通过肝动脉灌注80%乙醇建立肝硬化和门静脉高压模型。
Establishment of a hepatic cirrhosis and portal hypertension model by hepatic arterial perfusion with 80% alcohol.
作者信息
Wang Lei, He Fu-Liang, Liu Fu-Quan, Yue Zhen-Dong, Zhao Hong-Wei
机构信息
Lei Wang, Fu-Liang He, Fu-Quan Liu, Zhen-Dong Yue, Hong-Wei Zhao, Department of Interventional Therapy, Beijing Shijitan Hospital, Capital Medical University, Beijing 100038, China.
出版信息
World J Gastroenterol. 2015 Aug 28;21(32):9544-53. doi: 10.3748/wjg.v21.i32.9544.
AIM
To determine the feasibility and safety of establishing a porcine hepatic cirrhosis and portal hypertension model by hepatic arterial perfusion with 80% alcohol.
METHODS
Twenty-one healthy Guizhou miniature pigs were randomly divided into three experimental groups and three control groups. The pigs in the three experimental groups were subjected to hepatic arterial perfusion with 7, 12 and 17 mL of 80% alcohol, respectively, while those in the three control groups underwent hepatic arterial perfusion with 7, 12 and 17 mL of saline, respectively. Hepatic arteriography and direct portal phlebography were performed on all animals before and after perfusion, and the portal venous pressure and diameter were measured before perfusion, immediately after perfusion, and at 2, 4 and 6 wk after perfusion. The following procedures were performed at different time points: routine blood sampling, blood biochemistry, blood coagulation and blood ammonia tests before surgery, and at 2, 4 and 6 wk after surgery; hepatic biopsy before surgery, within 6 h after surgery, and at 1, 2, 3, 4 and 5 wk after surgery; abdominal enhanced computed tomography examination before surgery and at 6 wk after surgery; autopsy and multi-point sampling of various liver lobes for histological examination at 6 wk after surgery.
RESULTS
In experimental group 1, different degrees of hepatic fibrosis were observed, and one pig developed hepatic cirrhosis. In experimental group 2, there were cases of hepatic cirrhosis, different degrees of increased portal venous pressure, and intrahepatic portal venous bypass, but neither extrahepatic portal-systemic bypass circulation nor death occurred. In experimental group 3, two animals died and three animals developed hepatic cirrhosis, and different degrees of increased portal venous pressure and intrahepatic portal venous bypass were also observed, but there was no extrahepatic portal-systemic bypass circulation.
CONCLUSION
It is feasible to establish an animal model of hepatic cirrhosis and portal hypertension by hepatic arterial perfusion with 80% alcohol, however, the safety of this model depends on a suitable perfusion dose.
目的
探讨通过肝动脉灌注80%乙醇建立猪肝硬化和门静脉高压模型的可行性及安全性。
方法
将21只健康贵州小型猪随机分为3个实验组和3个对照组。3个实验组的猪分别接受7、12和17 mL 80%乙醇的肝动脉灌注,而3个对照组的猪分别接受7、12和17 mL生理盐水的肝动脉灌注。在灌注前后对所有动物进行肝动脉造影和直接门静脉造影,并在灌注前、灌注后即刻以及灌注后2、4和6周测量门静脉压力和直径。在不同时间点进行以下操作:术前、术后2、4和6周进行常规采血、血液生化、凝血和血氨检测;术前、术后6小时内以及术后1、2、3、4和5周进行肝活检;术前和术后6周进行腹部增强计算机断层扫描检查;术后6周进行尸检并对各肝叶进行多点取样进行组织学检查。
结果
实验组1观察到不同程度的肝纤维化,1只猪发生肝硬化。实验组2出现肝硬化病例,门静脉压力不同程度升高,肝内门静脉分流,但未发生肝外门静脉-体循环分流,也无死亡。实验组3有2只动物死亡,3只动物发生肝硬化,也观察到门静脉压力不同程度升高和肝内门静脉分流,但无肝外门静脉-体循环分流。
结论
通过肝动脉灌注80%乙醇建立肝硬化和门静脉高压动物模型是可行的,然而,该模型的安全性取决于合适的灌注剂量。
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