Nse1-dependent recruitment of Smc5/6 to lesion-containing loci contributes to the repair defects of mutant complexes

Akamatsu Y; Ampatzidou E; Andrews EA; Aono N; Birkenbihl RP; Birkenbihl RP; Branzei D; Broomfield S; Callegari AJ; Callegari AJ; Callegari AJ; Calonge TM; Calonge TM; Chavez A; Chen YH; Claudia Tapia-Alveal; Daigaku Y; Deshpande AM; Doe CL; Doyle JM; Duan X; Duan X; Forsburg S; Fujioka Y; Germe T; Harvey SH; Hirano T; Huang J; Irmisch A; Kai M; Karras GI; Keeney JB; Kegel A; Kunkel TA; Lee KM; Lee KY; Lehmann AR; Lindroos HB; Marti TM; Matthew J. O'Connell; McDonald WH; Memisoglu A; Moreno S; Morishita T; Morishita T; Murray JM; Orna Cohen-Fix; Osman F; Outwin EA; Palecek J; Pebernard S; Pebernard S; Potts PR; Potts PR; Rubio ED; Sergeant J; Sheedy DM; Strom L; Sugimoto T; Sun W; Szilard RK; Szuts D; Tapia-Alveal C; Tatebayashi K; Unal E; Vanoli F; Verkade HM; Wang SW; Wendt KS; Williams JS; Zaratiegui M

Nse1-dependent recruitment of Smc5/6 to lesion-containing loci contributes to the repair defects of mutant complexes

Abstract

The Smc5/6 complex is widely believed to be required for homologous recombination. It is shown that repair defects of Smc5/6 mutants are due to the Nse1-dependent recruitment of dysfunctional complexes to lesions

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Last time updated on 02/01/2020