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Activation of self-reactive B cells and autoimmune diseases

机译:自我反应性B细胞活化和自身免疫性疾病

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The development of antigen-specific cells of the immune system, the T and B lymphocytes, creates a dilemma. On the one hand, survival of the organism depends upon the generation of a nearly limitless repertoire of potential antigen-binding specificities so that cells able to respond to pathogens are present prior to contact. However, by devising genetic strategies to maximize receptor diversity, the generation of T and B cells with autoreactive receptors is inevitable. B cells have an even greater opportunity than T cells to become autoreactive, since they may randomly alter the amino acid sequence and hence the specificity of their receptors during an immune response. Observing the system, one might wonder not why autoimmune diseases occasionally develop, but rather why they are not more frequent or even unavoidable. In this review, we examine the generation of B cells and their repertoire of antigen receptors, describe mechanisms that have evolved to prevent self-reactive B cells from causing autoimmune diseased, and discuss scenarios that may lead to a breakdown of self tolerance.
机译:免疫系统的抗原特异性细胞(T和B淋巴细胞)的发展造成了两难境地。一方面,生物的存活取决于潜在抗原结合特异性的几乎无限的库的产生,使得能够在接触之前存在能够对病原体做出反应的细胞。然而,通过设计使受体多样性最大化的遗传策略,具有自身反应性受体的T细胞和B细胞的生成是不可避免的。 B细胞比T细胞具有更大的机会发生自身反应,这是因为B细胞可能会随机改变氨基酸序列,从而在免疫反应期间改变其受体的特异性。观察该系统,可能不会想知道为什么自身免疫性疾病偶尔会发展,而是为什么它们不会变得更加频繁甚至是不可避免。在这篇综述中,我们研究了B细胞的生成及其抗原受体库,描述了已发展为防止自我反应性B细胞引起自身免疫性疾病的机制,并讨论了可能导致自我耐受性下降的情况。

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