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他克莫司(FK506)和西罗莫司(雷帕霉素)单药及联合治疗对延长猴肾移植存活时间的影响。

Effect of tacrolimus (FK506) and sirolimus (rapamycin) mono- and combination therapy in prolongation of renal allograft survival in the monkey.

作者信息

Qi S, Xu D, Peng J, Vu M D, Wu J, Bekersky I, Fitzsimmons W E, Peets J, Sehgal S, Daloze P, Chen H

机构信息

Laboratories of Experimental Surgery and Transplantation Immunology, University of Montreal, Notre-Dame Hospital, Quebec, Canada.

出版信息

Transplantation. 2000 Apr 15;69(7):1275-83. doi: 10.1097/00007890-200004150-00012.

Abstract

BACKGROUND

Our previous studies confirmed that tacrolimus (FK506) and sirolimus [rapamycin (RAPA)], in combination, are not antagonistic but are synergistic in the prolongation of heart and small bowel grafts in the rodent. The aim of this study was to confirm further the synergistic effect of combined FK506 and RAPA in the more clinically relevant model, kidney transplantation in monkeys.

METHODS

A total of 60 male Vervet monkeys were randomly assigned to 10 groups (n> or =5). Monkeys with renal allografts were treated with different doses of FK506 and/or RAPA orally for 60 days. Graft survival, body weight, clinical biochemistry determinations, oral glucose tolerance test, trough levels of the two drugs, and histopathology were investigated.

RESULTS

Low doses of FK506 (1 or 4 mg/kg) combined with RAPA (0.5 mg/kg) produced synergistic effect in the prolongation of renal graft survival [combination index (CI) = 0.292, 0.565]. There were no additive or synergistic drug-associated toxicities such as hyperglycemia, nephrotoxicity, and hyperlipidemia. There also was no pharmacological antagonism.

CONCLUSION

Concomitant therapy of low-dose (drug-optimal) FK506 and RAPA produced a synergistic effect in the prolongation of kidney allograft survival in Vervet monkeys without additive drug-associated toxicities.

摘要

背景

我们之前的研究证实,他克莫司(FK506)和西罗莫司[雷帕霉素(RAPA)]联合使用时,在延长啮齿动物心脏和小肠移植物存活时间方面并非拮抗作用,而是具有协同作用。本研究的目的是在更具临床相关性的恒河猴肾移植模型中进一步证实FK506与RAPA联合使用的协同效应。

方法

总共60只雄性恒河猴被随机分为10组(每组n≥5)。接受肾移植的猴子口服不同剂量的FK506和/或RAPA,持续60天。观察移植物存活情况、体重、临床生化指标测定、口服葡萄糖耐量试验、两种药物的谷浓度以及组织病理学变化。

结果

低剂量的FK506(1或4mg/kg)与RAPA(0.5mg/kg)联合使用在延长肾移植物存活时间方面产生了协同效应[联合指数(CI)=0.292,0.565]。未出现如高血糖、肾毒性和高脂血症等药物相关的相加或协同毒性。也没有药理拮抗作用。

结论

低剂量(药物最佳剂量)FK506与RAPA联合治疗在延长恒河猴肾移植存活时间方面产生了协同效应,且未出现药物相关的相加毒性。

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