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Co-inhibition of ATM and ROCK synergistically improves cell proliferation in replicative senescence by activating FOXM1 and E2F1
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- Title
- Co-inhibition of ATM and ROCK synergistically improves cell proliferation in replicative senescence by activating FOXM1 and E2F1
- Issued Date
- 2022-07
- Citation
- Yang, Eun Jae. (2022-07). Co-inhibition of ATM and ROCK synergistically improves cell proliferation in replicative senescence by activating FOXM1 and E2F1. Communications Biology, 5(1). doi: 10.1038/s42003-022-03658-5
- Type
- Article
- Keywords
- SECRETORY PHENOTYPE ; DNA-REPLICATION ; LIFE-SPAN ; EXPRESSION ; TARGET ; INVOLVEMENT ; INTERACTS ; PATHWAYS ; LEVEL ; AXIS
- ISSN
- 2399-3642
- Abstract
-
The multifaceted nature of senescent cell cycle arrest necessitates the targeting of multiple factors arresting or promoting the cell cycle. We report that co-inhibition of ATM and ROCK by KU-60019 and Y-27632, respectively, synergistically increases the proliferation of human diploid fibroblasts undergoing replicative senescence through activation of the transcription factors E2F1 and FOXM1. Time-course transcriptome analysis identified FOXM1 and E2F1 as crucial factors promoting proliferation. Co-inhibition of the kinases ATM and ROCK first promotes the G2/M transition via FOXM1 activation, leading to accumulation of cells undergoing the G1/S transition via E2F1 activation. The combination of both inhibitors increased this effect more significantly than either inhibitor alone, suggesting synergism. Our results demonstrate a FOXM1- and E2F1-mediated molecular pathway enhancing cell cycle progression in cells with proliferative potential under replicative senescence conditions, and treatment with the inhibitors can be tested for senomorphic effect in vivo. © 2022, The Author(s).
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- Publisher
- Nature Publishing Group
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