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5-arylalkynyl-2-benzoyl thiophene: a novel microtubule inhibitor exhibits antitumor activity without neurological toxicity. | LitMetric

AI Article Synopsis

  • - The study focuses on microtubules, which are dynamic structures made from α-tubulin and β-tubulin; agents that target these structures can disrupt their polymerization and halt cancer cells in the G2/M phase of the cell cycle.
  • - A new compound, PST-3, shows strong anti-cancer effects by altering microtubule structures, stopping breast cancer cells from dividing, and leading them to die, while demonstrating minimal neurological toxicity.
  • - In tests on breast cancer models, PST-3 exhibited significant anti-tumor activity without causing neurological side effects, indicating its potential as a safe microtubule inhibitor for cancer treatment.

Article Abstract

The composition of microtubules involving several steps, including the polymerization and depolymerization of α-tubulin and β-tubulin heterodimers. Microtubule-targeting agents can increase or inhibit microtubule polymerization, thereby disrupting the dynamic process and stalling cells in G2/M phase. Microtubule-targeting agents are generally cytotoxic, which neurological toxicity being one of the significant adverse events associated. We recently reported a novel 5-arylalkynyl-2-benzoyl thiophene (PST-3) that exhibited broad-spectrum cellular cytotoxicity and potency with high safety. PST-3 was a substrate of p-gp, which could not cross the blood-brain barrier and lead to less neurotoxicity. The antitumor activities demonstrated that PST-3 combined with the colchicine-binding site on microtubule, induces morphological changes, disrupts microtubule networks, inhibits polymerization of tubulin, arrests breast cancer cells in the G2/M phase of the cell cycle and induces apoptosis. Evaluation of the antitumor effect demonstrated that PST-3 elicited MDA-MB-468 tumor %T/C of 11.75%, whereas elicited MCF7 tumor %T/C of 44.38% in breast cancer xenograft models. Besides, experiments of a higher dose (60 mg/kg) of PST-3 treatment for 21 days did not produce any significant neurotoxicity. These results provide evidence that PST-3 might possess the potential to be developed into a new microtubule inhibitor without neurological toxicity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8822276PMC

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