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头孢曲松与人血清白蛋白的结合:与胆红素的竞争。

Ceftriaxone binding to human serum albumin: competition with bilirubin.

作者信息

Brodersen R, Robertson A

机构信息

Institute of Medical Biochemistry, University of Aarhus, Denmark.

出版信息

Mol Pharmacol. 1989 Sep;36(3):478-83.

PMID:2779527
Abstract

Ceftriaxone, a cephalosporin, is bound reversibly to defatted human serum albumin from adults, with a first stoichiometric binding constant of 60,000 M-1, as found by equilibrium dialysis at pH 7.4, 37 degrees. A second molecule is weakly bound, with a binding constant of 500 M-1. Possible cobinding with bilirubin was studied by the peroxidase method and by equilibrium dialysis with and without added bilirubin. Results indicated competitive binding; formation of an albumin complex containing both bilirubin and ceftriaxone could not be demonstrated. Light absorption spectra of bilirubin-albumin showed little change on addition of ceftriaxone, in agreement with the competitive biding mechanism. Binding to serum albumin from newborn infants is weaker than to the protein from adults, with the first binding constant being about 36,000 M-1. Cobinding of ceftriaxone and bilirubin to albumin from newborn infants is likewise competitive. It is concluded that ceftriaxone is a strong bilirubin displacer with a potential of inducing bilirubin encephalopathy in predisposed newborns.

摘要

头孢曲松是一种头孢菌素,在pH 7.4、37℃条件下通过平衡透析发现,它与成人脱脂人血清白蛋白可逆结合,其一级化学计量结合常数为60,000 M⁻¹。第二个分子结合较弱,结合常数为500 M⁻¹。通过过氧化物酶法以及添加和不添加胆红素的平衡透析研究了与胆红素的可能共结合情况。结果表明存在竞争性结合;无法证明形成了同时含有胆红素和头孢曲松的白蛋白复合物。胆红素 - 白蛋白的光吸收光谱在添加头孢曲松后变化不大,这与竞争性结合机制一致。与新生儿血清白蛋白的结合比与成人蛋白质的结合弱,一级结合常数约为36,000 M⁻¹。头孢曲松和胆红素与新生儿白蛋白的共结合同样具有竞争性。得出的结论是,头孢曲松是一种强效胆红素置换剂,有在易患新生儿中诱发胆红素脑病的可能性。

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