Interaction of human HelQ with DNA polymerase delta halts DNA synthesis and stimulates DNA single-strand annealing

Author:

He Liu1,Lever Rebecca1,Cubbon Andrew1,Tehseen Muhammad2,Jenkins Tabitha1,Nottingham Alice O1,Horton Anya1,Betts Hannah3,Fisher Martin4,Hamdan Samir M2ORCID,Soultanas Panos3,Bolt Edward L1ORCID

Affiliation:

1. School of Life Sciences, University of Nottingham , Nottingham, UK

2. Bioscience Program, Biological and Environmental Science and Engineering, King Abdullah University of Science and Technology (KAUST) , Thuwal , Saudi Arabia

3. Biodiscovery Institute, School of Chemistry, University of Nottingham , Nottingham, UK

4. Nanna Therapeutics , Cambridge , UK

Abstract

AbstractDNA strand breaks are repaired by DNA synthesis from an exposed DNA end paired with a homologous DNA template. DNA polymerase delta (Pol δ) catalyses DNA synthesis in multiple eukaryotic DNA break repair pathways but triggers genome instability unless its activity is restrained. We show that human HelQ halts DNA synthesis by isolated Pol δ and Pol δ-PCNA-RPA holoenzyme. Using novel HelQ mutant proteins we identify that inhibition of Pol δ is independent of DNA binding, and maps to a 70 amino acid intrinsically disordered region of HelQ. Pol δ and its POLD3 subunit robustly stimulated DNA single-strand annealing by HelQ, and POLD3 and HelQ interact physically via the intrinsically disordered HelQ region. This data, and inability of HelQ to inhibit DNA synthesis by the POLD1 catalytic subunit of Pol δ, reveal a mechanism for limiting DNA synthesis and promoting DNA strand annealing during human DNA break repair, which centres on POLD3.

Funder

Nanna Therapeutics, Cambridge, U.K.

BBSRC

King Abdullah University of Science and Technology

BBSRC DTP

University of Nottingham School of Chemistry

Publisher

Oxford University Press (OUP)

Subject

Genetics

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