalence of immune cell types. Inflammation-dependent intestinal cis-eQTLs reveal genetic susceptibility under inflammatory conditions that can help identify the cell types involved in and the pathways underlying inflammation, knowledge that may guide future drug development and profile patients for precision medicine in IBD.
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