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The triphenyltin carboxylate derivative triphenylstannyl 2-(benzylcarbamoyl)benzoate impedes prostate cancer progression via modulation of Akt/FOXO3a signaling. | LitMetric

AI Article Synopsis

  • Prostate cancer (PCa) rates are rising in the U.S. and globally, leading researchers to investigate various compounds that could inhibit the PI3K/Akt signaling pathway, which is known to promote PCa growth.
  • The compound triphenylstannyl 2-(benzylcarbamoyl)benzoate (Ch-319) was found to reduce cancer cell viability, cause cell cycle arrest, and induce apoptosis in prostate cancer cells, while also enhancing the effectiveness of cabazitaxel, a common treatment for castration-resistant PCa.
  • In animal models, Ch-319 appeared to prevent tumor formation without causing organ toxicity, indicating its potential as a safe and effective anticancer agent targeting the Akt/

Article Abstract

Prostate cancer (PCa) incidence is surging in United States and other parts of the world. Synthetic and natural compounds have been explored as potential modulators of PI3K/Akt signaling that is known to drive PCa growth. Here, we evaluated the efficacy of a series of triphenyltin (IV) carboxylate derivatives against PCa. From this library, triphenylstannyl 2-(benzylcarbamoyl)benzoate (Ch-319) resulted in reduced viability and induction of cell cycle arrest in PTEN PC3M and PTEN DU145 cells. In parallel, downregulation of PI3K p85/p110 subunits, dephosphorylation of Akt-1 and increase in FOXO3a expression were observed. In silico studies indicated binding interactions of Ch-319 within the ATP binding site of Akt-1 at Met, Phe and Glu residues. Elevated po-pulation of apoptotic cells, activation of Bax and reduced Bcl2 expression indicated apoptosis by Ch-319. Pre-sensitization of PCa cells with Ch-319 augmented the effect of cabazitaxel, a commonly used taxane in patients with castration-resistant PCa. Next, in a prostate-specific PTEN mice, Ch-319 showed reduced weights of genitourinary apparatus as compared to DMSO treated controls. Histological studies indicated absence of neoplastic foci in Ch-319 treated prostates. Consistently, dephosphorylation of Akt-1, reduced expression of PRAS40 and androgen receptor and increase in FOXO3a were observed in treated group. Notably, no overt organ toxicity was noted in Ch-319 treated animals. Our studies identify Akt/FOXO3a signaling as a target of triphenyltin (IV) carboxylate Ch-319 and provide a molecular basis of its growth inhibitory effect in PCa cells. We propose that Ch-319 has the potential to be developed as an anticancer agent against PCa.

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Source
http://dx.doi.org/10.1016/j.taap.2020.115091DOI Listing

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