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Specificity and Plasticity of Memory Lymphocyte Migration

机译:记忆淋巴细胞迁移的特异性和可塑性

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To exert immunological activity, T and B cells must leave the blood and enter different extravascular compartments in the body. An essential step in this process is their adhesion to mkrovascular endothelhim and subsequent diapedesis into a target tissue. Naive and effector/memory T and B cells possess distinct repertoires of traffic molecules that restrict their ability to interact with specialized microvessels in different anatomic compartments and thus exhibit distinct patterns of migration. In addition, antigen-experienced lymphocytes are subdivided into different subsets based on their expression of characteristic sets of adhesion receptors that favor their accumulation in certain target organs, such as the skin and the gut. This article focuses on recent discoveries that have broadened our understanding of the "imprinting" mechanisms responsible for the generation of tissue-specific effector/memory lymphocytes, especially in the intestine. We discuss how gut-specific homing is acquired, maintained, and modulated and how these mechanisms might be harnessed to develop improved vaccine protocols and treatments for intestinal autoimmune diseases.
机译:为了发挥免疫活性,T细胞和B细胞必须离开血液并进入体内不同的血管外腔室。在此过程中,必不可少的步骤是它们粘附于血管内皮素和随后的透皮渗入目标组织。幼稚和效应/记忆T细胞和B细胞拥有不同的交通分子库,这些分子限制了它们与不同解剖区室中的专用微血管相互作用的能力,因此表现出不同的迁移模式。另外,基于抗原的淋巴细胞的表达根据粘附受体的特征性集合的表达而分为不同的亚群,粘附性受体的特征性集合有利于它们在某些靶器官如皮肤和肠中的积累。本文重点关注最近的发现,这些发现扩大了我们对负责组织特异性效应子/记忆淋巴细胞(尤其是肠道)生成的“印迹”机制的理解。我们讨论了如何获取,维持和调节肠道特异性归巢,以及如何利用这些机制来开发改进的疫苗方案和肠道自身免疫性疾病的治疗方法。

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