| Literature DB >> 29503179 |
Kyung-Ah Lee1, Kyu-Chan Cho2, Boram Kim2, In-Hwan Jang3, Kibum Nam3, Young Eun Kwon2, Myungjin Kim4, Do Young Hyeon5, Daehee Hwang6, Jae-Hong Seol2, Won-Jae Lee7.
Abstract
DUOX, a member of the NADPH oxidase family, acts as the first line of defense against enteric pathogens by producing microbicidal reactive oxygen species. DUOX is activated upon enteric infection, but the mechanisms regulating DUOX activity remain incompletely understood. Using Drosophila genetic tools, we show that enteric infection results in "pro-catabolic" signaling that initiates metabolic reprogramming of enterocytes toward lipid catabolism, which ultimately governs DUOX homeostasis. Infection induces signaling cascades involving TRAF3 and kinases AMPK and WTS, which regulate TOR kinase to control the balance of lipogenesis versus lipolysis. Enhancing lipogenesis blocks DUOX activity, whereas stimulating lipolysis via ATG1-dependent lipophagy is required for DUOX activation. Drosophila with altered activity in TRAF3-AMPK/WTS-ATG1 pathway components exhibit abolished infection-induced lipolysis, reduced DUOX activation, and enhanced susceptibility to enteric infection. Thus, this work uncovers signaling cascades governing inflammation-induced metabolic reprogramming and provides insight into the pathophysiology of immune-metabolic interactions in the microbe-laden gut epithelia.Entities:
Keywords: DUOX; Drosophila; dual oxidase; enteric infection; gut immunity; gut physiology; host defense; host-microbe interactions; innate immunity; metabolic reprogramming
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Year: 2018 PMID: 29503179 DOI: 10.1016/j.chom.2018.01.011
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023