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Asundexian衍生物的设计、合成及活性评价OA

Design,synthesis and biological evaluation of Asundexian derivatives

中文摘要英文摘要

凝血因子 XIa(factor XIa,FXIa)在血栓形成过程中发挥关键作用,因此开发高效且安全的 FXIa抑制剂具有重要意义.基于此,本文以课题组前期研究发现的化合物 F22为先导化合物,采用生物电子等排和活性片段拼接等药物设计原理,设计并合成了 4个系列共 14个未见文献报道的 Asundexian衍生物.目标化合物结构经1H NMR和 HRMS确证,并采用生色底物法测定其 FXIa酶抑制活性.结果显示,化合物 FD-1表现出最好的抑制活性,IC50 为 2.8 nmol/L,优于先导化合物F22(IC50=4.5 nmol/L)和阳性药 Asundexian(IC50=5.0 nmol/L).此外,在活化部分凝血活酶时间(activated partial thromboplastin time,aPTT)测试中,化合物 FD-1显示出的抗凝血活性与 Asundexian相当,且对凝血酶原时间(prothrombin time,PT)无明显影响.本研究为后续小分子FXIa抑制剂的结构设计优化提供了新的指导思路.

Coagulation factor XIa(FXIa)plays a crucial role in thrombus formation;therefore,the development of potent and safe FXIa inhibitors is of great significance.In this study,compound F22,previously discovered by our group,was selected as the lead compound.Based on the principles of bioisosterism and fragment-based drug design,four series comprising 14 novel Asundexian derivatives not previously reported in the literature were designed and synthesized.The structures of the target compounds were confirmed by 1H NMR and HRMS,and their inhibitory activities against FXIa were evaluated using chromogenic substrate assay.Results showed that compound FD-1 exhibited the most potent activity,with an IC50 value of 2.8 nmol/L,which was superior to that of the lead compound F22(IC50=4.5 nmol/L)and the reference drug Asundexian(IC50=5.0 nmol/L).Furthermore,in the activated partial thromboplastin time(aPTT)assay,compound FD-1 demonstrated excellent anticoagulant activity,outperforming Asundexian,showing no significant effect on prothrombin time(PT).These findings provide valuable insights for further structural optimization and rational design of small-molecule FXIa inhibitors.

吴杰;朱华超;王鑫浩;宫平

齐鲁医药学院药学院,淄博 255213齐鲁医药学院药学院,淄博 255213齐鲁医药学院药学院,淄博 255213沈阳药科大学制药工程学院,沈阳 110016

医药卫生

FXIa抑制剂Asundexian生物电子等排活性研究

FXIa inhibitorsAsundexianbioisosterismbiological activity

《中国药科大学学报》 2026 (2)

196-205,10

10.11665/j.issn.1000-5048.2025100902

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