| Literature DB >> 35247630 |
Sajjad Vakili-Samiani1, Omid Joodi Khanghah2, Elham Gholipour3, Fatemeh Najafi4, Elham Zeinalzadeh3, Parisa Samadi5, Parisa Sarvarian6, Shiva Pourvahdani3, Shohre Karimi Kelaye6, Michael R Hamblin7, Abbas Ali Hosseinpour Feizi8.
Abstract
Mitosis is the process of cell division and is regulated by checkpoints in the cell cycle. G1-S, S, and G2-M are the three main checkpoints that prevent initiation of the next phase of the cell cycle phase until previous phase has completed. DNA damage leads to activation of the G2-M checkpoint, which can trigger a downstream DNA damage response (DDR) pathway to induce cell cycle arrest while the damage is repaired. If the DNA damage cannot be repaired, the replication stress response (RSR) pathway finally leads to cell death by apoptosis, in this case called mitotic catastrophe. Many cancer treatments (chemotherapy and radiotherapy) cause DNA damages based on SSBs (single strand breaks) or DSBs (double strand breaks), which cause cell death through mitotic catastrophe. However, damaged cells can activate WEE1 kinase (as a part of the DDR and RSR pathways), which prevents apoptosis and cell death by inducing cell cycle arrest at G2 phase. Therefore, inhibition of WEE1 kinase could sensitize cancer cells to chemotherapeutic drugs. This review focuses on the role of WEE1 kinase (as a biological macromolecule which has a molecular mass of 96 kDa) in the cell cycle, and its interactions with other regulatory pathways. In addition, we discuss the potential of WEE1 inhibition as a new therapeutic approach in the treatment of various cancers, such as melanoma, breast cancer, pancreatic cancer, cervical cancer, etc.Entities:
Keywords: Cancer; Cell cycle; Checkpoint; DNA damage; WEE1 kinase
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Year: 2022 PMID: 35247630 DOI: 10.1016/j.mrfmmm.2022.111776
Source DB: PubMed Journal: Mutat Res ISSN: 0027-5107 Impact factor: 2.433