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Characterization of minor site probes for human serum albumin by high-performance affinity chromatography

机译:高效亲和色谱法表征人血清白蛋白的微量位点探针

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This study used high-performance affinity chromatography (HPAC) and:immobilized human serum albumin (HSA) columns to examine the specificity and cross-reactivity of various,compounds that have been proposed as markers for the minor binding sites of HSA. These agents included acetyldigitoxin and digitoxin as probes for the digitoxin site,:phenol red as a probe for the bilirubin site, and cis- or trans-clomiphene as markers for the tamoxifen site. None of these probes showed any significant binding at HSA's indole-benzodiazepine site. However, phenol red did bind at the warfarin-azapropazone site of HSA, and cis/trans-clomiphene gave positive allosteric effects caused by the binding of warfarin to HSA. Digitoxin and acetyldigitoxin were found to bind to a common, unique region on MSA; cis- and trans-clomiphene also appeared to interact at a unique site, although trans-clomiphene displayed additional direct competition with phenol red. From these results it was possible to develop a model that described the general relationship between these binding regions on HSA. This information should be useful in future studies that employ HPAC for characterizing the binding of HSA to other drugs or clinical agents. [References: 30]
机译:这项研究使用了高效亲和色谱(HPAC)和固定化人血清白蛋白(HSA)色谱柱,以检查各种化合物的特异性和交叉反应性,这些化合物已被提议作为HSA小分子结合位点的标记。这些药物包括乙酰数字毒素和洋地黄毒素作为洋地黄毒素部位的探针,酚红作为胆红素部位的探针,顺式或反式克罗米芬作为他莫昔芬部位的标记。这些探针均未在HSA的吲哚-苯并二氮杂卓位点显示任何显着结合。然而,酚红确实在HSA的华法林-氮杂za酮位点结合,顺式/反式克罗米芬具有由华法林与HSA结合引起的正构构效应。发现Digitoxin和acetyldigitoxin结合到MSA上一个共同的独特区域。顺式和反式克罗米芬也似乎在一个独特的位点相互作用,尽管反式克罗米芬显示出与酚红的额外直接竞争。根据这些结果,有可能建立一个描述HSA上这些结合区域之间一般关系的模型。该信息在将来使用HPAC表征HSA与其他药物或临床药物结合的研究中应该有用。 [参考:30]

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