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Comparison of anti-cancer effects of novel protein disulphide isomerase (PDI) inhibitors in breast cancer cells characterized by high and low PDIA17 expression.

Anna KurpinskaJoanna Suraj-PrażmowskaMarta StojakJoanna JaroszŁukasz MateuszukEwa Niedzielska-AndresMagdalena SmolikJoanna WietrzykIvars KalvinsMaria WalczakStefan Chlopicki
Published in: Cancer cell international (2022)
PDIA1 and PDIA3 represent major isoforms of multiple cancer cells, and their non-selective inhibition displays significant anti-proliferative effects irrespective of whether or not PDIA17 is present. The more pronounced anti-adhesive effects of PDI inhibition in hormone-sensitive MCF-7 cells featured by higher levels of PDIs when compared to triple-negative MDA-MB-231 cells suggests that targeting extracellular PDIA1 and PDIA3 with or without additional PDIA17 inhibition may represent a strategy for personalized anti-adhesive, anti-metastatic therapy in cancers with high PDI expression.
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