首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Impact of mycophenolic acid and tacrolimus on Th17-related immune response.
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Impact of mycophenolic acid and tacrolimus on Th17-related immune response.

机译:麦考酚酸和他克莫司对Th17相关免疫反应的影响。

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BACKGROUND: Little is known on the impact of immunosuppressive drugs on the development of the different T-cell subsets that compose the immune balance. We have explored the influence of mycophenolic acid (MPA) and tacrolimus on T cells response with a special focus on the Th17-cell subset. METHODS: In an in vitro model of human CD4 cells activation, we first compared the influence of MPA and tacrolimus on the transcription of different set of genes related to each of the main T-cell subsets and then investigated how these two drugs interfere with interleukin (IL)-17 production. We also studied, in stable kidney transplant patients, the relation between IL-17 serum concentration and systemic drug exposure. RESULTS: MPA and tacrolimus exhibited a comparable impact on T-cell response, dampening most Th1-related genes transcription and preserving regulatory T cells/Th2 molecular phenotypes. Although both MPA and tacrolimus decreased Th17-related transcripts after T-cell activation, MPA exerted a stronger inhibitory effect on IL-17 production than tacrolimus. Accordingly, renal transplant patients treated with MPA in combination with minimized dose of tacrolimus tended to have lower circulating IL-17 levels than patients treated with tacrolimus alone given at conventional dose. CONCLUSIONS: A treatment combining MPA and tacrolimus is susceptible to favorably tip the immune balance and might confer optimal allograft immunoprotection. Because of its ability to profoundly inhibit IL-17 production, MPA may help to better overcome Th17-related alloreactivity in the context of calcineurin inhibitor-minimizing protocol.
机译:背景:关于免疫抑制药物对构成免疫平衡的不同T细胞亚群发育的影响知之甚少。我们已经研究了麦考酚酸(MPA)和他克莫司对T细胞反应的影响,特别关注Th17细胞亚群。方法:在体外人类CD4细胞活化模型中,我们首先比较了MPA和他克莫司对与每个主要T细胞亚群相关的不同基因集转录的影响,然后研究了这两种药物如何干扰白介素(IL)-17生产。我们还在稳定的肾脏移植患者中研究了IL-17血清浓度与全身性药物暴露之间的关系。结果:MPA和他克莫司对T细胞反应具有类似的影响,抑制大多数Th1相关基因的转录,并保留调节性T细胞/ Th2分子表型。尽管MPA和他克莫司都在T细胞活化后降低了Th17相关的转录本,但MPA对IL-17产生的抑制作用比他克莫司强。因此,与常规剂量单独使用他克莫司治疗的患者相比,用MPA和最小剂量他克莫司治疗的肾移植患者的循环IL-17水平往往较低。结论:MPA和他克莫司联合治疗易引起免疫平衡失调,并可能提供最佳的同种异体移植免疫保护。由于它具有深刻抑制IL-17产生的能力,在钙调神经磷酸酶抑制剂最小化方案的背景下,MPA可能有助于更好地克服与Th17相关的同种异体反应。

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