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鬼笔环肽对离体灌注大鼠肝脏胆汁淤积、血流动力学和微循环的影响。

Effect of phalloidin on cholestasis, hemodynamics, and microcirculation in isolated perfused rat liver.

作者信息

Barriault C, Petit J L, Gascon-Barré M, Huet P M, Yousef I M, Tuchweber B

机构信息

Department of Pharmacology, Université de Montréal, Canada.

出版信息

Hepatology. 1996 Feb;23(2):294-302. doi: 10.1002/hep.510230215.

Abstract

In this study, the possible role of the hepatic microcirculation in phalloidin-induced cholestasis and hepatotoxicity was examined in isolated perfused rat livers (IPRL). Administration of a phalloidin bolus (1 mg/kg body weight) through the portal vein induced an immediate reduction of bile flow. In 16.9 minutes, bile flow was 50% lower than basal values. Portal pressure was only increased in 60 minutes after phalloidin injection and increased sharply from this time up to the end of perfusion (90 minutes). Under these conditions, phalloidin did not induce liver cell cytolysis, as assessed by aspartate transaminase (AST) and lactate dehydrogenase (LDH) release in the perfusate effluent. Under electron microscopy, hepatocytic vacuolization was mild 15 minutes after phalloidin administration but increased with time. At the end of perfusion, the hepatic architecture was markedly altered; erythrocyte accumulation was observed in both sinusoids and hepatocyte vacuoles. Evaluation by multiple indicator dilution curves showed that extravascular volume (EVV) was significantly affected by phalloidin. It was augmented in 30 minutes after phalloidin administration with values increasing gradually over time. Neither vascular nor cellular volume was altered. The hepatic swelling may be attributed to enlargement of the extravascular space of the liver. These results indicate that changes in the liver microcirculation are not the primary cause of phalloidin-induced cholestasis in the IPRL.

摘要

在本研究中,我们在离体灌注大鼠肝脏(IPRL)中研究了肝微循环在鬼笔环肽诱导的胆汁淤积和肝毒性中可能发挥的作用。通过门静脉给予一次大剂量鬼笔环肽(1mg/kg体重)可立即导致胆汁流量减少。在16.9分钟时,胆汁流量比基础值低50%。门静脉压力仅在注射鬼笔环肽后60分钟升高,并从此时开始直至灌注结束(90分钟)急剧升高。在这些条件下,通过灌注液流出物中天冬氨酸转氨酶(AST)和乳酸脱氢酶(LDH)的释放评估,鬼笔环肽未诱导肝细胞溶解。在电子显微镜下,给药15分钟后肝细胞空泡化较轻,但随时间增加。在灌注结束时,肝脏结构明显改变;在肝血窦和肝细胞空泡中均观察到红细胞聚集。通过多指标稀释曲线评估表明,血管外容积(EVV)受到鬼笔环肽的显著影响。给药30分钟后增加,且随着时间推移值逐渐升高。血管容积和细胞容积均未改变。肝脏肿胀可能归因于肝脏血管外间隙的扩大。这些结果表明,肝脏微循环的变化不是IPRL中鬼笔环肽诱导胆汁淤积的主要原因。

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