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肾移植后OKT3肾毒性的预防。

Prevention of OKT3 nephrotoxicity after kidney transplantation.

作者信息

Abramowicz D, De Pauw L, Le Moine A, Sermon F, Surquin M, Doutrelepont J M, Ickx B, Depierreux M, Vanherweghem J L, Kinnaert P, Goldman M, Vereerstraeten P

机构信息

Department of Nephrology, Hopital Erasme, Université Libre de Bruxelles, Belgium.

出版信息

Kidney Int Suppl. 1996 Jan;53:S39-43.

PMID:8770989
Abstract

In our experience the use of OKT3 as prophylaxis in renal transplantation has been associated with an increased incidence of both delayed graft function and thromboses of graft vessels. OKT3 nephrotoxicity might have been favored by restriction of perioperative fluid infusion to prevent pulmonary edema and by the use of very high dose (30 mg/kg) of methylprednisolone (mPDS) before the first OKT3 injection to reduce the release of cytokines. This led us to modify our perioperative management in three ways: (1) hydration status was optimalized; (2) the calcium-channel blocker diltiazem, considered beneficial for recovery of graft function, was administered on the day of transplantation; and (3) the dose of mPDS given before the first OKT3 injection was fixed at 8 mg/kg. Comparison of two consecutive series of patients (group 1, control patients, N = 172; group 2, managed as described above, N = 173) showed that: (1) the incidence of delayed graft function fell from 52% in group 1 to 22% in group 2 (P < 0.0001): (2) the incidence of pulmonary edema was not significantly increased in group 2 (3.5% vs. 1.7% in group 1, P = 0.5); and (3) the frequency of intragraft thrombosis fell from 7.6% in group 1 to 1.2% in group 2 (P = 0.0034). Multivariate analysis showed that the volemia/diltiazem program and avoidance of high mPDS dose were the most important factors responsible for the reduced occurrence of delayed graft function and graft vessels thrombosis, respectively. We conclude that a combined strategy of appropriate dosage of steroids before the first OKT3 injection, administration of a calcium-channel blocker and optimalization of volemia is safe and efficiently prevents against OKT3 nephrotoxic effects.

摘要

根据我们的经验,在肾移植中使用OKT3进行预防与移植肾功能延迟恢复及移植血管血栓形成的发生率增加有关。围手术期限制液体输注以预防肺水肿,以及在首次注射OKT3前使用非常高剂量(30mg/kg)的甲基强的松龙(mPDS)以减少细胞因子释放,可能会加重OKT3肾毒性。这促使我们从三个方面对围手术期管理进行调整:(1)优化水化状态;(2)移植当天给予被认为对移植肾功能恢复有益的钙通道阻滞剂地尔硫卓;(3)将首次注射OKT3前给予的mPDS剂量固定为8mg/kg。对连续两组患者(第1组,对照组,N = 172;第2组,按上述方法管理,N = 173)进行比较,结果显示:(1)移植肾功能延迟恢复的发生率从第1组的52%降至第2组的22%(P < 0.0001);(2)第2组肺水肿的发生率没有显著增加(第1组为3.5%,第2组为1.7%,P = 0.5);(3)移植内血栓形成的频率从第1组的7.6%降至第2组的1.2%(P = 0.0034)。多因素分析表明,血容量/地尔硫卓方案和避免高剂量mPDS分别是移植肾功能延迟恢复和移植血管血栓形成发生率降低的最重要因素。我们得出结论,首次注射OKT3前给予适当剂量的类固醇、给予钙通道阻滞剂和优化血容量的联合策略是安全有效的,可预防OKT3的肾毒性作用。

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