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The RECQL helicase prevents replication fork collapse during replication stress.


ABSTRACT: Most tumors lack the G1/S phase checkpoint and are insensitive to antigrowth signals. Loss of G1/S control can severely perturb DNA replication as revealed by slow replication fork progression and frequent replication fork stalling. Cancer cells may thus rely on specific pathways that mitigate the deleterious consequences of replication stress. To identify vulnerabilities of cells suffering from replication stress, we performed an shRNA-based genetic screen. We report that the RECQL helicase is specifically essential in replication stress conditions and protects stalled replication forks against MRE11-dependent double strand break (DSB) formation. In line with these findings, knockdown of RECQL in different cancer cells increased the level of DNA DSBs. Thus, RECQL plays a critical role in sustaining DNA synthesis under conditions of replication stress and as such may represent a target for cancer therapy.

SUBMITTER: Benedict B 

PROVIDER: S-EPMC7441523 | biostudies-literature | 2020 Oct

REPOSITORIES: biostudies-literature

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The RECQL helicase prevents replication fork collapse during replication stress.

Benedict Bente B   van Bueren Marit Ae MA   van Gemert Frank Pa FP   Lieftink Cor C   Guerrero Llobet Sergi S   van Vugt Marcel Atm MA   Beijersbergen Roderick L RL   Te Riele Hein H  

Life science alliance 20200820 10


Most tumors lack the G1/S phase checkpoint and are insensitive to antigrowth signals. Loss of G1/S control can severely perturb DNA replication as revealed by slow replication fork progression and frequent replication fork stalling. Cancer cells may thus rely on specific pathways that mitigate the deleterious consequences of replication stress. To identify vulnerabilities of cells suffering from replication stress, we performed an shRNA-based genetic screen. We report that the RECQL helicase is  ...[more]

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