DNA binding modes influence Rap1 activity in the regulation of telomere length and MRX functions at DNA ends

Author:

Bonetti Diego1,Rinaldi Carlo1,Vertemara Jacopo1,Notaro Marco1,Pizzul Paolo1,Tisi Renata1,Zampella Giuseppe1,Longhese Maria Pia1ORCID

Affiliation:

1. Dipartimento di Biotecnologie e Bioscienze, Università degli Studi di Milano – Bicocca, 20126 Milano, Italy

Abstract

AbstractThe cellular response to DNA double-strand breaks (DSBs) is initiated by the Mre11–Rad50–Xrs2 (MRX) complex that has structural and catalytic functions. MRX association at DSBs is counteracted by Rif2, which is known to interact with Rap1 that binds telomeric DNA through two tandem Myb-like domains. Whether and how Rap1 acts at DSBs is unknown. Here we show that Rif2 inhibits MRX association to DSBs in a manner dependent on Rap1, which binds to DSBs and promotes Rif2 association to them. Rap1 in turn can negatively regulate MRX function at DNA ends also independently of Rif2. In fact, a characterization of Rap1 mutant variants shows that Rap1 binding to DNA through both Myb-like domains results in formation of Rap1-DNA complexes that control MRX functions at both DSBs and telomeres primarily through Rif2. By contrast, Rap1 binding to DNA through a single Myb-like domain results in formation of high stoichiometry complexes that act at DNA ends mostly in a Rif2-independent manner. Altogether these findings indicate that the DNA binding modes of Rap1 influence its functional properties, thus highlighting the structural plasticity of this protein.

Funder

AIRC

Progetti di Ricerca di Interesse Nazionale

MIUR

Publisher

Oxford University Press (OUP)

Subject

Genetics

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3. Telomere maintenance in African trypanosomes;Frontiers in Molecular Biosciences;2023-11-24

4. Dynamic Properties of the DNA Damage Response Mre11/Rad50 Complex;International Journal of Molecular Sciences;2023-08-03

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