| Literature DB >> 28515360 |
Izumi Ohigashi1, Yuki Ohte2, Kazuya Setoh3, Hiroshi Nakase1, Akiko Maekawa1, Hiroshi Kiyonari4, Yoko Hamazaki5, Miho Sekai5, Tetsuo Sudo6, Yasuharu Tabara3, Hiromi Sawai7, Yosuke Omae7, Rika Yuliwulandari8, Yasuhito Tanaka9, Masashi Mizokami10, Hiroshi Inoue11, Masanori Kasahara12, Nagahiro Minato5, Katsushi Tokunaga7, Keiji Tanaka13, Fumihiko Matsuda3, Shigeo Murata2, Yousuke Takahama1.
Abstract
The Psmb11-encoded β5t subunit of the thymoproteasome, which is specifically expressed in cortical thymic epithelial cells (cTECs), is essential for the optimal positive selection of functionally competent CD8+ T cells in mice. Here, we report that a human genomic PSMB11 variation, which is detectable at an appreciable allele frequency in human populations, alters the β5t amino acid sequence that affects the processing of catalytically active β5t proteins. The introduction of this variation in the mouse genome revealed that the heterozygotes showed reduced β5t expression in cTECs and the homozygotes further exhibited reduction in the cellularity of CD8+ T cells. No severe health problems were noticed in many heterozygous and 5 homozygous human individuals. Long-term analysis of health status, particularly in the homozygotes, is expected to improve our understanding of the role of the thymoproteasome-dependent positive selection of CD8+ T cells in humans.Entities:
Keywords: Genetics; Immunology
Year: 2017 PMID: 28515360 PMCID: PMC5436549 DOI: 10.1172/jci.insight.93664
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708