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在兔异位心脏移植模型中雷帕霉素和环孢素血药浓度与同种异体移植排斥反应抑制的关系。

The relationship of blood concentrations of rapamycin and cyclosporine to suppression of allograft rejection in a rabbit heterotopic heart transplant model.

作者信息

Fryer J, Yatscoff R W, Pascoe E A, Thliveris J

机构信息

Department of Surgery, University of Manitoba, Winnipeg, Canada.

出版信息

Transplantation. 1993 Feb;55(2):340-5. doi: 10.1097/00007890-199302000-00021.

Abstract

Heterotopic heart transplants were performed on 50 New Zealand white rabbits. Groups of 5 rabbits were randomly assigned to receive, through an intravenous route, rapamycin (RAPA) or cyclosporine at the following doses: RAPA (0.05, 0.1, 0.5, and 1.0 mg/kg/day); CsA (5.0, 10.0, and 15.0 mg/kg/day). Drug vehicle and saline controls were also included. Trough blood concentrations were monitored in both RAPA- and CsA-treated groups on a weekly basis throughout the study. Biochemical assessment of renal and liver function was performed at the beginning and end of the study. Animals receiving RAPA exhibited excellent allograft survival; only two animals in the lowest dosage group (0.05 mg/kg/day) rejected their grafts. In contrast, no rejection occurred in the CsA-treated groups. Animals that rejected their grafts were maintained on the drug until the endpoint of the study was reached at 60 days posttransplant to monitor drug induced side-effects. In some instances animals were sacrificed prior to this time due to infectious and other complications. No significant changes in renal or liver function were noted in the RAPA-treated group, while in the group of animals receiving the highest dose of CsA (15.0 mg/kg/day) a significant decrease in creatinine clearance was noted. A correlation was shown to exist between dose and the trough concentrations of both drugs. The whole-blood concentrations of RAPA that resulted in maximal efficacy with minimal toxicity was in the range of 10-60 micrograms/L. Rabbits having trough whole-blood concentrations of < 10 micrograms/L rejected their grafts. A much wider therapeutic range for CsA (50-300 micrograms/L) was noted. The results suggest that RAPA is as efficacious as CsA in prevention of allograft rejection in the animal model tested. The therapeutic monitoring of trough blood concentrations of RAPA, as with CsA, may be useful in guiding dosage adjustments to maximize the immunosuppressive efficacy while minimizing drug-induced side-effects.

摘要

对50只新西兰白兔进行了异位心脏移植。将5只兔子分为一组,随机分配通过静脉途径接受以下剂量的雷帕霉素(RAPA)或环孢素:RAPA(0.05、0.1、0.5和1.0毫克/千克/天);环孢素A(CsA)(5.0、10.0和15.0毫克/千克/天)。还包括药物载体和生理盐水对照组。在整个研究过程中,每周对接受RAPA和CsA治疗的组监测谷血药浓度。在研究开始和结束时对肾功能和肝功能进行生化评估。接受RAPA的动物表现出优异的同种异体移植物存活率;最低剂量组(0.05毫克/千克/天)中只有两只动物排斥其移植物。相比之下,CsA治疗组未发生排斥反应。排斥其移植物的动物持续使用药物直至移植后60天达到研究终点,以监测药物引起的副作用。在某些情况下,由于感染和其他并发症,动物在此之前被处死。在接受RAPA治疗的组中未观察到肾功能或肝功能有显著变化,而在接受最高剂量CsA(15.0毫克/千克/天)的动物组中,肌酐清除率显著降低。两种药物的剂量与谷浓度之间存在相关性。产生最大疗效且毒性最小的RAPA全血浓度范围为10 - 60微克/升。谷全血浓度<10微克/升的兔子排斥其移植物。观察到CsA的治疗范围要宽得多(50 - 300微克/升)。结果表明,在测试的动物模型中,RAPA在预防同种异体移植物排斥方面与CsA一样有效。与CsA一样,对RAPA谷血药浓度进行治疗监测可能有助于指导剂量调整,以最大限度地提高免疫抑制疗效,同时尽量减少药物引起的副作用。

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