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The HSA affinity of warfarin and flurbiprofen determined by fluorescence anisotropy measurements of camptothecin

机译:通过喜树碱的荧光各向异性测量确定华法林和氟比洛芬的HSA亲和力

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The determination of affinity of warfarin and flurbiprofen to human serum albumin (HSA) by fluorescence anisotropy measurements of carboxylate form of camptothecin (CPT-C) is the subject of this paper. A simple method based on measurements of fluorescence anisotropy of CPT-C allows to determine the affinity constant of CPT-C to HSA by computation of the fraction of bound CPT-C molecules with HSA It was observed, that adding of competing drug to plasma significant reduces the rate of increase of CPT-C fluorescence anisotropy with increase of albumin concentration and, the affinity constant of CPT-C to HSA decreases. The hypothesis of interactions between competing drug and CPT-C is presented. The results of these studies suggest that CPT-C displaces other drug from protein binding site and the degree of this displacement depends on concentration of drug and drug-HSA binding affinity. The presented in this paper biosystems research allows to estimate the affinity constant of warfarin and flurbiprofen. It was also confirmed that despite that most of drugs bind predominantly to Site I or Site II of HSA (only one of these sites is high-affinity site), at elevated concentrations, part of drug molecules can be bound to low-affinity site of HSA.
机译:通过荧光各向异性测定喜树碱(CPT-C)的羧酸盐形式来测定华法林和氟比洛芬对人血清白蛋白(HSA)的亲和力。一种简单的基于CPT-C荧光各向异性测量的方法,可以通过计算与HSA结合的CPT-C分子的分数来确定CPT-C对HSA的亲和常数。观察到,将竞争药物添加到血浆中随着白蛋白浓度的增加,CPT-C荧光各向异性的增加速率降低,并且CPT-C对HSA的亲和常数降低。提出了竞争药物和CPT-C之间相互作用的假说。这些研究的结果表明,CPT-C从蛋白质结合位点置换了其他药物,这种置换的程度取决于药物浓度和药物-HSA结合亲和力。本文在生物系统研究中提出的方法可以估算出华法林和氟比洛芬的亲和常数。还证实,尽管大多数药物主要与HSA的I位或II位结合(这些位点中只有一个是高亲和力位点),但在升高的浓度下,部分药物分子仍可以与HSA的低亲和力位点结合HSA。

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