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首页> 外文期刊>The journal of clinical investigation >Nanogel-based delivery of mycophenolic acid ameliorates systemic lupus erythematosus in mice
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Nanogel-based delivery of mycophenolic acid ameliorates systemic lupus erythematosus in mice

机译:基于纳米凝胶的霉酚酸的递送改善了小鼠系统性红斑狼疮

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The ability to selectively inactivate immune cells with immunosuppressants is a much sought-after modality for the treatment of systemic lupus erythematosus and autoimmunity in general. Here, we designed and tested a novel nanogel drug delivery vehicle for the immunosuppressant mycophenolic acid (MPA). Treatment with MPA-loaded nanogels increased the median survival time (MST) of lupus-prone NZB/W F1 mice by 3 months with prophylactic use (MST was 50 weeks versus 38 weeks without treatment), and by 2 months when administered after the development of severe renal damage (MST after proteinuria onset was 12.5 weeks versus 4 weeks without treatment). Equivalent and greater doses of MPA administered in buffer were not efficacious. Nanogels had enhanced biodistribution to organs and association with immune cells. CD4-targeted nanogels yielded similar therapeutic results compared with nontargeted formulations, with protection from glomerulonephritis and decreases in IFN-γ–positive CD4 T cells. DCs that internalized nanogels helped mediate immunosuppression, as they had reduced production of inflammatory cytokines such as IFN-γ and IL-12. Our results demonstrate efficacy of nanogel-based lupus therapy and implicate a mechanism by which immunosuppression is enhanced, in part, by the targeting of antigen-presenting cells.
机译:一般而言,用免疫抑制剂选择性灭活免疫细胞的能力是广受欢迎的治疗系统性红斑狼疮和自身免疫的方法。在这里,我们设计并测试了一种用于免疫抑制剂霉酚酸(MPA)的新型纳米凝胶药物递送载体。使用MPA负载的纳米凝胶进行治疗,可将预防狼疮的NZB / W F1小鼠的中位生存时间(MST)延长3个月(MST为50周,而未经治疗为38周),而在发育后给药则增加了2个月严重肾脏损害(蛋白尿发作后的MST为12.5周,而未经治疗为4周)。在缓冲液中给予等量和较大剂量的MPA无效。纳米凝胶增强了对器官的生物分布以及与免疫细胞的结合。与非靶向制剂相比,靶向CD4的纳米凝胶具有相似的治疗效果,可预防肾小球肾炎并减少IFN-γ阳性CD4 T细胞。内在化纳米凝胶的DC有助于介导免疫抑制,因为它们减少了炎性细胞因子(如IFN-γ和IL-12)的产生。我们的结果证明了基于纳米凝胶的狼疮治疗的功效,并暗示了通过部分抑制抗原呈递细胞增强免疫抑制的机制。

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