ELOF1 is a transcription-coupled DNA repair factor that directs RNA polymerase II ubiquitylation

ELOF1 是一种转录偶联的 DNA 修复因子,可指导 RNA 聚合酶 II 的泛素化。

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作者:Yana van der Weegen # ,Klaas de Lint # ,Diana van den Heuvel ,Yuka Nakazawa ,Tycho E T Mevissen ,Janne J M van Schie ,Marta San Martin Alonso ,Daphne E C Boer ,Román González-Prieto ,Ishwarya V Narayanan ,Noud H M Klaassen ,Annelotte P Wondergem ,Khashayar Roohollahi ,Josephine C Dorsman ,Yuichiro Hara ,Alfred C O Vertegaal ,Job de Lange ,Johannes C Walter ,Sylvie M Noordermeer ,Mats Ljungman ,Tomoo Ogi ,Rob M F Wolthuis ,Martijn S Luijsterburg

Abstract

Cells employ transcription-coupled repair (TCR) to eliminate transcription-blocking DNA lesions. DNA damage-induced binding of the TCR-specific repair factor CSB to RNA polymerase II (RNAPII) triggers RNAPII ubiquitylation of a single lysine (K1268) by the CRL4CSA ubiquitin ligase. How CRL4CSA is specifically directed towards K1268 is unknown. Here, we identify ELOF1 as the missing link that facilitates RNAPII ubiquitylation, a key signal for the assembly of downstream repair factors. This function requires its constitutive interaction with RNAPII close to K1268, revealing ELOF1 as a specificity factor that binds and positions CRL4CSA for optimal RNAPII ubiquitylation. Drug-genetic interaction screening also revealed a CSB-independent pathway in which ELOF1 prevents R-loops in active genes and protects cells against DNA replication stress. Our study offers key insights into the molecular mechanisms of TCR and provides a genetic framework of the interplay between transcriptional stress responses and DNA replication.

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