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DMSO-Perturbing Assay for Identifying Promiscuous Enzyme Inhibitors

机译:用于鉴定混杂酶抑制剂的DMSO扰动测定

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摘要

In search for enzyme inhibitors, we often encounter "promiscuous" enzyme inhibitors exhibiting nonspecific binding property toward enzyme active site. Therefore, inhibitory candidates should be mechanistically characterized as early as possible in discovery processes. However, there remains a lack of highly reliable and readily available methodology to evaluate specificity of initial hits inhibitors. The present study developed and established a novel DMSO-perturbing assay to identify promiscuous enzyme inhibitors. The assay successfully identified nonspecific binding inhibitors with a broad scope, typically by the attenuation of inhibitory activity by the influence of DMSO-addition. This attenuation would be attributed to the nonspecific binding property of inhibitors toward both productive and nonproductive (nondenatured) states of enzymes in perturbation solution. This working hypothesis was supported by spectroscopic analyses of enzyme conformations and analyses of solvent effects on perturbation. Overall, these results provided a novel concept of the DMSO-perturbing assay.
机译:在寻找酶抑制剂中,我们经常遇到“混杂的”酶抑制剂,对酶活性位点表现出非特异性的结合性。因此,在发现过程中应尽早在机械手中表征抑制候选者。然而,仍然缺乏高度可靠和容易获得的方法,以评估初始击中抑制剂的特异性。本研究开发并建立了一种新型DMSO扰动测定以鉴定混杂酶抑制剂。该测定成功地确定了具有宽范围的非特异性结合抑制剂,通常通过DMSO-添加的抑制活性衰减。这种衰减将归因于抑制剂对扰动溶液中酶的生产和非培养(Nondenatuped)状态的非特异性结合性。该工作假设得到了酶综合征的光谱分析和对扰动溶剂效应的分析。总体而言,这些结果提供了DMSO扰动测定的新颖概念。

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