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首页> 外文期刊>Journal of Medicinal Chemistry >Investigating the role of metal chelation in HIV-1 integrase strand transfer inhibitors
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Investigating the role of metal chelation in HIV-1 integrase strand transfer inhibitors

机译:研究金属螯合剂在HIV-1整合酶链转移抑制剂中的作用

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HIV-1 integrase (IN) has been validated as an attractive target for the treatment of HIV/AIDS. Several studies have confirmed that the metal binding function is a crucial feature in many of the reported IN inhibitors. To provide new insights on the metal chelating mechanism of IN inhibitors, we prepared a series of metal complexes of two ligands (HL~1 and HL~2), designed as representative models of the clinically used compounds raltegravir and elvitegravir. Potentiometric measurements were conducted for HL~2 in the presence of Mg(II), Mn(II), Co(II), and Zn(II) in order to delineate a metal speciation model. We also determined the X-ray structures of both of the ligands and of three representative metal complexes. Our results support the hypothesis that several selective strand transfer inhibitors preferentially chelate one cation in solution and that the metal complexes can interact with the active site of the enzyme. (Figure presented)
机译:HIV-1整合酶(IN)已被证实是治疗HIV / AIDS的诱人靶标。几项研究证实,金属结合功能是许多报道的IN抑制剂中的关键特征。为了提供有关IN抑制剂的金属螯合机理的新见解,我们制备了两个配体(HL〜1和HL〜2)的一系列金属配合物,被设计为临床使用的化合物raltegravir和elvitegravir的代表模型。在Mg(II),Mn(II),Co(II)和Zn(II)的存在下对HL〜2进行电位测量,以描绘金属形态模型。我们还确定了两个配体和三个代表性金属配合物的X射线结构。我们的结果支持以下假设:几种选择性链转移抑制剂优先螯合溶液中的一个阳离子,并且金属络合物可以与酶的活性位点相互作用。 (图示)

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