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罗库溴铵在肝移植三个阶段的药代动力学

Pharmacokinetics of rocuronium during the three stages of liver transplantation.

作者信息

Fisher D M, Ramsay M A, Hein H A, Marcel R J, Sharma M, Ramsay K J, Miller R D

机构信息

Department of Anesthesia, University of California, San Francisco 94143-0648, USA.

出版信息

Anesthesiology. 1997 Jun;86(6):1306-16. doi: 10.1097/00000542-199706000-00012.

Abstract

BACKGROUND

Little is known about the influence of liver transplantation on the pharmacokinetics of most anesthetic drugs. The authors determined the pharmacokinetics of rocuronium during liver transplantation and examined whether variability in pharmacokinetics could explain variability in recovery of neuromuscular function.

METHODS

Twenty patients undergoing liver transplantation were given rocuronium, 600 microg/kg, after induction of anesthesia and again after perfusion of the transplanted liver. Plasma was sampled to determine rocuronium concentrations. Pharmacokinetic models were fit to rocuronium concentrations versus time data using a mixed-effects population approach. Various models permitted changes in clearance (Cl) or central compartment volume to account for changes in hepatic function and circulatory status during the paleohepatic, anhepatic, and neohepatic periods. Time to initial recovery of four twitches of the orbicularis oculi was determined.

RESULTS

During the paleohepatic and anhepatic periods, the typical value of Cl was 2.47 ml x kg(-1) x min(-1) and was not influenced by the magnitude of preexisting liver disease (as evidenced by prothrombin time, bilirubin, serum albumin, alanine transaminase [ALT], and aspartate transaminase [AST]). During the neohepatic period, the typical value of Cl varied as a function of the duration of warm ischemia of the hepatic allograft and was 2.72 ml x kg(-1) x min(-1) for a patient with an average 60-min period of warm ischemia; time to neuromuscular recovery varied as a function of Cl.

CONCLUSIONS

Despite prolonged hypothermic ischemia, the newly transplanted liver eliminates rocuronium as well as the diseased native liver (and comparably with historical control values). However, some patients had decreased rocuronium Cl during the neohepatic period, apparently a result of prolonged graft warm ischemia. The authors' finding of preservation of hepatic drug elimination in the hepatic allograft is consistent with limited data for other drugs evaluated during anesthesia.

摘要

背景

肝移植对大多数麻醉药物药代动力学的影响鲜为人知。作者测定了肝移植期间罗库溴铵的药代动力学,并研究药代动力学的变异性是否可以解释神经肌肉功能恢复的变异性。

方法

20例接受肝移植的患者在麻醉诱导后给予罗库溴铵600μg/kg,在移植肝灌注后再次给药。采集血浆以测定罗库溴铵浓度。使用混合效应群体方法将药代动力学模型拟合到罗库溴铵浓度与时间的数据。各种模型允许清除率(Cl)或中央室容积发生变化,以解释无肝前期、无肝期和新肝期肝功能和循环状态的变化。测定眼轮匝肌四个肌颤搐初始恢复的时间。

结果

在无肝前期和无肝期,Cl的典型值为2.47ml·kg⁻¹·min⁻¹,且不受既往肝病严重程度(以凝血酶原时间、胆红素、血清白蛋白、丙氨酸转氨酶[ALT]和天冬氨酸转氨酶[AST]为证)的影响。在新肝期,Cl的典型值随肝移植热缺血持续时间而变化,对于平均热缺血时间为60分钟的患者,Cl为2.72ml·kg⁻¹·min⁻¹;神经肌肉恢复时间随Cl而变化。

结论

尽管存在长时间低温缺血,新移植的肝脏清除罗库溴铵的能力与患病的原肝相同(且与历史对照值相当)。然而,一些患者在新肝期罗库溴铵的Cl降低,这显然是移植肝热缺血时间延长的结果。作者关于肝移植中肝脏药物清除功能得以保留的发现与麻醉期间评估的其他药物的有限数据一致。

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