胆红素/大鼠血清白蛋白相互作用。

P C Frandsen, R Brodersen
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引用次数: 10

摘要

胆红素与大鼠血清蛋白和人血清白蛋白的结合存在本质差异。添加和未添加胆红素的大鼠血清的酸度滴定表明,在pH 6.8 ~ 8.8范围内胆红素酸的结合发生,每分子结合的胆红素释放的氢离子少于一个。在人血清中,释放出两个氢离子,表明与胆红素的结合。N-[4-[(4-氨基苯基)-磺酰基]苯基]-乙酰胺(MADDS)与大鼠血清白蛋白的结合平衡受胆红素共结合的轻微影响,而MADDS与胆红素与人血清白蛋白的结合是竞争性的。最后,加入大鼠血清白蛋白能适度降低胆红素与过氧化氢和过氧化物酶的氧化速率,而加入人血清白蛋白则能显著降低胆红素与大鼠血清白蛋白复合物的氧化速率,说明胆红素与人血清白蛋白复合物受到氧化作用,而与人血清白蛋白复合物受到保护。在以大鼠为模型进行旨在预防人类新生儿胆红素脑病的实验研究时,应考虑到这些差异。
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Bilirubin/rat serum albumin interaction.

Essential differences are demonstrated between bilirubin binding to rat serum proteins and to albumin in human serum. Acidimetric titration of rat serum with and without added bilirubin shows that binding of bilirubin acid in the range of pH from 6.8 to 8.8 takes place with release of less than one hydrogen ion per molecule of bound bilirubin. With human serum, two hydrogen ions are released, indicating binding of bilirubin dianion. The binding equilibrium of N-[4-[(4-aminophenyl)-sulfonyl]phenyl]-acetamide (MADDS) to rat serum albumin is influenced slightly by cobinding of bilirubin whereas MADDS and bilirubin bind competitively to human serum albumin. Finally, the rate of oxidation of bilirubin with hydrogen peroxide and peroxidase is decreased moderately by addition of rat serum albumin and strongly by the human protein, indicating that biliribin in its complex with rat serum albumin is subject to oxidation while the complex with human serum albumin is protected. These differences should be considered when rats are used as a model in experimental studies aiming at prevention of bilirubin encephalopathy in human neonates.

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