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微管对肝脏内源性和外源性溶酶体成分胆汁排泄的调节作用。

Microtubule modulation of biliary excretion of endogenous and exogenous hepatic lysosomal constituents.

作者信息

Sewell R B, Barham S S, Zinsmeister A R, LaRusso N F

出版信息

Am J Physiol. 1984 Jan;246(1 Pt 1):G8-15. doi: 10.1152/ajpgi.1984.246.1.G8.

Abstract

We tested the hypothesis that hepatocyte microtubules modulate the biliary excretion of endogenous and exogenous constituents of hepatocyte lysosomes. We collected bile via bile fistulas from male rats before and after acute administration of colchicine and vinblastine, agents known to bind to hepatocyte microtubules; rats were then killed and livers were homogenized for biochemical analyses or processed for electron microscopy. Colchicine caused biphasic, parallel alterations in the biliary excretion of three lysosomal enzymes compared with control rats given saline or lumicolchicine; a peak rise in enzyme outputs of approximately 175% at 45-60 min after colchicine administration was followed by a sustained fall to approximately 25% of control values, which persisted for 2-4 h. When hepatocyte lysosomes were prelabeled in vivo by administration of [3H]Triton WR-1339, a nonionic detergent that is sequestered in hepatic lysosomes, the biliary excretion of radiolabel in response to colchicine paralleled the biliary excretion of the three lysosomal enzymes. Vinblastine also induced a biphasic response in biliary lysosomal enzyme output that was similar to that produced by colchicine administration. Morphometric analysis of electron micrographs of rat livers demonstrated changes in the number of lysosomelike vesicles in the vicinity of bile canaliculi after colchicine and vinblastine administration; the initial increase in lysosomal enzyme secretion was associated with a significant decrease in the number of pericanalicular lysosomes after both agents, while the subsequent decrease in enzyme secretion coincided with an increase in the number of pericanalicular lysosomes after vinblastine.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

我们验证了以下假说

肝细胞微管调节肝细胞溶酶体内源性和外源性成分的胆汁排泄。我们通过胆管瘘从雄性大鼠急性给予秋水仙碱和长春碱(已知与肝细胞微管结合的药物)前后收集胆汁;然后处死大鼠,将肝脏匀浆进行生化分析或用于电子显微镜检查。与给予生理盐水或光秋水仙碱的对照大鼠相比,秋水仙碱导致三种溶酶体酶的胆汁排泄出现双相、平行变化;秋水仙碱给药后45 - 60分钟,酶输出量峰值上升约175%,随后持续下降至对照值的约25%,并持续2 - 4小时。当通过给予[3H] Triton WR - 1339(一种被肝溶酶体摄取的非离子去污剂)在体内预先标记肝细胞溶酶体时,秋水仙碱引起的放射性标记物胆汁排泄与三种溶酶体酶的胆汁排泄平行。长春碱也诱导了胆汁溶酶体酶输出的双相反应,与秋水仙碱给药产生的反应相似。对大鼠肝脏电子显微镜照片的形态计量分析表明,秋水仙碱和长春碱给药后胆小管附近溶酶体样小泡数量发生变化;两种药物给药后,溶酶体酶分泌的初始增加与胆小管周围溶酶体数量的显著减少相关,而随后酶分泌的减少与长春碱给药后胆小管周围溶酶体数量的增加一致。(摘要截短于250字)

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