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Diversity-oriented synthesis as a tool for identifying new modulators of mitosis

机译:面向多样性的合成作为鉴定有丝分裂新调节剂的工具

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The synthesis of diverse three-dimensional libraries has become of paramount importance for obtaining better leads for drug discovery. Such libraries are predicted to fare better than traditional compound collections in phenotypic screens and against difficult targets. Herein we report the diversity-oriented synthesis of a compound library using rhodium carbenoid chemistry to access structurally diverse three-dimensional molecules and show that they access biologically relevant areas of chemical space using cheminformatic analysis. High-content screening of this library for antimitotic activity followed by chemical modification identified ‘Dosabulin’, which causes mitotic arrest and cancer cell death by apoptosis. Its mechanism of action is determined to be microtubule depolymerization, and the compound is shown to not significantly affect vinblastine binding to tubulin; however, experiments suggest binding to a site vicinal or allosteric to Colchicine . This work validates the combination of diversity-oriented synthesis and phenotypic screening as a strategy for the discovery of biologically relevant chemical entities.
机译:为了获得更好的药物发现线索,各种三维文库的合成已变得至关重要。预计此类库在表型筛选中的表现要优于传统的化合物馆藏,并且针对困难的目标。在这里,我们报告了使用铑类胡萝卜素化学来访问结构多样的三维分子的化合物库的面向多样性的合成方法,并显示它们使用化学信息学分析访问了化学空间的生物学相关区域。对该库的抗有丝分裂活性进行高内涵筛选,然后进行化学修饰,鉴定出“ Dosabulin”,这会导致有丝分裂停滞并通过凋亡导致癌细胞死亡。确定其作用机理是微管解聚,并且该化合物显示出不会显着影响长春碱与微管蛋白的结合。然而,实验表明与秋水仙碱的邻位或变构位点结合。这项工作验证了多样性为导向的合成和表型筛选的组合作为发现生物学相关化学实体的策略。

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