| Literature DB >> 29907708 |
Kenta Kikuchi1, Mayumi Iida1, Naoki Ikeda1, Shigetaka Moriyama1, Michito Hamada2, Satoru Takahashi2, Hiroshi Kitamura3, Takashi Watanabe4, Yoshinori Hasegawa5, Koji Hase6, Takeshi Fukuhara7,8, Hideyo Sato9, Eri H Kobayashi10, Takafumi Suzuki10, Masayuki Yamamoto10, Masato Tanaka11, Kenichi Asano11.
Abstract
Macrophages manifest distinct phenotype according to the organs in which they reside. In addition, they flexibly switch their character in adaptation to the changing environment. However, the molecular basis that explains the conversion of the macrophage phenotype has so far been unexplored. We find that CD169+ macrophages change their phenotype by regulating the level of a transcription factor Maf both in vitro and in vivo in C57BL/6J mice. When CD169+ macrophages were exposed to bacterial components, they expressed an array of acute inflammatory response genes in Maf-dependent manner and simultaneously start to downregulate Maf. This Maf suppression is dependent on accelerated degradation through proteasome pathway and microRNA-mediated silencing. The downregulation of Maf unlocks the NF-E2-related factor 2-dominant, cytoprotective/antioxidative program in the same macrophages. The present study provides new insights into the previously unanswered question of how macrophages initiate proinflammatory responses while retaining their capacity to repair injured tissues during inflammation.Entities:
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Year: 2018 PMID: 29907708 DOI: 10.4049/jimmunol.1800040
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422