TLR-activated repression of Fe-S cluster biogenesis drives a metabolic shift and alters histone and tubulin acetylation

Tong, Wing-Hang; Maio, Nunziata; Zhang, De-Liang; Palmieri, Erika M.; Ollivierre, Hayden; Ghosh, Manik C.; McVicar, Daniel W.; Rouault, Tracey A.

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American Society of Hematology, Blood Advances, 10(2), p. 1146-1156, 2018

DOI: 10.1182/bloodadvances.2018015669

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TLR-activated repression of Fe-S cluster biogenesis drives a metabolic shift and alters histone and tubulin acetylation

Journal article published in 2018 by Wing-Hang Tong

, Nunziata Maio, De-Liang Zhang

, Erika M. Palmieri, Hayden Ollivierre, Manik C. Ghosh, Daniel W. McVicar

, Tracey A. Rouault

This paper is made freely available by the publisher.

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Abstract

Key Points TLR activation suppresses expression of Fe-S cluster biogenesis factors NFS1, ISCU, HSC20, FXN, ISD11, GLRX5, CIAO1, FAM96A, and FAM96B. Restriction of Fe-S cluster biogenesis not only impairs oxidative metabolism but also modulates histone and tubulin acetylation profiles.

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TLR-activated repression of Fe-S cluster biogenesis drives a metabolic shift and alters histone and tubulin acetylation

Abstract