Synthesis of 1, 2-Disubstituted Benzimidazoles at Ambient Temperature Catalyzed by 1-Methylimidazolium Tetraflouroborate ([Hmim] BF_4) and Investigating Their Anti-ovarian Cancer Properties Through Molecular Docking Studies and Calculations

Qeios Pub Date : 2024-03-20 DOI:10.32388/r7liup
Abdulhamid Dehghani, Yousef Delshad, Moslem Ahmadpour, Milad Ghezelsofloo
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Abstract

An environmentally benign method for the synthesis of 1, 2-disubstituted benzimidazoles by the reaction of aromatic aldehydes and o-phenylenediamines (OPD) in the presence of 1-methylimidazolium tetraflouroborate ([Hmim] BF4) at ambient temperature under green conditions is described. A broad range of structurally diverse benzaldehydes were applied successfully, and corresponding products were obtained in good to excellent yields in very short times. All products were identified by the melting points, 1H and 13C NMR techniques. Furthermore, with the help of computational chemistry and drug design methods, the anti-ovarian cancer properties of these compounds were studied and investigated. All the synthesized compounds bind to an agonist at the active site of the 6LAD protein, which leads to the inactivation of this protein and produces beneficial effects during ovarian cancer treatment. In this study, it was found that these compounds have the potential to become an oral anti-cancer drug.
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在 1-甲基咪唑鎓四氟硼酸盐([Hmim] BF_4)催化下常温合成 1, 2-二取代苯并咪唑,并通过分子对接研究和计算探讨其抗卵巢癌特性
本研究介绍了一种在绿色条件下,通过芳香醛和邻苯二胺(OPD)在 1-甲基咪唑四氟硼酸盐([Hmim] BF4)存在下于常温反应合成 1,2-二取代苯并咪唑的环保方法。研究人员成功地应用了多种结构不同的苯甲醛,并在很短的时间内以良好到极佳的收率获得了相应的产物。所有产物都通过熔点、1H 和 13C NMR 技术进行了鉴定。此外,在计算化学和药物设计方法的帮助下,对这些化合物的抗卵巢癌特性进行了研究和调查。所有合成的化合物都与 6LAD 蛋白活性位点的激动剂结合,从而导致该蛋白失活,并在卵巢癌治疗过程中产生有益的效果。这项研究发现,这些化合物具有成为口服抗癌药物的潜力。
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