Genetics. Published Articles Ahead of Print: February 1, 2008, Copyright © 2008
doi:10.1534/genetics.107.081331


A more recent version of this article appeared on February 1, 2008.

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Functional interactions between Sae2 and the Mre11 complex

Hee-Sook Kim 1, Sangeetha Vijayakumar 2, Mike Reger 3, Jake Harrison 4, James E Haber 4, Cliff Weil 3 and John H.J. Petrini 2*

1 Rockefeller University
2 Memorial Sloan-Kettering Cancer Center
3 Purdue University
4 Brandeis University

* To whom correspondence should be addressed. E-mail: petrinij{at}mskcc.org.

Submitted on August 30, 2007
Revised on October 15, 2007
Accepted on 18 December 2007


Abstract

The Mre11 complex functions in double strand break (DSB) repair, meiotic recombination and DNA damage checkpoint pathways. Sae2 deficiency has opposing effects on the Mre11 complex. On one hand, it appears to impair Mre11 nuclease function in DNA repair and meiotic DSB processing, and on the other, Sae2 deficiency activates Mre11 complex-dependent DNA damage signaling via the Tel1-Mre11 complex (TM) pathway. We demonstrate that SAE2 overexpression blocks the TM pathway, suggesting that Sae2 antagonizes Mre11 complex checkpoint functions. To understand how Sae2 regulates the Mre11 complex, we screened for sae2 alleles that behaved as the null with respect to Mre11 complex checkpoint functions, but left nuclease function intact. Phenotypic characterization of these sae2 alleles suggests that Sae2 functions as a multimer and influences the substrate specificity of the Mre11 nuclease. We show that Sae2 oligomerizes independently of DNA damage and that oligomerization is required for its regulatory influence on the Mre11 nuclease and checkpoint functions.

Key Words: DNA damage response, Hairpin processing, Mre11 complex, Sae2, Sae2 oligomerization