Inflammation-Modulated Metabolic Reprogramming Is Required for DUOX-Dependent Gut Immunity in Drosophila

Lee, Kyung-Ah; Cho, Kyu-Chan; Kim, Boram; Jang, In-Hwan; Nam, Kibum; Kwon, Young Eun; Kim, Myungjin; Hyeon, Do Young; Hwang, Daehee; Seol, Jae-Hong; Lee, Won-Jae

doi:10.1016/j.chom.2018.01.011

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Inflammation-Modulated Metabolic Reprogramming Is Required for DUOX-Dependent Gut Immunity in Drosophila

Authors: Lee, Kyung-Ah; Cho, Kyu-Chan; Kim, Boram; Jang, In-Hwan; Nam, Kibum; Kwon, Young Eun; Kim, Myungjin; Hyeon, Do Young; Hwang, Daehee; Seol, Jae-Hong; Lee, Won-Jae

Issue Date: Mar-2018

Publisher: CELL PRESS

Citation: CELL HOST & MICROBE, v.23, no.3, pp.338 - +

Journal Title: CELL HOST & MICROBE

Volume: 23

Number: 3

Start Page: 338

End Page: +

URI: http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/750

DOI: 10.1016/j.chom.2018.01.011

ISSN: 1931-3128

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.

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