雷帕霉素改善实验性膜性肾病的蛋白尿并恢复肾素和足素的表达。

Clinical & Developmental Immunology Pub Date : 2013-01-01 Epub Date: 2013-08-31 DOI:10.1155/2013/941893
Stavros Stratakis, Kostas Stylianou, Ioannis Petrakis, Vasiliki Mavroeidi, Rafaela Poulidaki, Christina Petra, Demitrios Moisiadis, Spyros Stratigis, Eleftheria Vardaki, Lydia Nakopoulou, Eugene Daphnis
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引用次数: 12

摘要

目的:最近的研究显示雷帕霉素对被动和主动海曼肾炎(HN)的有益作用。然而,这种有益作用的机制尚未阐明。方法:采用单次静脉滴注抗fx1诱导12只雄性Sprague-Dawley大鼠被动海曼肾炎(PHN)。1周后,6只大鼠开始每日皮下注射0.5 mgr/kg (PHN-Rapa)雷帕霉素。其余6只大鼠作为蛋白尿对照组(PHN),其余6只无PHN大鼠给予雷帕霉素溶剂作为健康对照组(HC)。第7周末处死所有大鼠。结果:雷帕霉素可显著减少PHN自体期蛋白尿。雷帕霉素对组织学病变有明显改善。免疫荧光显示治疗大鼠体内的自体同种异体抗体沉积减弱。未经治疗的大鼠肾小球中nephrin和podocin的含量下降,而雷帕霉素则恢复了它们的表达。结论:雷帕霉素单药治疗可显著改善实验性膜性肾病的蛋白尿和组织学病变。这种有益的作用可能是通过抑制PHN自身期的同种免疫反应和恢复足细胞蛋白nephrin和podocin的正常表达来介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Rapamycin ameliorates proteinuria and restores nephrin and podocin expression in experimental membranous nephropathy.

Rapamycin ameliorates proteinuria and restores nephrin and podocin expression in experimental membranous nephropathy.

Rapamycin ameliorates proteinuria and restores nephrin and podocin expression in experimental membranous nephropathy.

Rapamycin ameliorates proteinuria and restores nephrin and podocin expression in experimental membranous nephropathy.

Objective: Recent studies have shown a beneficial effect of rapamycin in passive and active Heymann Nephritis (HN). However, the mechanisms underlying this beneficial effect have not been elucidated.

Methods: Passive Heymann Nephritis (PHN) was induced by a single intravenous infusion of anti-Fx1 in 12 Sprague-Dawley male rats. One week later, six of these rats were commenced on daily treatment with subcutaneous rapamycin 0.5 mgr/kg (PHN-Rapa). The remaining six rats were used as the proteinuric control group (PHN) while six more rats without PHN were given the rapamycin solvent and served as the healthy control group (HC). All rats were sacrificed at the end of the 7th week.

Results: Rapamycin significantly reduced proteinuria during the autologous phase of PHN. Histological lesions were markedly improved by rapamycin. Immunofluorescence revealed attenuated deposits of autologous alloantibodies in treated rats. Untreated rats showed decreased glomerular content of both nephrin and podocin whereas rapamycin restored their expression.

Conclusions: Rapamycin monotherapy significantly improves proteinuria and histological lesions in experimental membranous nephropathy. This beneficial effect may be mediated by inhibition of the alloimmune response during the autologous phase of PHN and by restoration of the normal expression of the podocyte proteins nephrin and podocin.

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