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缺血持续时间以及供体用甲基泼尼松龙或其大分子前药预处理对冷保存大鼠肝脏中吲哚菁绿处置的影响。

Effects of duration of ischemia and donor pretreatment with methylprednisolone or its macromolecular prodrug on the disposition of indocyanine green in cold-preserved rat livers.

作者信息

Chimalakonda Anjaneya P, Mehvar Reza

机构信息

School of Pharmacy, Texas Tech University Health Sciences Center, Amarillo, Texas 79106, USA.

出版信息

Pharm Res. 2004 Jun;21(6):1000-8. doi: 10.1023/b:pham.0000029290.54167.7c.

Abstract

PURPOSE

Cold preservation of the liver before transplantation may change uptake and excretory functions of hepatocytes. We hypothesized that an increase in the duration of preservation would result in a progressive decrease in the hepatic uptake and/or biliary excretion of indocyanine green (ICG), which would be attenuated by pharmacologic interventions.

METHODS

Donor rats (n = 40) were administered saline (control) or single 5 mg/kg doses of methylprednisolone (MP) or its liver-targeted prodrug (DMP) 2 h prior to liver harvest. Following preservation in cold University of Wisconsin solution for 0, 24, 48, or 72 h, livers were reperfused in a single-pass manner for 30 min in the presence of ICG (approximately 4 microg/ml), followed by 60 min of ICG-free perfusion. The inlet, outlet, and bile concentrations of ICG were measured periodically by high performance liquid chromatography (HPLC), and kinetic parameters were estimated.

RESULTS

Effects of duration of preservation: In unpreserved livers, a significant portion of ICG dose (16%) was effluxed from the liver during the washout period. Cold preservation for 24-72 h progressively increased (p < 0.05) the efflux of ICG (>2-fold at 72 h). Similarly, average extraction ratio showed a modest (30-40%) decrease with increasing preservation time (p < 0.05). However, biliary excretion of ICG showed the most sensitivity to the preservation time (14 to >800-fold decline). Effects of pretreatment: DMP caused significant (p < 0.05) increases in biliary ICG levels (>12-fold) and bile flow rates (6-15-fold) of preserved livers. Although MP pretreatment significantly (p < 0.05) increased (6-fold) bile flow rates in 48-h preserved livers, its effects on biliary ICG levels were not significant (p > 0.05).

CONCLUSIONS

Biliary excretion of ICG is the most sensitive kinetic parameter to prolonged cold ischemia-reperfusion injury in a rat liver perfusion model. The injury may be significantly attenuated by pharmacologic pretreatment of the liver donors.

摘要

目的

肝脏移植前进行冷保存可能会改变肝细胞的摄取和排泄功能。我们推测,保存时间的延长会导致吲哚菁绿(ICG)的肝脏摄取和/或胆汁排泄逐渐减少,而药物干预可使其减弱。

方法

在供体大鼠(n = 40)肝脏采集前2小时,给予生理盐水(对照组)或单次5 mg/kg剂量的甲泼尼龙(MP)或其肝脏靶向前药(DMP)。在冷威斯康星大学溶液中保存0、24、48或72小时后,肝脏在ICG(约4μg/ml)存在的情况下以单通道方式再灌注30分钟,随后进行60分钟无ICG灌注。通过高效液相色谱(HPLC)定期测量ICG的入口、出口和胆汁浓度,并估算动力学参数。

结果

保存时间的影响:在未保存的肝脏中,冲洗期有相当一部分ICG剂量(16%)从肝脏流出。冷保存24 - 72小时使ICG的流出量逐渐增加(p < 0.05)(72小时时增加超过2倍)。同样,随着保存时间的增加,平均提取率适度下降(30 - 40%)(p < 0.05)。然而,ICG的胆汁排泄对保存时间最为敏感(下降14至超过800倍)。预处理的影响:DMP使保存肝脏的胆汁ICG水平显著(p < 0.05)升高(超过12倍),胆汁流速显著(p < 0.05)升高(6 - 15倍)。虽然MP预处理使48小时保存肝脏的胆汁流速显著(p < 0.05)升高(6倍),但其对胆汁ICG水平的影响不显著(p > 0.05)。

结论

在大鼠肝脏灌注模型中,ICG的胆汁排泄是对延长的冷缺血-再灌注损伤最敏感的动力学参数。肝脏供体的药物预处理可显著减轻这种损伤。

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