Discovery of benzimidazole-2-amide BNZ-111 as new tubulin inhibitor

IF 2.5 4区 医学 Q3 CHEMISTRY, MEDICINAL Bioorganic & Medicinal Chemistry Letters Pub Date : 2024-09-11 DOI:10.1016/j.bmcl.2024.129953
Jiyoon Jang , Byumseok Koh , Kwangho Lee
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Abstract

Methyl benzimidazole-2-carbamate anthelmintics are a class of oral drugs to treat parasitic worm infections via microtubule disruption for non-systemic indications and currently in use. In order to use for anticancer treatment, the new benzimidazoles needs to improve solubility and pharmacokinetic parameters while maintaining its cellular potency as for systemic drug. Structure–activity-relationship on the benzimidazole is thoroughly examined and a novel benzimidazole-2 propionamide BNZ-111 is identified having good oral exposure and bioavailability in rat. Molecular docking study suggests BNZ-111 have a specific binding mode to the β subunit of curved tubulin. BNZ-111 is potent to cancer cells and possesses good drug-like properties as oral drug. Especially, BNZ-111 is not a P-gp substrate and it demonstrates its efficacy over Paclitaxel-resistance tumor in vivo.

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发现苯并咪唑-2-酰胺 BNZ-111 作为新的管蛋白抑制剂
苯并咪唑-2-氨基甲酸甲酯类抗虫药是一类通过破坏微管来治疗寄生虫感染的口服药物,目前用于非全身性适应症。为了用于抗癌治疗,新的苯并咪唑类药物需要改善溶解度和药代动力学参数,同时保持其作为全身用药的细胞效力。对苯并咪唑的结构-活性-关系进行了深入研究,发现了一种新型苯并咪唑-2 丙酰胺 BNZ-111,它在大鼠体内具有良好的口服暴露和生物利用度。分子对接研究表明,BNZ-111 与弯曲微管蛋白的 β 亚基具有特异性结合模式。作为口服药物,BNZ-111对癌细胞具有强效作用,并具有良好的类药物特性。特别是,BNZ-111不是P-gp底物,在体内对紫杉醇耐药的肿瘤有疗效。
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来源期刊
CiteScore
5.70
自引率
3.70%
发文量
463
审稿时长
27 days
期刊介绍: Bioorganic & Medicinal Chemistry Letters presents preliminary experimental or theoretical research results of outstanding significance and timeliness on all aspects of science at the interface of chemistry and biology and on major advances in drug design and development. The journal publishes articles in the form of communications reporting experimental or theoretical results of special interest, and strives to provide maximum dissemination to a large, international audience.
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