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大鼠门腔静脉转位:一种有价值的肝脏研究模型的定义

Portacaval transposition in the rat: definition of a valuable model for hepatic research.

作者信息

Benjamin I S, Ryan C J, Engelbrecht G H, Campbell J A, van Hoorn-Hickman R, Blumgart L H

出版信息

Hepatology. 1984 Jul-Aug;4(4):704-8. doi: 10.1002/hep.1840040424.

Abstract

Portacaval transposition (PCT) in rats results in a smaller loss of body mass and liver mass than end-to-side portacaval shunt (PCS). Detailed studies of liver function, mass and histology were not previously available and have been undertaken in two different strains of growing rat in order to define the value of this model. PCT rats gained weight normally, while only 50% of PCS rats regained their preoperative weight by the tenth week. Wet and dry weights of liver fell relative to control values after both operations, but the fall was significantly greater after PCS than after PCT: there were parallel changes in hepatocyte size. There was a marked rise in liver-associated enzymes in the first 2 days after PCS only, and minimal enzyme elevations persisted in this group. The extent of cellular damage seen histologically closely parallelled the rise in SGOT in individual rats. At 72 hr, PCS rats showed focal necrotic changes, and by 10 weeks there was marked fatty infiltration: PCT rats had normal histology or showed minimal changes. PCT therefore provides a model in which there is total portal diversion without the more severe effects of the conventional PCS on hepatic structure and function. This has particular value in studies of experimental hepatic encephalopathy, of hormonal and amino acid changes after portal diversion, and of factors initiating or controlling liver regeneration.

摘要

大鼠门腔静脉转位术(PCT)导致的体重和肝脏重量损失比端侧门腔静脉分流术(PCS)小。此前尚无关于肝功能、肝脏重量和组织学的详细研究,为了确定该模型的价值,我们在两种不同品系的生长大鼠中进行了相关研究。PCT大鼠体重正常增加,而到第十周时,只有50%的PCS大鼠恢复到术前体重。两种手术后肝脏的湿重和干重相对于对照值均下降,但PCS术后的下降幅度明显大于PCT术后:肝细胞大小也有类似变化。仅在PCS术后的头2天,肝脏相关酶显著升高,且该组中酶的升高持续存在且幅度最小。组织学上观察到的细胞损伤程度与个体大鼠中谷草转氨酶(SGOT)的升高密切平行。在72小时时,PCS大鼠出现局灶性坏死变化,到10周时出现明显的脂肪浸润:PCT大鼠组织学正常或仅有轻微变化。因此,PCT提供了一种模型,其中存在完全的门静脉分流,而不会像传统的PCS那样对肝脏结构和功能产生更严重的影响。这在实验性肝性脑病、门静脉分流后激素和氨基酸变化以及启动或控制肝脏再生的因素的研究中具有特殊价值。

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