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Thermal Proteome Profiling Strategy Identifies CNPY3 as a Cellular Target of Gambogic Acid for Inducing Prostate Cancer Pyroptosis.

Xiao-Wen ZhangLing LiMin LiaoDan LiuAsma RehmanYang LiuZheng-Ping LiuPeng-Fei TuKe-Wu Zeng
Published in: Journal of medicinal chemistry (2024)
There is an urgent requirement to acquire a comprehensive comprehension of novel therapeutic targets for prostate cancer to facilitate the development of medications with innovative mechanisms. In this study, we identified gambogic acid (GBA) as a specific pyroptosis inducer in prostatic cancer cells. By using a thermal proteome profiling (TPP) strategy, we revealed that GBA induces pyroptosis by directly targeting the canopy FGF signaling regulator (CNPY3), which was previously considered "undruggable". Moreover, through the utilization of the APEX2-based proximity labeling method, we found that GBA recruited delactatease SIRT1, resulting in the elimination of lysine lactylation (Kla) on CNPY3. Of note, SIRT1-mediated delactylation influenced the cellular localization of CNPY3 to promote lysosome rupture for triggering pyroptosis. Taken together, our study identified CNPY3 as a distinctive cellular target for pyroptosis induction and its potential application in prostate cancer therapy.
Keyphrases
  • prostate cancer
  • nlrp inflammasome
  • cancer therapy
  • radical prostatectomy
  • single cell
  • oxidative stress
  • drug delivery
  • genome wide
  • transcription factor
  • ischemia reperfusion injury
  • benign prostatic hyperplasia