Cnd2 Has Dual Roles in Mitotic Condensation and Interphase

Overview

Journal Nature

Specialty Science

Date 2002 May 10

PMID 12000964

Citations 78

Authors

Nobuki Aono

Takashi Sutani

Takeshi Tomonaga

Satoru Mochida

Mitsuhiro Yanagida

Affiliations

Soon will be listed here.

Abstract

Chromosome condensation requires condensin, which comprises five subunits. Two of these subunits--both being structural maintenance of chromosome (SMC) proteins-are coiled-coils with globular terminal domains that interact with ATP and DNA. The remaining three, non-SMC subunits also have essential, albeit undefined, roles in condensation. Here we report that Cnd2 (ref. 6), a non-SMC subunit of fission yeast similar to Drosophila Barren and the budding yeast protein Brn1 (refs 8, 9), is required for both interphase and mitotic condensation. In cnd2-1 mutants, ultraviolet-induced DNA damage is not repaired, and cells arrested by hydroxyurea do not recover. A definitive defect of interphase is abolishment of Cds1 (a checkpoint kinase) activation in the presence of hydroxyurea in both cnd2-1 mutant cells and in cells where other condensin subunits have been genetically disrupted. In the absence of hydroxyurea, a G2 checkpoint delay occurred in cnd2-1 mutants in a manner dependent on Cds1 and ATM-like Rad3, but not Chk1 (refs 10-13), before the mitotic condensation defect. Furthermore, cnd2-1 was synthetic-lethal with mutations of excision repair, RecQ helicase and DNA replication enzymes. These interphase and mitotic defects provide insight into the mechanistic role of non-SMC subunits that interact with the globular SMC domains in the heteropentameric holocomplex.

Citing Articles

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Potential roles of condensin in genome organization and beyond in fission yeast.

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Comparison of loop extrusion and diffusion capture as mitotic chromosome formation pathways in fission yeast.

Gerguri T, Fu X, Kakui Y, Khatri B, Barrington C, Bates P Nucleic Acids Res. 2021; 49(3):1294-1312.

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Fission yeast condensin contributes to interphase chromatin organization and prevents transcription-coupled DNA damage.

Kakui Y, Barrington C, Barry D, Gerguri T, Fu X, Bates P Genome Biol. 2020; 21(1):272.

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