1,4-苯并恶嗪-3(4H)-酮作为血小板聚集的有效抑制剂:设计、合成及构效关系
1,4-Benzoxazine-3(4H)-ones as potent inhibitors of platelet aggregation: design, synthesis and structure-activity relations.
作者信息
Liu Chang, Tan Jia-Lian, Xiao Si-Yu, Liao Jie-Feng, Zou Guang-Rong, Ai Xi-Xi, Chen Jian-Bin, Xiang Yi, Yang Quan, Zuo Hua
机构信息
College of Pharmaceutical Sciences, Southwest University.
出版信息
Chem Pharm Bull (Tokyo). 2014;62(9):915-20. doi: 10.1248/cpb.c14-00330. Epub 2014 Jul 9.
A series of novel potentially platelet aggregation-inhibiting 1,4-benzoxazine-3(4H)-one derivatives was designed and synthesized through Smiles rearrangement, reduction and acetylation reactions. The antiaggregatory activities of the target molecules on arterial blood samples from rabbits, expressed by IC₅₀ values (μM), were then evaluated in vitro against ADP induced platelet aggregation. The favorable IC₅₀ values of compound 8c (IC₅₀=8.99 µM) and 8d (IC₅₀=8.94 µM) indicated that these two compounds were the most potent molecules among all the synthesized compounds. A detailed molecular docking study to explore the interaction of compounds 8c and 8d with GP IIb/IIIa receptor showed that they these two compounds were docked into the active site of GPIIb/IIIa receptor. These results suggest that the 1,4-benzoxazine-3(4H)-one derivatives are promising lead compounds to develop new platelet aggregation inhibitors.
通过斯迈尔斯重排、还原和乙酰化反应设计并合成了一系列新型的、具有潜在血小板聚集抑制活性的1,4-苯并恶嗪-3(4H)-酮衍生物。然后,以IC₅₀值(μM)表示,在体外评估目标分子对兔动脉血样本中ADP诱导的血小板聚集的抗聚集活性。化合物8c(IC₅₀ = 8.99 μM)和8d(IC₅₀ = 8.94 μM)的良好IC₅₀值表明,这两种化合物是所有合成化合物中活性最强的分子。一项详细的分子对接研究,以探索化合物8c和8d与GP IIb/IIIa受体的相互作用,结果表明这两种化合物被对接至GPIIb/IIIa受体的活性位点。这些结果表明,1,4-苯并恶嗪-3(4H)-酮衍生物是开发新型血小板聚集抑制剂的有前景的先导化合物。
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