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梗阻性黄疸对大鼠亲肾性有机阴离子转归的影响。

Effect of obstructive jaundice on the fate of a nephrophilic organic anion in the rat.

作者信息

Sugi K, Inoue M, Morino Y, Sato T

机构信息

Department of Biochemistry, Kumamoto University Medical School, Japan.

出版信息

Biochim Biophys Acta. 1989 Dec 28;987(2):217-21. doi: 10.1016/0005-2736(89)90548-8.

Abstract

Renal transtubular transport of phenolsulfophthalein (PSP), a nephrophilic organic anion that circulates bound to albumin, was studied in normal and bile-duct-ligated rats. Intravenously injected PSP disappeared from the circulation more rapidly in bile-duct-ligated jaundiced rats than in intact animals. However, urinary excretion of PSP was significantly lower in the former than in the latter. Kinetic analysis revealed that binding of PSP to plasma protein(s) was significantly lower with jaundiced rats than with intact animals. Addition of albumin to plasma samples from bile-duct-ligated rats markedly increased PSP binding. The decreased PSP binding returned to normal levels after treating the jaundiced plasma with bilirubin oxidase, an enzyme that degrades amphiphilic bilirubin to water soluble metabolites. These results suggest that bilirubin might be the major metabolite that occupied the PSP binding site(s) on albumin in jaundiced rats. When PSP was injected bound to equimolar amount of albumin, the rate of PSP disappearance from the circulation decreased and urinary excretion of the ligand increased markedly; urinary excretion of PSP was significantly larger in bile-duct-ligated rats than in intact animals. These results suggest that the renal transport capacity for amphiphilic organic anions, such as PSP, might be increased compensatively in bile-duct-ligated animals, and that the apparent decrease in renal secretory transport for PSP might result from, at least in part, random distribution of the ligand to extrarenal tissues due to decrease in the binding activity of albumin.

摘要

酚红(PSP)是一种亲肾性有机阴离子,在循环中与白蛋白结合,我们对正常大鼠和胆管结扎大鼠的PSP肾跨管转运进行了研究。静脉注射的PSP在胆管结扎的黄疸大鼠体内从循环中消失的速度比正常动物更快。然而,前者的PSP尿排泄量明显低于后者。动力学分析显示,黄疸大鼠中PSP与血浆蛋白的结合明显低于正常动物。向胆管结扎大鼠的血浆样本中添加白蛋白可显著增加PSP的结合。用胆红素氧化酶(一种将两亲性胆红素降解为水溶性代谢产物的酶)处理黄疸血浆后,降低的PSP结合恢复到正常水平。这些结果表明,胆红素可能是占据黄疸大鼠白蛋白上PSP结合位点的主要代谢产物。当PSP与等摩尔量的白蛋白结合注射时,PSP从循环中消失的速度降低,配体的尿排泄量显著增加;胆管结扎大鼠的PSP尿排泄量明显大于正常动物。这些结果表明,胆管结扎动物对两亲性有机阴离子(如PSP)的肾转运能力可能会代偿性增加,而PSP肾分泌转运的明显降低可能至少部分是由于白蛋白结合活性降低导致配体随机分布到肾外组织所致。

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