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用于在肝再生或肝移植前成功进行肝支持的体外肝灌注系统:一项临床前对照试验。

Extracorporeal liver perfusion system for successful hepatic support pending liver regeneration or liver transplantation: a pre-clinical controlled trial.

作者信息

Abouna G M, Ganguly P K, Hamdy H M, Jabur S S, Tweed W A, Costa G

机构信息

College of Medicine and Medical Sciences, Arabian Gulf University, Manama, Bahrain.

出版信息

Transplantation. 1999 Jun 27;67(12):1576-83. doi: 10.1097/00007890-199906270-00012.

Abstract

BACKGROUND

There is a well recognized need for a system capable of providing effective support for patients with hepatic failure pending liver regeneration or liver transplantation. Recent attempts of using bioartificial liver containing encapsulated porcine hepatocytes, the deployment of emergency whole liver, or hepatocyte transplantation are complex and not consistently successful. The technique of ex vivo hepatic perfusion developed and used clinically by Abouna in the 1970s, has now been redesigned in a perfusion circuitry that mimics the physiological conditions of a normal liver. Before clinical application of this system, a preclinical trial was carried out in dogs with induced hepatic failure.

METHODS

Acute hepatic failure was induced in dogs by an end-to-side porto caval shunt, followed 24 hr later, by a 2-hr occlusion of the hepatic artery. All animals (n=18) were medically supported and were divided into three groups. In the control group (n=6) only medical support was used. In the experimental group (n=12) the animals were connected to the ex vivo liver support apparatus during acute hepatic failure via an AV shunt using a dog liver (n=6) or calf liver (n=6) (after a temporary extracorporeal bovine kidney transplant to remove preformed xeno antibody). Hepatic perfusion was carried out at 37 degrees C through the hepatic artery and portal vein at physiological pressures, and blood flow rate for 6-8 hr.

RESULTS

All control animals died of progressive hepatic failure at 14-19 hr after clamping the hepatic artery. The animals treated with ex vivo liver showed remarkable clinical and biochemical improvement. Five animals survived for 36-60 hr. Another seven animals recovered completely and became long-term survivors with biochemical and histological evidence of regeneration of their own liver. Biopsy of the allogeneic ex vivo liver at the end of perfusion showed some interstitial edema. Similar biopsy of the xenogeneic calf liver showed only mild and delayed xenograft rejection, which was most likely due to removal of preformed xeno antibody by temporary transplantation of the calf kidney before liver perfusion.

CONCLUSIONS

The observations and results obtained in this trial strongly confirm that extracorporeal perfusion through a whole liver, using the system described, is very successful and cost effective for the treatment of acute, but reversible hepatic failure, as well as serving as a bridge to liver transplantation. The time has come for this form of liver support technology to be reintroduced and widely used.

摘要

背景

人们普遍认识到需要一种能够为肝功能衰竭患者在肝脏再生或肝移植前提供有效支持的系统。最近尝试使用含有封装猪肝细胞的生物人工肝、紧急全肝移植或肝细胞移植,这些方法复杂且并非始终成功。20世纪70年代由阿博纳研发并临床应用的体外肝脏灌注技术,现在已在模拟正常肝脏生理条件的灌注回路中重新设计。在该系统临床应用之前,在诱导肝功能衰竭的犬类中进行了一项临床前试验。

方法

通过端侧门腔分流术诱导犬急性肝功能衰竭,24小时后,再对肝动脉进行2小时阻断。所有动物(n = 18)均接受医学支持并分为三组。对照组(n = 6)仅采用医学支持。实验组(n = 12)的动物在急性肝功能衰竭期间,通过动静脉分流,使用犬肝(n = 6)或小牛肝(n = 6)(在临时进行体外牛肾移植以去除预先形成的异种抗体后)连接到体外肝脏支持装置。在37摄氏度下,通过肝动脉和门静脉以生理压力和血流速率进行肝脏灌注6 - 8小时。

结果

所有对照动物在肝动脉夹闭后14 - 19小时死于进行性肝功能衰竭。接受体外肝脏治疗的动物在临床和生化方面有显著改善。5只动物存活了36 - 60小时。另外7只动物完全康复并成为长期存活者,有自身肝脏再生的生化和组织学证据。灌注结束时对同种异体体外肝脏进行活检显示有一些间质水肿。对异种小牛肝脏进行类似活检仅显示轻度且延迟的异种移植排斥反应,这很可能是由于在肝脏灌注前通过临时移植小牛肾脏去除了预先形成的异种抗体。

结论

该试验中获得的观察结果和结果有力地证实,使用所述系统通过全肝进行体外灌注对于治疗急性但可逆的肝功能衰竭非常成功且具有成本效益,同时也可作为肝移植的桥梁。这种形式的肝脏支持技术重新引入并广泛应用的时机已经到来。

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