| Literature DB >> 33591315 |
Ekaterina Akimova1,2,3, Franz Josef Gassner1,2, Maria Schubert1,2, Stefan Rebhandl1,2, Claudia Arzt1,2, Stefanie Rauscher1,2,3, Vanessa Tober1,2,3, Nadja Zaborsky1,2, Richard Greil1,2, Roland Geisberger1,2.
Abstract
Aberrant end joining of DNA double strand breaks leads to chromosomal rearrangements and to insertion of nuclear or mitochondrial DNA into breakpoints, which is commonly observed in cancer cells and constitutes a major threat to genome integrity. However, the mechanisms that are causative for these insertions are largely unknown. By monitoring end joining of different linear DNA substrates introduced into HEK293 cells, as well as by examining end joining of CRISPR/Cas9 induced DNA breaks in HEK293 and HeLa cells, we provide evidence that the dNTPase activity of SAMHD1 impedes aberrant DNA resynthesis at DNA breaks during DNA end joining. Hence, SAMHD1 expression or low intracellular dNTP levels lead to shorter repair joints and impede insertion of distant DNA regions prior end repair. Our results reveal a novel role for SAMHD1 in DNA end joining and provide new insights into how loss of SAMHD1 may contribute to genome instability and cancer development.Entities:
Year: 2021 PMID: 33591315 PMCID: PMC7969033 DOI: 10.1093/nar/gkab051
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971