Early life gut microbiota sustains liver-resident natural killer cells maturation via the butyrate-IL-18 axis

Author:

Tian Panpan,Yang Wenwen,Guo XiaoweiORCID,Wang Tixiao,Tan Siyu,Sun Renhui,Xiao Rong,Wang Yuzhen,Jiao Deyan,Xu Yachen,Wei Yanfei,Wu Zhuanchang,Li ChunyangORCID,Gao LifenORCID,Ma ChunhongORCID,Liang XiaohongORCID

Abstract

AbstractLiver-resident natural killer cells, a unique lymphocyte subset in liver, develop locally and play multifaceted immunological roles. However, the mechanisms for the maintenance of liver-resident natural killer cell homeostasis remain unclear. Here we show that early-life antibiotic treatment blunt functional maturation of liver-resident natural killer cells even at adulthood, which is dependent on the durative microbiota dysbiosis. Mechanistically, early-life antibiotic treatment significantly decreases butyrate level in liver, and subsequently led to defective liver-resident natural killer cell maturation in a cell-extrinsic manner. Specifically, loss of butyrate impairs IL-18 production in Kupffer cells and hepatocytes through acting on the receptor GPR109A. Disrupted IL-18/IL-18R signaling in turn suppresses the mitochondrial activity and the functional maturation of liver-resident natural killer cells. Strikingly, dietary supplementation of experimentally or clinically used Clostridium butyricum restores the impaired liver-resident natural killer cell maturation and function induced by early-life antibiotic treatment. Our findings collectively unmask a regulatory network of gut-liver axis, highlighting the importance of the early-life microbiota in the development of tissue-resident immune cells.

Funder

Taishan Scholar Foundation of Shandong Province

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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