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在免疫抑制剂诱导的肾损伤模型中,环孢素和雷帕霉素以协同和剂量依赖的方式发挥作用。

Cyclosporine and rapamycin act in a synergistic and dose-dependent manner in a model of immunosuppressant-induced kidney damage.

作者信息

Brook N R, Waller J R, Bicknell G R, Nicholson M L

机构信息

Transplantation Surgery Group, University of Leicester, Leicester, UK.

出版信息

Transplant Proc. 2005 Mar;37(2):837-8. doi: 10.1016/j.transproceed.2004.12.147.

DOI:10.1016/j.transproceed.2004.12.147
PMID:15848549
Abstract

The combination of cyclosporine (CSA) and rapamycin (RAPA) is a potent and commonly used approach to immunosuppression following solid-organ transplantation. By applying varying doses of CSA and RAPA to the rat salt-depleted model, we aimed to find a dose combination that favored antiproliferation/antifibrosis rather than toxicity. Male Sprague-Dawley rats (350 to 500 g) were salt-depleted for 7 days prior to commencing CSA and RAPA treatment. Serum creatinine and urinary protein/creatinine ratios were measured. Fibrosis was estimated with Sirius red staining of extracellular collagen. mRNA expression of TGF-beta, MMP-2, MMP-9, TIMP-1, and collagen III was assessed with reverse transcriptase PCR. A rise in serum creatinine at 7 and 28 days was observed for CSA 15 mg/kg/d (P = .002) but not CSA 7.5 mg (P = .06) or RAPA 1 mg (P = .69) compared to controls. Twenty-four-hour urinary protein excretion was unchanged compared to controls for all drug doses and combinations. Of the dose combinations, CSA 7.5 mg/d + RAPA 0.5 mg/d produced the lowest serum creatinine for all time points, and inhibited profibrotic TIMP-1 (P = .017), while increasing antifibrotic MMP-2 (P = .009) mRNA expression, compared to CSA treatment alone. Expression of TGF-beta and collagen III was unaltered between groups. CSA treatment produced molecular and biochemical changes indicating renal damage. Addition of RAPA can attenuate this damage, but only with a dose reduction of both agents. The most favorable results were for the dose combination CSA 7.5 mg/kg/d plus RAPA 0.5 mg/kg/d.

摘要

环孢素(CSA)与雷帕霉素(RAPA)联合使用是实体器官移植后一种强效且常用的免疫抑制方法。通过对大鼠盐耗竭模型应用不同剂量的CSA和RAPA,我们旨在找到一种有利于抗增殖/抗纤维化而非毒性的剂量组合。雄性Sprague-Dawley大鼠(350至500克)在开始CSA和RAPA治疗前7天进行盐耗竭处理。测量血清肌酐和尿蛋白/肌酐比值。用天狼星红对细胞外胶原进行染色来评估纤维化情况。用逆转录聚合酶链反应评估转化生长因子-β(TGF-β)、基质金属蛋白酶-2(MMP-2)、基质金属蛋白酶-9(MMP-9)、金属蛋白酶组织抑制因子-1(TIMP-1)和III型胶原的mRNA表达。与对照组相比,CSA 15毫克/千克/天在第7天和第28天血清肌酐升高(P = 0.002),但CSA 7.5毫克(P = 0.06)或RAPA 1毫克(P = 0.69)时未出现这种情况。与对照组相比,所有药物剂量和组合的24小时尿蛋白排泄均未改变。在所有剂量组合中,CSA 7.5毫克/天 + RAPA 0.5毫克/天在所有时间点产生的血清肌酐最低,与单独使用CSA治疗相比,其抑制促纤维化的TIMP-1(P = 0.017),同时增加抗纤维化的MMP-2(P = 0.009)mRNA表达。各组之间TGF-β和III型胶原的表达未改变。CSA治疗产生了表明肾损伤的分子和生化变化。添加RAPA可减轻这种损伤,但只有在两种药物剂量都降低的情况下才行。最有利的结果是CSA 7.5毫克/千克/天加RAPA 0.5毫克/千克/天的剂量组合。

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