| Literature DB >> 31853059 |
Kosaku Nanki1,2, Masayuki Fujii1,3, Mariko Shimokawa1, Mami Matano1, Shingo Nishikori1,4, Shoichi Date1,4, Ai Takano1, Kohta Toshimitsu1,2, Yuki Ohta1, Sirirat Takahashi1, Shinya Sugimoto1,2, Kazuhiro Ishimaru1,3, Kenta Kawasaki1,2, Yoko Nagai4, Ryota Ishii5, Kosuke Yoshida1,2, Nobuo Sasaki1,2, Toshifumi Hibi2,6, Soichiro Ishihara3, Takanori Kanai2, Toshiro Sato7,8.
Abstract
With ageing, normal human tissues experience an expansion of somatic clones that carry cancer mutations1-7. However, whether such clonal expansion exists in the non-neoplastic intestine remains unknown. Here, using whole-exome sequencing data from 76 clonal human colon organoids, we identify a unique pattern of somatic mutagenesis in the inflamed epithelium of patients with ulcerative colitis. The affected epithelium accumulates somatic mutations in multiple genes that are related to IL-17 signalling-including NFKBIZ, ZC3H12A and PIGR, which are genes that are rarely affected in colon cancer. Targeted sequencing validates the pervasive spread of mutations that are related to IL-17 signalling. Unbiased CRISPR-based knockout screening in colon organoids reveals that the mutations confer resistance to the pro-apoptotic response that is induced by IL-17A. Some of these genetic mutations are known to exacerbate experimental colitis in mice8-11, and somatic mutagenesis in human colon epithelium may be causally linked to the inflammatory process. Our findings highlight a genetic landscape that adapts to a hostile microenvironment, and demonstrate its potential contribution to the pathogenesis of ulcerative colitis.Entities:
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Year: 2019 PMID: 31853059 DOI: 10.1038/s41586-019-1844-5
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962