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Cytostatic sensitivity and MDR in bladder carcinoma cells: implications for tumor therapy. | LitMetric

AI Article Synopsis

  • The study investigates the effectiveness of R-verapamil and linolenic acid in enhancing chemotherapy sensitivity in cisplatin-resistant bladder cancer cells.
  • Results show that R-verapamil significantly boosts the toxic effects of doxorubicin, especially in cells with higher membrane order, while linolenic acid increases sensitivity to both cisplatin and methotrexate.
  • Bile salts were found to have minimal impact on cytotoxicity, suggesting that the mechanisms of action for R-verapamil and linolenic acid may relate to changes in cell membrane fluidity.

Article Abstract

The clinical success generally seen in chemotherapy of advanced bladder carcinoma is far from optimal. The mechanism of resistance development is unclear and the expression of P-170 glycoprotein is generally low. The aim of this study, carried out in vitro in sensitive and cisplatin-resistant cell lines, was to examine sensitivity modulation using R-verapamil and cell membrane perturbing agents. Cell growth rates and changes in the order of the cell membrane, determined using electron-paramagnetic resonance spectrometry, were recorded. R-verapamil increased the toxic effect of doxorubicin in the cisplatin-resistant cell line which showed the highest membrane order. Linolenic acid had a similar effect and also increased sensitivity to cisplatin and methotrexate. Bile salts (tauro-cheno-deoxycholate,TCDC, and tauro-urso-deoxycholate TUDC), had little effect on cytotoxicity. These results indicate that R-verapamil and linolenic acid can act as sensitivity modulators in bladder carcinoma cells and that the action of these agents may involve membrane fluidity changes, a phenomenon noted previously in regard to sensitivity modulation in chinese hamster ovary cell lines.

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Source
http://dx.doi.org/10.5414/cpp38204DOI Listing

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