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茴香霉素抗利什曼原虫活性的官能团相关性系统探究。

Systematic Exploration of Functional Group Relevance for Anti-Leishmanial Activity of Anisomycin.

作者信息

Nguyen Anh Minh Thao, Shalev-Benami Moran, Rosa-Teijeiro Chloé, Ibarra-Meneses Ana Victoria, Yonath Ada, Bashan Anat, Jaffe Charles L, Olivier Martin, Fernandez-Prada Christopher, Lubell William D

机构信息

Department of Chemistry, Université de Montréal, Montreal, QC H3T 1J4, Canada.

Department of Chemical and Structural Biology, Weizmann Institute of Science, Rehovot 7610001, Israel.

出版信息

Biomedicines. 2023 Sep 15;11(9):2541. doi: 10.3390/biomedicines11092541.

Abstract

Assessment of structure-activity relationships for anti-protozoan activity revealed a strategy for preparing potent anisomycin derivatives with reduced host toxicity. Thirteen anisomycin analogs were synthesized by modifying the alcohol, amine, and aromatic functional groups. Examination of anti-protozoal activity against various strains of and cytotoxicity against leucocytes with comparison against the parent natural product demonstrated typical losses of activity with modifications of the alcohol, amine, and aromatic meta-positions. On the other hand, the para-phenol moiety of anisomycin proved an effective location for introducing substituents without significant loss of anti-protozoan potency. An entry point for differentiating activity against versus host has been uncovered by this systematic study.

摘要

抗原生动物活性的构效关系评估揭示了一种制备宿主毒性降低的强效茴香霉素衍生物的策略。通过修饰醇、胺和芳香族官能团合成了13种茴香霉素类似物。与母体天然产物相比,检测其对各种疟原虫菌株的抗原生动物活性和对白细胞的细胞毒性,结果表明,对醇、胺和芳香族间位进行修饰会导致活性典型丧失。另一方面,茴香霉素的对苯酚部分被证明是引入取代基的有效位置,且抗原生动物效力不会显著丧失。通过这项系统研究发现了区分对疟原虫与宿主活性的切入点。

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