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首页> 外文期刊>International archives of allergy and immunology >Cellular and humoral mechanisms of immune tolerance in immediate-type allergy induced by specific immunotherapy.
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Cellular and humoral mechanisms of immune tolerance in immediate-type allergy induced by specific immunotherapy.

机译:特异性免疫疗法诱导的即时型变态反应的免疫耐受的细胞和体液机制。

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摘要

The management of immediate-type allergy (ITA) is based on allergen avoidance, symptomatic pharmacological therapy and specific immunotherapy (SIT). Among these, SIT presents the only curative treatment. The efficacy of SIT in the treatment of IgE-mediated ITA has been proven in numerous clinical studies and is well established. This review discusses the relevance of immunoregulative humoral and cellular mechanisms leading to immune tolerance in ITA. Special focus is placed on the role of antibodies potentially interfering with the IgE-mediated immune reaction and regulatory T (T reg) cells including their immunosuppressive cytokines, which play a critical role in shifting the T helper 2 cell-driven allergic immune response towards allergen tolerance. Distinct subsets of constitutive and inducible T reg cells have been identified inhibiting the activation of allergen-specific effector T cells via cell contact- or cytokine-dependent suppression. Current research suggests that both inducible interleukin-10-producing CD4+ T reg cells and naturally occurring CD4+CD25+ T reg cells actively control allergic responses and that the disturbance of their function or number may contribute to the development or progression of allergy. Thus, the fine balance between allergen-specific T helper 2 and T reg cells constitutes a critical factor for the successful treatment of ITA by SIT.
机译:立即型过敏(ITA)的治疗基于避免过敏原,对症药理疗法和特异性免疫疗法(SIT)。其中,SIT是唯一的治疗方法。 SIT治疗IgE介导的ITA的功效已在众多临床研究中得到证实,并且已得到充分确立。这篇综述讨论了免疫调节性体液和细胞机制在ITA中引起免疫耐受的相关性。特别关注抗体可能会干扰IgE介导的免疫反应和调节性T(T reg)细胞(包括其免疫抑制细胞因子)的作用,这些抗体在将T辅助2细胞驱动的变态免疫反应转变为变应原中起关键作用公差。已经鉴定出组成型和诱导型T reg细胞的不同亚组通过细胞接触或细胞因子依赖性抑制来抑制变应原特异性效应T细胞的活化。当前的研究表明,可诱导的产生白介素10的CD4 + T reg细胞和天然存在的CD4 + CD25 + T reg细胞均能主动控制过敏反应,其功能或数量的紊乱可能有助于过敏的发生或发展。因此,变应原特异性T辅助细胞2和T reg细胞之间的良好平衡构成了SIT成功治疗ITA的关键因素。

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