The influence of perfusion solution on renal graft viability assessment.

Colin H Wilson, Hugh Wyrley-Birch, Dhakshinarmoorthy Vijayanand, Anabelle Leea, Noel M Carter, Malcolm Haswell, Anne C Cunningham, David Talbot
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引用次数: 3

Abstract

Background: Kidneys from donors after cardiac or circulatory death are exposed to extended periods of both warm ischemia and intra-arterial cooling before organ recovery. Marshall's hypertonic citrate (HOC) and Bretschneider's histidine-tryptophan-ketoglutarate (HTK) preservation solutions are cheap, low viscosity preservation solutions used clinically for organ flushing. The aim of the present study was to evaluate the effects of these two solutions both on parameters used in clinical practice to assess organ viability prior to transplantation and histological evidence of ischemic injury after reperfusion.

Methods: Rodent kidneys were exposed to post-mortem warm ischemia, extended intra-arterial cooling (IAC) (up to 2 h) with preservation solution and reperfusion with either Krebs-Hensleit or whole blood in a transplant model. Control kidneys were either reperfused directly after retrieval or stored in 0.9% saline. Biochemical, immunological and histological parameters were assessed using glutathione-S-transferase (GST) enzymatic assays, polymerase chain reaction and mitochondrial electron microscopy respectively. Vascular function was assessed by supplementing the Krebs-Hensleit perfusion solution with phenylephrine to stimulate smooth muscle contraction followed by acetylcholine to trigger endothelial dependent relaxation.

Results: When compared with kidneys reperfused directly post mortem, 2 h of IAC significantly reduced smooth muscle contractile function, endothelial function and upregulated vascular cellular adhesion molecule type 1 (VCAM-1) independent of the preservation solution. However, GST release, vascular resistance, weight gain and histological mitochondrial injury were dependent on the preservation solution used.

Conclusions: We conclude that initial machine perfusion viability tests, including ischemic vascular resistance and GST, are dependent on the perfusion solution used during in situ cooling. HTK-perfused kidneys will be heavier, have higher GST readings and yet reduced mitochondrial ischemic injury when compared with HOC-perfused kidneys. Clinicians should be aware of this when deciding which kidneys to transplant or discard.

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灌注液对肾移植活力评估的影响。
背景:心脏或循环死亡后供者的肾脏在器官恢复前暴露于长时间的热缺血和动脉内冷却。Marshall’s高渗柠檬酸盐(HOC)和Bretschneider’s组氨酸-色氨酸-酮戊二酸盐(HTK)保存液是临床上用于器官冲洗的廉价、低粘度的保存液。本研究的目的是评估这两种溶液对临床实践中用于评估移植前器官活力的参数和再灌注后缺血性损伤的组织学证据的影响。方法:啮齿动物肾脏死后热缺血,保存液延长动脉内冷却(IAC)(长达2小时),移植模型用Krebs-Hensleit或全血再灌注。对照肾脏取肾后直接再灌注或保存在0.9%生理盐水中。分别采用谷胱甘肽- s -转移酶(GST)酶法、聚合酶链反应法和线粒体电镜法评估生化、免疫学和组织学参数。血管功能通过在Krebs-Hensleit灌注液中添加苯肾上腺素来刺激平滑肌收缩,然后添加乙酰胆碱来触发内皮依赖性松弛。结果:与死后直接再灌注肾脏相比,2 h IAC显著降低了与保存液无关的平滑肌收缩功能、内皮功能和血管细胞粘附分子1型(VCAM-1)的上调。然而,GST释放、血管阻力、体重增加和组织学线粒体损伤取决于所使用的保存液。结论:我们得出的结论是,初始机器灌注活力测试,包括缺血血管阻力和GST,取决于在原位冷却期间使用的灌注溶液。与hoc灌注的肾脏相比,htk灌注的肾脏会更重,GST读数更高,但线粒体缺血损伤减少。临床医生在决定移植或丢弃哪个肾脏时应该意识到这一点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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