SUMO fosters assembly and functionality of the MutSγ complex to facilitate meiotic crossing over

Wei He; Gerrik F. Verhees; Nikhil Bhagwat; Ye Yang; Dhananjaya S. Kulkarni; Zane Lombardo; Sudipta Lahiri; Pritha Roy; Jiaming Zhuo; Brian Dang; Andriana Snyder; Shashank Shastry; Michael Moezpoor; Lilly Alocozy; Kathy Gyehyun Lee; Daniel Painter; Ishita Mukerji; Neil Hunter

doi:10.1016/j.devcel.2021.06.012

SUMO fosters assembly and functionality of the MutSγ complex to facilitate meiotic crossing over

Publikation: Beitrag in Fachzeitschrift › Forschungsartikel › Beigetragen › Begutachtung

Beitragende

Wei He - , University of California at Davis (Autor:in)
Gerrik F. Verhees - , Institut für Physiologische Chemie, University of California at Davis (Autor:in)
Nikhil Bhagwat - , University of California at Davis (Autor:in)
Ye Yang - , University of California at Davis (Autor:in)
Dhananjaya S. Kulkarni - , University of California at Davis (Autor:in)
Zane Lombardo - , Wesleyan University (Autor:in)
Sudipta Lahiri - , Wesleyan University (Autor:in)
Pritha Roy - , University of California at Davis (Autor:in)
Jiaming Zhuo - , University of California at Davis (Autor:in)
Brian Dang - , University of California at Davis (Autor:in)
Andriana Snyder - , University of California at Davis (Autor:in)
Shashank Shastry - , University of California at Davis (Autor:in)
Michael Moezpoor - , University of California at Davis (Autor:in)
Lilly Alocozy - , University of California at Davis (Autor:in)
Kathy Gyehyun Lee - , University of California at Davis (Autor:in)
Daniel Painter - , University of California at Davis (Autor:in)
Ishita Mukerji - , Wesleyan University (Autor:in)
Neil Hunter - , University of California at Davis (Autor:in)

Abstract

Crossing over is essential for chromosome segregation during meiosis. Protein modification by SUMO is implicated in crossover control, but pertinent targets have remained elusive. Here we identify Msh4 as a target of SUMO-mediated crossover regulation. Msh4 and Msh5 constitute the MutSγ complex, which stabilizes joint-molecule (JM) recombination intermediates and facilitates their resolution into crossovers. Msh4 SUMOylation enhances these processes to ensure that each chromosome pair acquires at least one crossover. Msh4 is directly targeted by E2 conjugase Ubc9, initially becoming mono-SUMOylated in response to DNA double-strand breaks, then multi/poly-SUMOylated forms arise as homologs fully engage. Mechanistically, SUMOylation fosters interaction between Msh4 and Msh5. We infer that initial SUMOylation of Msh4 enhances assembly of MutSγ in anticipation of JM formation, while secondary SUMOylation may promote downstream functions. Regulation of Msh4 by SUMO is distinct and independent of its previously described stabilization by phosphorylation, defining MutSγ as a hub for crossover control.

Details

Originalsprache	Englisch
Seiten (von - bis)	2073-2088.e3
Fachzeitschrift	Developmental cell
Jahrgang	56
Ausgabenummer	14
Publikationsstatus	Veröffentlicht - 26 Juli 2021
Peer-Review-Status	Ja

Externe IDs

PubMed	34214491
ORCID	/0000-0002-6808-2968/work/158767973

Schlagworte

ASJC Scopus Sachgebiete

Molekularbiologie
Allgemeine Biochemie, Genetik und Molekularbiologie
Entwicklungsbiologie
Zellbiologie

Schlagwörter

aneuploidy, chromosome segregation, crossing over, DNA repair, double-strand break, homologous recombination, meiosis, MutS, protein modification, SUMO

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