Key Proteins of Replication Stress Response and Cell Cycle Control as Cancer Therapy Targets

Khamidullina, Alvina I. and Abramenko, Yaroslav E. and Bruter, Alexandra V. and Tatarskiy, Victor V. (2024) Key Proteins of Replication Stress Response and Cell Cycle Control as Cancer Therapy Targets. International Journal of Molecular Sciences, 25 (2). p. 1263. ISSN 1422-0067

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Abstract

Replication stress (RS) is a characteristic state of cancer cells as they tend to exchange precision of replication for fast proliferation and increased genomic instability. To overcome the consequences of improper replication control, malignant cells frequently inactivate parts of their DNA damage response (DDR) pathways (the ATM-CHK2-p53 pathway), while relying on other pathways which help to maintain replication fork stability (ATR-CHK1). This creates a dependency on the remaining DDR pathways, vulnerability to further destabilization of replication and synthetic lethality of DDR inhibitors with common oncogenic alterations such as mutations of TP53, RB1, ATM, amplifications of MYC, CCNE1 and others. The response to RS is normally limited by coordination of cell cycle, transcription and replication. Inhibition of WEE1 and PKMYT1 kinases, which prevent unscheduled mitosis entry, leads to fragility of under-replicated sites. Recent evidence also shows that inhibition of Cyclin-dependent kinases (CDKs), such as CDK4/6, CDK2, CDK8/19 and CDK12/13 can contribute to RS through disruption of DNA repair and replication control. Here, we review the main causes of RS in cancers as well as main therapeutic targets—ATR, CHK1, PARP and their inhibitors.

Item Type: Article
Subjects: Impact Archive > Multidisciplinary
Depositing User: Managing Editor
Date Deposited: 20 Jan 2024 11:45
Last Modified: 20 Jan 2024 11:45
URI: http://research.sdpublishers.net/id/eprint/3848

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