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首页> 外文期刊>Nature clinical practice. Rheumatology >CD4+CD25+FoxP3+ regulatory T cells in autoimmune diseases.
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CD4+CD25+FoxP3+ regulatory T cells in autoimmune diseases.

机译:自身免疫性疾病中的CD4 + CD25 + FoxP3 +调节性T细胞。

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摘要

Maintenance of immune tolerance in the periphery can be envisioned as a balance between autoreactive lymphocytes and regulatory mechanisms that counteract them. The naturally occurring CD4(+)CD25(+) regulatory T cells (T(REGs)) have a major role in modulating the activity of self-reactive cells. The identification of Forkhead box P3 transcription factor (FoxP3) as the critical determinant of T(REG) development and function has provided new opportunities and generated expanded interest in studying the balance between autoimmunity and regulatory mechanisms in human autoimmune diseases. The identification of both human and mouse diseases resulting from the lack of FoxP3 expression, and consequently the absence of T(REGs), has rapidly expanded knowledge of T(REG) development and function during the past 5 years. Although it is still unclear how these regulatory cells function, they can inhibit the activation of potentially pathogenic T cells in vitro. Using in vitro functional assays and phenotypic analysis, T(REGs) isolated from patients with a variety of autoimmune diseases have been shown to exhibit reduced regulatory function as compared with those isolated from healthy controls. This Review will focus on the current state of knowledge on human T(REGs) and their association with specific autoimmune diseases.
机译:可以设想维持外周免疫耐受性是自身反应性淋巴细胞和抵消它们的调节机制之间的平衡。天然存在的CD4(+)CD25(+)调节性T细胞(T(REGs))在调节自我反应性细胞的活性中起主要作用。叉头盒P3转录因子(FoxP3)作为T(REG)发育和功能的关键决定因素的鉴定,为研究人类自身免疫性疾病中自身免疫和调节机制之间的平衡提供了新的机会,并引起了越来越多的兴趣。由于缺乏FoxP3表达而导致的人类和小鼠疾病的鉴定,因此也缺乏T(REGs),在过去5年中迅速扩展了对T(REG)发育和功能的认识。尽管尚不清楚这些调节细胞如何发挥作用,但它们可在体外抑制潜在致病性T细胞的活化。使用体外功能测定和表型分析,与健康对照相比,从多种自身免疫性疾病患者中分离出的T(REG)已显示出调节功能降低。这篇综述将着重于人类T(REG)及其与特定自身免疫性疾病的关系的当前知识状态。

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