USP39 promotes non-homologous end-joining repair by poly(ADP-ribose)-induced liquid demixing

Jae Jin Kim; Seo Yun Lee; Yiseul Hwang; Soyeon Kim; Jee Min Chung; Sangwook Park; Junghyun Yoon; Hansol Yun; Jae Hoon Ji; Sunyoung Chae; Hyeseong Cho; Chan Gil Kim; Ted M. Dawson; Hongtae Kim; Valina L. Dawson; Ho Chul Kang

doi:10.1093/nar/gkab892

USP39 promotes non-homologous end-joining repair by poly(ADP-ribose)-induced liquid demixing

Jae Jin Kim, Seo Yun Lee, Yiseul Hwang, Soyeon Kim, Jee Min Chung, Sangwook Park, Junghyun Yoon, Hansol Yun, Jae Hoon Ji, Sunyoung Chae, Hyeseong Cho, Chan Gil Kim, Ted M. Dawson, Hongtae Kim, Valina L. Dawson, Ho Chul Kang

School of Medicine

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

Abstract

Mutual crosstalk among poly(ADP-ribose) (PAR), activated PAR polymerase 1 (PARP1) metabolites, and DNA repair machinery has emerged as a key regulatory mechanism of the DNA damage response (DDR). However, there is no conclusive evidence of how PAR precisely controls DDR. Herein, six deubiquitinating enzymes (DUBs) associated with PAR-coupled DDR were identified, and the role of USP39, an inactive DUB involved in spliceosome assembly, was characterized. USP39 rapidly localizes to DNA lesions in a PAR-dependent manner, where it regulates non-homologous end-joining (NHEJ) via a tripartite RG motif located in the N-terminus comprising 46 amino acids (N46). Furthermore, USP39 acts as a molecular trigger for liquid demixing in a PAR-coupled N46-dependent manner, thereby directly interacting with the XRCC4/LIG4 complex during NHEJ. In parallel, the USP39-associated spliceosome complex controls homologous recombination repair in a PAR-independent manner. These findings provide mechanistic insights into how PAR chains precisely control DNA repair processes in the DDR.

Original language	English (US)
Pages (from-to)	11083-11102
Number of pages	20
Journal	Nucleic acids research
Volume	49
Issue number	19
DOIs	https://doi.org/10.1093/nar/gkab892
State	Published - Nov 8 2021

ASJC Scopus subject areas

Genetics

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@article{b08734f44d784a6a9136e5cfe52d3b53,

title = "USP39 promotes non-homologous end-joining repair by poly(ADP-ribose)-induced liquid demixing",

abstract = "Mutual crosstalk among poly(ADP-ribose) (PAR), activated PAR polymerase 1 (PARP1) metabolites, and DNA repair machinery has emerged as a key regulatory mechanism of the DNA damage response (DDR). However, there is no conclusive evidence of how PAR precisely controls DDR. Herein, six deubiquitinating enzymes (DUBs) associated with PAR-coupled DDR were identified, and the role of USP39, an inactive DUB involved in spliceosome assembly, was characterized. USP39 rapidly localizes to DNA lesions in a PAR-dependent manner, where it regulates non-homologous end-joining (NHEJ) via a tripartite RG motif located in the N-terminus comprising 46 amino acids (N46). Furthermore, USP39 acts as a molecular trigger for liquid demixing in a PAR-coupled N46-dependent manner, thereby directly interacting with the XRCC4/LIG4 complex during NHEJ. In parallel, the USP39-associated spliceosome complex controls homologous recombination repair in a PAR-independent manner. These findings provide mechanistic insights into how PAR chains precisely control DNA repair processes in the DDR.",

author = "Kim, {Jae Jin} and Lee, {Seo Yun} and Yiseul Hwang and Soyeon Kim and Chung, {Jee Min} and Sangwook Park and Junghyun Yoon and Hansol Yun and Ji, {Jae Hoon} and Sunyoung Chae and Hyeseong Cho and Kim, {Chan Gil} and Dawson, {Ted M.} and Hongtae Kim and Dawson, {Valina L.} and Kang, {Ho Chul}",

note = "Publisher Copyright: {\textcopyright} 2021 The Author(s). Published by Oxford University Press on behalf of Nucleic Acids Research.",

year = "2021",

month = nov,

day = "8",

doi = "10.1093/nar/gkab892",

language = "English (US)",

volume = "49",

pages = "11083--11102",

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T1 - USP39 promotes non-homologous end-joining repair by poly(ADP-ribose)-induced liquid demixing

AU - Kim, Jae Jin

AU - Lee, Seo Yun

AU - Hwang, Yiseul

AU - Kim, Soyeon

AU - Chung, Jee Min

AU - Park, Sangwook

AU - Yoon, Junghyun

AU - Yun, Hansol

AU - Ji, Jae Hoon

AU - Chae, Sunyoung

AU - Cho, Hyeseong

AU - Kim, Chan Gil

AU - Dawson, Ted M.

AU - Kim, Hongtae

AU - Dawson, Valina L.

AU - Kang, Ho Chul

PY - 2021/11/8

Y1 - 2021/11/8

N2 - Mutual crosstalk among poly(ADP-ribose) (PAR), activated PAR polymerase 1 (PARP1) metabolites, and DNA repair machinery has emerged as a key regulatory mechanism of the DNA damage response (DDR). However, there is no conclusive evidence of how PAR precisely controls DDR. Herein, six deubiquitinating enzymes (DUBs) associated with PAR-coupled DDR were identified, and the role of USP39, an inactive DUB involved in spliceosome assembly, was characterized. USP39 rapidly localizes to DNA lesions in a PAR-dependent manner, where it regulates non-homologous end-joining (NHEJ) via a tripartite RG motif located in the N-terminus comprising 46 amino acids (N46). Furthermore, USP39 acts as a molecular trigger for liquid demixing in a PAR-coupled N46-dependent manner, thereby directly interacting with the XRCC4/LIG4 complex during NHEJ. In parallel, the USP39-associated spliceosome complex controls homologous recombination repair in a PAR-independent manner. These findings provide mechanistic insights into how PAR chains precisely control DNA repair processes in the DDR.

AB - Mutual crosstalk among poly(ADP-ribose) (PAR), activated PAR polymerase 1 (PARP1) metabolites, and DNA repair machinery has emerged as a key regulatory mechanism of the DNA damage response (DDR). However, there is no conclusive evidence of how PAR precisely controls DDR. Herein, six deubiquitinating enzymes (DUBs) associated with PAR-coupled DDR were identified, and the role of USP39, an inactive DUB involved in spliceosome assembly, was characterized. USP39 rapidly localizes to DNA lesions in a PAR-dependent manner, where it regulates non-homologous end-joining (NHEJ) via a tripartite RG motif located in the N-terminus comprising 46 amino acids (N46). Furthermore, USP39 acts as a molecular trigger for liquid demixing in a PAR-coupled N46-dependent manner, thereby directly interacting with the XRCC4/LIG4 complex during NHEJ. In parallel, the USP39-associated spliceosome complex controls homologous recombination repair in a PAR-independent manner. These findings provide mechanistic insights into how PAR chains precisely control DNA repair processes in the DDR.

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USP39 promotes non-homologous end-joining repair by poly(ADP-ribose)-induced liquid demixing

Abstract

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