| Literature DB >> 29670289 |
Flavie Coquel1, Maria-Joao Silva1,2, Hervé Técher3, Karina Zadorozhny4, Sushma Sharma5, Jadwiga Nieminuszczy6, Clément Mettling7, Elodie Dardillac8, Antoine Barthe1, Anne-Lyne Schmitz1, Alexy Promonet1, Alexandra Cribier9, Amélie Sarrazin10, Wojciech Niedzwiedz6, Bernard Lopez8, Vincenzo Costanzo3, Lumir Krejci4,11, Andrei Chabes5, Monsef Benkirane9, Yea-Lih Lin12, Philippe Pasero13.
Abstract
SAMHD1 was previously characterized as a dNTPase that protects cells from viral infections. Mutations in SAMHD1 are implicated in cancer development and in a severe congenital inflammatory disease known as Aicardi-Goutières syndrome. The mechanism by which SAMHD1 protects against cancer and chronic inflammation is unknown. Here we show that SAMHD1 promotes degradation of nascent DNA at stalled replication forks in human cell lines by stimulating the exonuclease activity of MRE11. This function activates the ATR-CHK1 checkpoint and allows the forks to restart replication. In SAMHD1-depleted cells, single-stranded DNA fragments are released from stalled forks and accumulate in the cytosol, where they activate the cGAS-STING pathway to induce expression of pro-inflammatory type I interferons. SAMHD1 is thus an important player in the replication stress response, which prevents chronic inflammation by limiting the release of single-stranded DNA from stalled replication forks.Entities:
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Year: 2018 PMID: 29670289 DOI: 10.1038/s41586-018-0050-1
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962