AI Article Synopsis
- Epithelial transdifferentiation, like squamous metaplasia (SQM), often occurs in tissue hyperplasia and can lead to diseases, with SQM being a precursor to aggressive lung cancer but less common in mammary glands.
- Research conducted on human lung and mammary cells reveals that exposure to genotoxic drugs, such as Doxorubicin and carcinogens like DMBA, can trigger SQM and polyploidization, suggesting a link between DNA damage and this cellular change.
- Enhancing DNA repair or inhibiting specific mitotic checkpoints reduces the extent of SQM, highlighting potential targets for treatments aimed at lung squamous cell carcinoma and explaining the frequency of SCC in the
Article Abstract
Epithelial transdifferentiation is frequent in tissue hyperplasia and contributes to disease in various degrees. Squamous metaplasia (SQM) precedes epidermoid lung cancer, an aggressive and frequent malignancy, but it is rare in the epithelium of the mammary gland. The mechanisms leading to SQM in the lung have been very poorly investigated. We have studied this issue on human freshly isolated cells and organoids. Here we show that human lung or mammary cells strikingly undergo SQM with polyploidisation when they are exposed to genotoxic or mitotic drugs, such as Doxorubicin or the cigarette carcinogen DMBA, Nocodazole, Taxol or inhibitors of Aurora-B kinase or Polo-like kinase. To note, the epidermoid response was attenuated when DNA repair was enhanced by Enoxacin or when mitotic checkpoints where abrogated by inhibition of Chk1 and Chk2. The results show that DNA damage has the potential to drive SQM via mitotic checkpoints, thus providing novel molecular candidate targets to tackle lung SCC. Our findings might also explain why SCC is frequent in the lung, but not in the mammary gland and why chemotherapy often causes complicating skin toxicity.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9867756 | PMC |
| http://dx.doi.org/10.1038/s41420-023-01330-3 | DOI Listing |
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