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活体供肝和劈离式肝移植术后小肝综合征。

Small for size syndrome following living donor and split liver transplantation.

机构信息

Hector Daniel Gonzalez, Zi Wei Liu, Sophia Cashman, Giuseppe K Fusai, Centre for HPB Surgery and Liver Transplantation, Royal Free Hospital, Pond Street, NW3 2QG, London, United Kingdom.

出版信息

World J Gastrointest Surg. 2010 Dec 27;2(12):389-94. doi: 10.4240/wjgs.v2.i12.389.

Abstract

The field of liver transplantation is limited by the availability of donor organs. The use of living donor and split cadaveric grafts is one potential method of expanding the donor pool. However, primary graft dysfunction can result from the use of partial livers despite the absence of other causes such as vascular obstruction or sepsis. This increasingly recognised phenomenon is termed "Small-for-size syndrome" (SFSS). Studies in animal models and humans have suggested portal hyperperfusion of the graft combined with poor venous outflow and reduced arterial flow might cause sinusoidal congestion and endothelial dysfunction. Graft related factors such as graft to recipient body weight ratio < 0.8, impaired venous outflow, steatosis > 30% and prolonged warm/cold ischemia time are positively predictive of SFSS. Donor related factors include deranged liver function tests and prolonged intensive care unit stay greater than five days. Child-Pugh grade C recipients are at relatively greater risk of developing SFSS. Surgical approaches to prevent SFSS fall into two categories: those targeting portal hyperperfusion by reducing inflow to the graft, including splenic artery modulation and portacaval shunts; and those aiming to relieve parenchymal congestion. This review aims to examine the controversial diagnosis of SFSS, including current strategies to predict and prevent its occurrence. We will also consider whether such interventions could jeopardize the graft by compromising regeneration.

摘要

肝移植领域受到供体器官可用性的限制。使用活体供体和分体尸体移植物是扩大供体库的一种潜在方法。然而,尽管不存在其他原因,如血管阻塞或败血症,但部分肝脏的使用仍可能导致原发性移植物功能障碍。这种日益被认识到的现象被称为“小肝综合征”(SFSS)。动物模型和人类研究表明,移植物的门静脉高灌注加上静脉流出不良和动脉流量减少可能导致窦状隙充血和内皮功能障碍。与 SFSS 相关的移植物相关因素包括:移植物与受体体重比 < 0.8、静脉流出受损、脂肪变性 > 30%和热/冷缺血时间延长,这些因素具有阳性预测价值。与供体相关的因素包括肝功能检查异常和 ICU 住院时间延长超过 5 天。Child-Pugh 分级为 C 的受者发生 SFSS 的风险相对较高。预防 SFSS 的手术方法可分为两类:一类是通过减少流入移植物的血流量来降低门静脉高灌注,包括脾动脉调节和门腔分流术;另一类是旨在缓解实质充血。本文旨在探讨 SFSS 的有争议的诊断,包括目前预测和预防其发生的策略。我们还将考虑这些干预措施是否会通过损害再生而危及移植物。

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本文引用的文献

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