AI Article Synopsis
- - GSDME is a newly identified player in pyroptosis (a form of programmed cell death) that may influence both tumor growth and immune responses, but details on how it's regulated are still unclear.
- - Research revealed a positive correlation between GSDME levels and epithelial-mesenchymal transition (EMT) gene signatures in various human cancers, with key EMT factors (ZEB1/2) directly activating GSDME expression.
- - The study suggests that high GSDME levels can lead to cell death and inflammation when cancer cells are treated with anti-cancer drugs, indicating that targeting GSDME could be a promising therapeutic strategy for certain types of cancer.
Article Abstract
GSDME is a newly recognized executor of cellular pyroptosis, and has been recently implicated in tumor growth and immunity. However, knowledge about the molecular regulators underlying GSDME abundance remains limited. Here, we performed integrative bioinformatics analyses and identified that epithelial-mesenchymal transition (EMT) gene signatures exhibited positive correlation with GSDME levels across human cancers. A causal role was supported by the observation that EMT dictated GSDME reversible upregulation in multiple experimental models. Mechanistically, transcriptional activation of was directly driven by core EMT-activating transcription factors ZEB1/2, which bound to the promoter region. Of functional importance, elevated GSDME in mesenchymally transdifferentiated derivatives underwent proteolytic cleavage upon antineoplastic drug exposure, leading to pyroptotic cell death and consequent cytokine release. Taken together, our findings pinpointed a key transcriptional machinery controlling GSDME expression and indicated potential therapeutic avenues to exploit GSDME-mediated inflammatory pyroptosis for the treatment of mesenchymal malignancies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8660972 | PMC |
| http://dx.doi.org/10.3389/fcell.2021.781365 | DOI Listing |
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