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Recruitment of Saccharomyces cerevisiae Dnl4-Lif1 complex to a double-strand break requires interactions with Yku80 and the Xrs2 FHA domain

Authors :
Palmbos, Phillip L.
Wu, Dongliang
Daley, James M.
Wilson, Thomas E.
Source :
Genetics. Dec, 2008, Vol. 180 Issue 4, p1809, 11 p.
Publication Year :
2008

Abstract

Nonhomologous end joining (NHEJ) in yeast depends on eight different proteins in at least three different functional complexes: Yku70--Yku80 (Ku), Dnl4--Lif1--Nej1 (DNA ligase IV), and Mre11--Rad50--Xrs2 (MRX). Interactions between these complexes at DNA double-strand breaks (DSBs) are poorly understood but critical for the completion of repair. We previously identified two such contacts that are redundantly required for NHEJ, one between Dnl4 and the C terminus of Yku80 and one between the forkhead-associated (FHA) domain of Xrs2 and the C terminus of Lif1. Here, we first show that mutation of the Yku80 C terminus did not impair Ku binding to DSBs, supporting specificity of the mutant defect to the ligase interaction. We next show that the Xrs2--Lif1 interaction depends on Xrs2 FHA residues (R32, S47, R48, and K75) analogous to those known in other proteins to contact phosphorylated threonines. Two potential target threonines in Lif1 (T417 and T387) were inferred by identifying regions similar to a site in the human Lif1 homolog, XRCC4, known to be bound by the FHA domain of polynucleotide kinase. Mutating these threonines, especially T417, abolished the Xrs2--Lif1 interaction and impaired NHEJ epistatically with Xrs2 FHA mutation. Combining mutations that selectively disable the Yku80--Dnl4 and Xrs2--Lifl interactions abrogated both NHEJ and DNA ligase IV recruitment to a DSB. The collected results indicate that the Xrs--Lif1 and Yku80--Dnl4 interactions are important for formation of a productive ligase--DSB intermediate.

Details

Language :
English
ISSN :
00166731
Volume :
180
Issue :
4
Database :
Gale General OneFile
Journal :
Genetics
Publication Type :
Academic Journal
Accession number :
edsgcl.191646646