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稳态环孢素浓度对肾移植结局的影响。

The impact of steady-state cyclosporine concentrations on renal allograft outcome.

作者信息

Dunn J, Grevel J, Napoli K, Lewis R M, Van Buren C T, Kahan B D

机构信息

Department of Surgery, University of Texas Medical School, Houston 77030.

出版信息

Transplantation. 1990 Jan;49(1):30-4. doi: 10.1097/00007890-199001000-00007.

Abstract

It has been reported that initial cyclosporine levels over 400 ng/ml posttransplantation result in an increased incidence of delayed graft function (DGF). Several studies have shown early graft function to be a major determinant for long-term graft survival. Continuous intravenous infusion (CIVI) has been employed to induce immunosuppression establishing therapeutic drug levels while minimizing toxicity in renal allograft recipients. This study examines the impact of the achieved serum CsA steady-state concentration (Css) levels upon transplant outcome in 228 patients given CsA by CIVI. In spite of administration of a specific drug dose, interindividual variation in elimination rates yields a broad range of Css levels. Six groups were stratified by CsA Css levels: group A 0-75 ng/ml, group B 76-100 ng/ml, group C 101-150 ng/ml, group D 151-200 ng/ml, group E 201-250 ng/ml, and group F greater than 250 ng/ml. Group A showed a significantly lower age and greater incidence of rejection at 0-10 days. Group F had significantly higher incidences of nephrotoxicity, hepatotoxicity, and delayed graft function. The findings suggest that the antirejection Css threshold for CsA may be at least 75 ng/ml, and the toxicity threshold above 250 ng/ml. Controversy exists about whether CsA influences the incidence of DGF, therefore risk factors for DGF were examined among the groups stratified by CsA Css levels. While cold ischemia time for all 228 patients as a group was highly correlated with DGF (P less than 0.001), neither cold ischemia time nor donor age was significantly different among the groups. There does appear to be a synergistic effect between CsA Css and CIT, since the incidence of DGF was significantly higher when the cold ischemia time was 21-24 hr and CsA Css greater than 200 ng/ml. Long-term graft function did not appear to be affected by early CsA Css levels. The Css of 100-250 ng/ml appears to achieve a satisfactory outcome with a 19.5% incidence of rejection within 10 days, 29.7% DGF, and 5.1% nephrotoxicity. Only 118/228 patients (52%) in this study achieved that range despite a fixed low CIVI of CsA. Thus potential renal allograft recipients may benefit from a pretransplant pharmacokinetic study to predict the proper CIVI dose.

摘要

据报道,移植后初始环孢素水平超过400 ng/ml会导致移植肾功能延迟恢复(DGF)的发生率增加。多项研究表明,早期移植肾功能是长期移植存活的主要决定因素。持续静脉输注(CIVI)已被用于诱导免疫抑制,以建立治疗药物水平,同时将肾移植受者的毒性降至最低。本研究考察了228例接受CIVI环孢素治疗患者的血清环孢素稳态浓度(Css)水平对移植结局的影响。尽管给予了特定的药物剂量,但个体消除率的差异导致Css水平范围很广。根据环孢素Css水平将患者分为六组:A组0 - 75 ng/ml,B组76 - 100 ng/ml,C组101 - 150 ng/ml,D组151 - 200 ng/ml,E组201 - 250 ng/ml,F组大于250 ng/ml。A组在0 - 10天的年龄显著较低且排斥发生率较高。F组的肾毒性、肝毒性和移植肾功能延迟恢复的发生率显著更高。研究结果表明,环孢素的抗排斥Css阈值可能至少为75 ng/ml,毒性阈值高于250 ng/ml。关于环孢素是否影响移植肾功能延迟恢复的发生率存在争议,因此在按环孢素Css水平分层的各组中考察了移植肾功能延迟恢复的危险因素。虽然作为一个整体的228例患者的冷缺血时间与移植肾功能延迟恢复高度相关(P < 0.001),但各组之间的冷缺血时间和供体年龄均无显著差异。环孢素Css和冷缺血时间(CIT)之间似乎存在协同效应,因为当冷缺血时间为21 - 24小时且环孢素Css大于200 ng/ml时,移植肾功能延迟恢复的发生率显著更高。早期环孢素Css水平似乎未影响长期移植肾功能。Css为100 - 250 ng/ml似乎能取得满意的结果,10天内排斥发生率为19.5%,移植肾功能延迟恢复发生率为29.7%,肾毒性发生率为5.1%。尽管环孢素的CIVI剂量固定较低,但本研究中只有118/228例患者(52%)达到该范围。因此,潜在的肾移植受者可能会从移植前药代动力学研究中受益,以预测合适的CIVI剂量。

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