USP38 Inhibits Type I Interferon Signaling by Editing TBK1 Ubiquitination through NLRP4 Signalosome

Meng Lin; Zhiyao Zhao; Zhifen Yang; Qingcai Meng; Peng Tan; Weihong Xie; Yunfei Qin; Rong Fu Wang; Jun Cui

doi:10.1016/j.molcel.2016.08.029

USP38 Inhibits Type I Interferon Signaling by Editing TBK1 Ubiquitination through NLRP4 Signalosome

Meng Lin, Zhiyao Zhao, Zhifen Yang, Qingcai Meng, Peng Tan, Weihong Xie, Yunfei Qin, Rong Fu Wang, Jun Cui

Research output: Contribution to journal › Article › peer-review

103 Scopus citations

Abstract

TBK1 is a component of the type I interferon (IFN) signaling pathway, yet the mechanisms controlling its activity and degradation remain poorly understood. Here we report that USP38 negatively regulates type I IFN signaling by targeting the active form of TBK1 for degradation in vitro and in vivo. USP38 specifically cleaves K33-linked poly-ubiquitin chains from TBK1 at Lys670, and it allows for subsequent K48-linked ubiquitination at the same position mediated by DTX4 and TRIP. Knockdown or knockout of USP38 increases K33-linked ubiquitination, but it abrogates K48-linked ubiquitination and degradation of TBK1, thus enhancing type I IFN signaling. Our findings identify an essential role for USP38 in negatively regulating type I IFN signaling, and they provide insights into the mechanisms by which USP38 regulates TBK1 ubiquitination through the NLRP4 signalosome.

Original language	English (US)
Pages (from-to)	267-281
Number of pages	15
Journal	Molecular Cell
Volume	64
Issue number	2
DOIs	https://doi.org/10.1016/j.molcel.2016.08.029
State	Published - Oct 20 2016

Keywords

K33 ubiquitination
TBK1 degradation
TBK1 ubiquitination
USP38 deubiquitination
innate immune signaling
type I interferon response

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1016/j.molcel.2016.08.029

Cite this

@article{94e5cd653a15415d901c019d6ac6d7c7,

title = "USP38 Inhibits Type I Interferon Signaling by Editing TBK1 Ubiquitination through NLRP4 Signalosome",

abstract = "TBK1 is a component of the type I interferon (IFN) signaling pathway, yet the mechanisms controlling its activity and degradation remain poorly understood. Here we report that USP38 negatively regulates type I IFN signaling by targeting the active form of TBK1 for degradation in vitro and in vivo. USP38 specifically cleaves K33-linked poly-ubiquitin chains from TBK1 at Lys670, and it allows for subsequent K48-linked ubiquitination at the same position mediated by DTX4 and TRIP. Knockdown or knockout of USP38 increases K33-linked ubiquitination, but it abrogates K48-linked ubiquitination and degradation of TBK1, thus enhancing type I IFN signaling. Our findings identify an essential role for USP38 in negatively regulating type I IFN signaling, and they provide insights into the mechanisms by which USP38 regulates TBK1 ubiquitination through the NLRP4 signalosome.",

keywords = "K33 ubiquitination, TBK1 degradation, TBK1 ubiquitination, USP38 deubiquitination, innate immune signaling, type I interferon response",

author = "Meng Lin and Zhiyao Zhao and Zhifen Yang and Qingcai Meng and Peng Tan and Weihong Xie and Yunfei Qin and Wang, {Rong Fu} and Jun Cui",

note = "Funding Information: This work was supported by National Key Basic Research Program of China (2014CB910800 and 2015CB859800), National Natural Science Foundation of China (31370869 and 31522018), Guangdong Natural Science Funds for Distinguished Young Scholar (S2013050014772), Guangdong Innovative Research Team Program (NO. 2011Y035 and 201001Y0104687244), and was in part supported by grants (CA101795 and DA030338) from National Cancer Institute (NCI) and National Institute on Drug Abuse (NIDA), NIH (to R.-F.W.). We thank Dr. Ning for the graphical abstract. We also thank Dr. Fan for the mass spectrometry analysis of TBK1 ubiquitination. Publisher Copyright: {\textcopyright} 2016 Elsevier Inc.",

year = "2016",

month = oct,

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doi = "10.1016/j.molcel.2016.08.029",

language = "English (US)",

volume = "64",

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T1 - USP38 Inhibits Type I Interferon Signaling by Editing TBK1 Ubiquitination through NLRP4 Signalosome

AU - Lin, Meng

AU - Zhao, Zhiyao

AU - Yang, Zhifen

AU - Meng, Qingcai

AU - Tan, Peng

AU - Xie, Weihong

AU - Qin, Yunfei

AU - Wang, Rong Fu

AU - Cui, Jun

N1 - Funding Information: This work was supported by National Key Basic Research Program of China (2014CB910800 and 2015CB859800), National Natural Science Foundation of China (31370869 and 31522018), Guangdong Natural Science Funds for Distinguished Young Scholar (S2013050014772), Guangdong Innovative Research Team Program (NO. 2011Y035 and 201001Y0104687244), and was in part supported by grants (CA101795 and DA030338) from National Cancer Institute (NCI) and National Institute on Drug Abuse (NIDA), NIH (to R.-F.W.). We thank Dr. Ning for the graphical abstract. We also thank Dr. Fan for the mass spectrometry analysis of TBK1 ubiquitination. Publisher Copyright: © 2016 Elsevier Inc.

PY - 2016/10/20

Y1 - 2016/10/20

N2 - TBK1 is a component of the type I interferon (IFN) signaling pathway, yet the mechanisms controlling its activity and degradation remain poorly understood. Here we report that USP38 negatively regulates type I IFN signaling by targeting the active form of TBK1 for degradation in vitro and in vivo. USP38 specifically cleaves K33-linked poly-ubiquitin chains from TBK1 at Lys670, and it allows for subsequent K48-linked ubiquitination at the same position mediated by DTX4 and TRIP. Knockdown or knockout of USP38 increases K33-linked ubiquitination, but it abrogates K48-linked ubiquitination and degradation of TBK1, thus enhancing type I IFN signaling. Our findings identify an essential role for USP38 in negatively regulating type I IFN signaling, and they provide insights into the mechanisms by which USP38 regulates TBK1 ubiquitination through the NLRP4 signalosome.

AB - TBK1 is a component of the type I interferon (IFN) signaling pathway, yet the mechanisms controlling its activity and degradation remain poorly understood. Here we report that USP38 negatively regulates type I IFN signaling by targeting the active form of TBK1 for degradation in vitro and in vivo. USP38 specifically cleaves K33-linked poly-ubiquitin chains from TBK1 at Lys670, and it allows for subsequent K48-linked ubiquitination at the same position mediated by DTX4 and TRIP. Knockdown or knockout of USP38 increases K33-linked ubiquitination, but it abrogates K48-linked ubiquitination and degradation of TBK1, thus enhancing type I IFN signaling. Our findings identify an essential role for USP38 in negatively regulating type I IFN signaling, and they provide insights into the mechanisms by which USP38 regulates TBK1 ubiquitination through the NLRP4 signalosome.

KW - K33 ubiquitination

KW - TBK1 degradation

KW - TBK1 ubiquitination

KW - USP38 deubiquitination

KW - innate immune signaling

KW - type I interferon response

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