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Hepatic clearance of tissue-type plasminogen activator and plasma kallikrein in experimental liver fibrosis.

机译:实验性肝纤维化中组织型纤溶酶原激活物和血浆激肽释放酶的肝清除率。

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摘要

We have previously shown that tissue-type plasminogen activator (tPA) and rat plasma kallikrein (RPK) share a common, but not unique, pathway for liver clearance. AIM: To evaluate the hepatic clearance of both proteases in experimental liver fibrosis. METHODS: The hepatic clearance of these proteases was studied in porcine serum-induced liver fibrosis using the isolated and perfused rat liver model. To better interpret the results, we also studied four other experimental groups: the turpentine oil-induced acute-phase response (AP group), AP group followed by GdCl3 administration (AP/Gd group), CCl4-induced cirrhosis (CCl4 group) and normal group. RESULTS: The tPA clearance decreased significantly by both fibrotic and cirrhotic rat livers whereas the RPK clearance was not altered by the fibrotic rat liver. The hepatic clearance of tPA was reduced in the AP and AP/Gd groups; on the other hand, RPK clearance was increased in the AP group and, interestingly, this effect was neutralized by concomitant GdCl3administration. CONCLUSIONS: We observed that tPA and RPK clearances were affected differently by fibrosis as well as by different stimuli of the acute-phase response, despite the fact that they share a common hepatic clearance mechanism in normal livers, and they were equally affected in cirrhosis.
机译:先前我们已经表明,组织型纤溶酶原激活物(tPA)和大鼠血浆激肽释放酶(RPK)共有一个共同但非唯一的肝脏清除途径。目的:评估两种蛋白酶在实验性肝纤维化中的肝清除率。方法:使用分离和灌注的大鼠肝脏模型研究了猪蛋白酶诱导的肝纤维化中这些蛋白酶的肝清除率。为了更好地解释结果,我们还研究了其他四个实验组:松节油诱导的急性期反应(AP组),AP组继之以GdCl3给药(AP / Gd组),CCl4引起的肝硬化(CCl4组)和正常组。结果:肝纤维化和肝硬化大鼠肝脏的tPA清除率均显着降低,而纤维化大鼠肝脏的RPK清除率未改变。 AP和AP / Gd组tPA的肝清除率降低。另一方面,AP组的RPK清除率增加,有趣的是,同时施用GdCl3可以中和该作用。结论:我们观察到纤维化以及急性期反应的不同刺激对tPA和RPK清除的影响不同,尽管它们在正常肝脏中具有相同的肝脏清除机制,并且在肝硬化中也同样受到影响。

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