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一种在循环系统中具有相对较长半衰期的胆红素氧化酶衍生物对血浆胆红素的降解作用。

Degradation of plasma bilirubin by a bilirubin oxidase derivative which has a relatively long half-life in the circulation.

作者信息

Sugi K, Inoue M, Morino Y

机构信息

Department of Biochemistry, Kumamoto University Medical School, Japan.

出版信息

Biochim Biophys Acta. 1989 Jun 27;991(3):405-9. doi: 10.1016/0304-4165(89)90065-2.

Abstract

To enhance degradation of unconjugated bilirubin in hyperbilirubinemic subjects, we synthesized a bilirubin oxidase (EC 1.3.3.5) (BO) derivative (PEGBO) by covalently linking (2,4-bis[O-methoxy(polyethyleneglycol)]-6-chloro-s-triazine) (PEG) to the enzyme. Intravenously injected BO in rats disappeared from the circulation with a half-life of 2.5 min; the half-life of PEGBO was 190 min. Intravenously injected BO minimally and transiently decreased plasma bilirubin levels in jaundiced Gunn rats and in bile-duct-ligated jaundiced rats. In contrast, PEGBO rapidly and substantially decreased plasma bilirubin levels and the effect persisted for longer than 3 h. Renal dysfunction often occurs in patients with liver diseases. To study the role of bilirubin toxicity for the kidney, functions of transtubular transport for organic anions was measured in bile-duct-ligated jaundiced animals before and after treatment with PEGBO. Bile duct ligation decreased urinary excretion of phenolsulfophthalein (PSP), an organic anion used for renal function test. Treatment of the jaundiced animals with PEGBO increased the rate of PSP disappearance from the circulation and normalized its urinary excretion. Thus, PEGBO might be useful for the study of bilirubin toxicity in jaundiced animals.

摘要

为增强高胆红素血症患者体内未结合胆红素的降解,我们通过将(2,4-双[O-甲氧基(聚乙二醇)]-6-氯-s-三嗪)(PEG)共价连接到胆红素氧化酶(EC 1.3.3.5)(BO)上,合成了一种BO衍生物(PEGBO)。静脉注射的BO在大鼠体内从循环中消失的半衰期为2.5分钟;而PEGBO的半衰期为190分钟。静脉注射BO对黄疸Gunn大鼠和胆管结扎所致黄疸大鼠的血浆胆红素水平仅有轻微且短暂的降低作用。相比之下,PEGBO能迅速且显著降低血浆胆红素水平,且该作用持续超过3小时。肝功能不全患者常出现肾功能障碍。为研究胆红素毒性对肾脏的作用,在胆管结扎所致黄疸动物接受PEGBO治疗前后,测定了其肾小管对有机阴离子的转运功能。胆管结扎减少了用于肾功能测试的有机阴离子酚红(PSP)的尿排泄量。用PEGBO治疗黄疸动物可提高PSP从循环中消失的速率,并使其尿排泄量恢复正常。因此,PEGBO可能有助于研究黄疸动物体内的胆红素毒性。

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