AI Article Synopsis
- Senescence, which is a biological response to prevent cancer cell growth, can be triggered by chemotherapy but is not always effective, allowing some cancer cells to adapt and become more aggressive.
- Recent studies reveal that an incomplete senescence response contributes significantly to chemotherapy resistance, enabling a subpopulation of cells to survive and potentially proliferate again.
- Understanding the diverse responses of senescent cells in transformed tissues is crucial for improving therapeutic strategies and preventing cancer recurrence.
Article Abstract
Senescence is activated in response to chemotherapy to prevent the propagation of cancer cells. In transformed cells, recent studies have shown that this response is not always definitive and that persistent populations can use senescence as an adaptive pathway to restart proliferation and become more aggressive. Here we discuss the results showing that an incomplete and heterogeneous senescence response plays a key role in chemotherapy resistance. Surviving to successive chemotherapy regimens, chronically existing senescent cells can create a survival niche through paracrine cooperations with neighboring cells. This favors chemotherapy escape of premalignant clones but might also allow the survival of adjacent clones presenting a lower fitness. A better characterization of senescence heterogeneity in transformed cells is therefore necessary. This will help us to understand this incomplete response to therapy and how it could generate clones with increased tumor capacity leading to disease relapse.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6738909 | PMC |
| http://dx.doi.org/10.1080/15384101.2019.1652047 | DOI Listing |
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