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A Possible Role for Idiotype/Anti-idiotype B–T Cell Interactions in Maintaining Immune Memory

机译:独特型/抗独特型B–T细胞相互作用在维持免疫记忆中的可能作用

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摘要

Variable regions of both B-cell receptors (BCRs) and T-cell receptors (TCRs) are completely formed in the postnatal period, and, consequently, no innate immune tolerance against these structures exists in adulthood. Indeed, antibodies (Abs) specific to TCRs have been found in both animals and humans. These facts clearly indicate the existence of B cells able to directly interact with T cells through binding of BCRs to TCRs without implicating major histocompatibility complex molecules. A novel paradigm is proposed in that the immune memory is based on idiotype/anti-idiotype interactions occurring between BCRs and TCRs following clearance of the antigen that elicited immune responses. It is envisaged that direct contact between memory T and B cells could provide co-stimulatory signals needed to sustain viability, growth, and differentiation of the interacting immune cells. In contrast, plasma cells originating from memory B-cells could produce anti-TCR Abs that inhibit direct BCR-to-TCR interactions, thereby downregulating the B- to T-cell contact-based immune memory via a negative feedback mechanism.
机译:B细胞受体(BCRs)和T细胞受体(TCRs)的可变区在出生后完全形成,因此,成年后不存在针对这些结构的先天免疫耐受。实际上,在动物和人类中都发现了对TCR具有特异性的抗体(Abs)。这些事实清楚地表明了存在能够通过BCR与TCR结合而直接与T细胞相互作用而又不牵涉主要组织相容性复合物分子的B细胞。提出了一种新的范例,其中免疫记忆是基于清除引起免疫反应的抗原后,BCR和TCR之间发生的独特型/抗独特型相互作用。设想记忆T细胞和B细胞之间的直接接触可以提供维持相互作用的免疫细胞的活力,生长和分化所需的共刺激信号。相反,源自记忆B细胞的浆细胞可产生抗TCR Abs,抑制直接的BCR与TCR相互作用,从而通过负反馈机制下调基于B细胞与T细胞接触的免疫记忆。

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