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SERPINB3 Delays Glomerulonephritis and Attenuates the Lupus-Like Disease in Lupus Murine Models by Inducing a More Tolerogenic Immune Phenotype

机译:SERPINB3通过诱导更具耐受性的免疫表型延缓肾小球肾炎并减轻狼疮鼠模型中的狼疮样疾病。

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摘要

>Objective: To explore the effects of SERPINB3 administration in murine lupus models with a focus on lupus-like nephritis.>Methods: 40 NZB/W F1 mice were subdivided into 4 groups and intraperitoneally injected with recombinant SERPINB3 (7.5 μg/0.1 mL or 15 μg/0.1 mL) or PBS (0.1 mL) before (group 1 and 2) or after (group 3 and 4) the development of proteinuria (≥100 mg/dl). Two additional mice groups were provided by including 20 MRL/lpr mice which were prophylactically injected with SERPINB3 (10 mice, group 5) or PBS (10 mice, group 6). Time of occurrence and levels of anti-dsDNA and anti-C1q antibodies, proteinuria and serum creatinine, overall- and proteinuria-free survival were assessed in mice followed up to natural death. Histological analysis was performed in kidneys of both lupus models. The Th17:Treg cell ratio was assessed by flow-cytometry in splenocytes of treated and untreated MRL/lpr mice. Statistical analysis was performed using non parametric tests and Kaplan-Meier curves, when indicated.>Results: Autoantibody levels and proteinuria were significantly decreased and time of occurrence significantly delayed in SERPINB3-treated mice vs. controls. In agreement with these findings, proteinuria-free and overall survival were significantly improved in SERPINB3-treated groups vs. controls. Histological analysis demonstrated a lower prevalence of severe tubular lesions in kidneys of group 5 vs. group 6. SERPINB3-treated mice showed an overall trend toward a reduced prevalence of severe lesions in both strains. Th17:Treg ratio was significantly decreased in splenocytes of MRL/lpr mice treated with SERPINB3, compared to untreated control mice.>Conclusions: SERPINB3 significantly improves disease course and delays the onset of severe glomerulonephritis in lupus-prone mice, possibly inducing a more tolerogenic immune phenotype.
机译:>目的:探讨SERPINB3在鼠狼疮模型中的作用,重点是狼疮样肾炎。>方法:将40只NZB / W F1小鼠分为4组,每组1只。腹膜内注射重组SERPINB3(7.5μg/ 0.1 mL或15μg/ 0.1 mL)或PBS(0.1 mL)在(第1组和第2组)或发生蛋白尿(≥100mg / dl)之前或之后(第3组和第4组) 。通过包括20只MRL / lpr小鼠提供了另外两个小鼠组,所述小鼠被预防性地注射了SERPINB3(10只小鼠,第5组)或PBS(10只小鼠,第6组)。评估小鼠的死亡时间和抗dsDNA和抗C1q抗体的水平,蛋白尿和血清肌酐,无总蛋白尿和无蛋白尿的存活率,直至自然死亡。在两个狼疮模型的肾脏中进行组织学分析。通过流式细胞术评估处理和未处理的MRL / lpr小鼠脾细胞中的Th17:Treg细胞比例。 >结果:与对照组相比,SERPINB3处理的小鼠自身抗体水平和蛋白尿明显降低,发生时间明显延迟。与这些发现相符,与对照组相比,SERPINB3治疗组的无蛋白尿和总生存期显着提高。组织学分析表明,与第6组相比,第5组的肾脏中严重肾小管病变的患病率较低。在两种品系中,用SERPINB3处理的小鼠均显示出严重病变的患病率降低的总体趋势。与未治疗的对照小鼠相比,SERPINB3治疗的MRL / lpr小鼠脾细胞中Th17:Treg比率显着降低。>结论: SERPINB3显着改善易患狼疮的小鼠的病程并延迟严重肾小球肾炎的发作,可能诱导更多的耐受性免疫表型。

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