Selective Differences in the Expression of the Homing Receptors of Helper Lymphocyte Subsets

Samuele E. Burastero , Giovanni A. Rossi , Emanuele Crimi
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引用次数: 13

Abstract

Effector functions are acquired by mature CD4 T lymphocytes in an exquisitely antigen-specific and antigen-dependent fashion. T cell receptor recognition of the processed antigen presented on the major histocompatibility complex molecule by antigen-presenting cells dictates the specificity of the T cell clones that will be expanded. A complex array of further coreceptor and lymphokine-mediated interactions determines whether activation or inhibition will follow and which effector phenotype will be acquired by the lymphocytes. On the basis of a first antigen encounter, CD4 T cells are functionally defined as naive or memory/effector cells. In memory/effector T cells, the pattern of cytokine production permits further classification as Th1 or Th2 cells. Th1 cells mainly produce IFN-γ, whereas Th2 cells mainly produce IL-4. The functional properties of these cell subsets derive from the biological activities of these (and the related) lymphokines they produce. An established body of data supports the view that the migration of T lymphocytes is distinctively different in naive and memory/effector T cells. Both CD4 and CD8 memory/effector T cells selectively migrate into nonlymphoid organs, such as the skin, the gut, and the lung through the peripheral extravascular route, whereas naive T cells migrate through the high endothelial venules and enter lymphoid tissues, such as lymph nodes, Peyers' patches, and tonsils. Furthermore, the acquisition of a Th1 or Th2 profile further implies the coordinated expression of a relatively selective array of receptors capable of rerouting them differentially. These events have a dramatic effect on the outcome of an immune response and determine whether it will be protective or not. New therapeutic strategies can be envisaged that interfere with the key molecular processes taking place during these coordinated differentiation events.

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辅助淋巴细胞亚群归巢受体表达的选择性差异
成熟的CD4 T淋巴细胞以一种精巧的抗原特异性和抗原依赖性的方式获得效应功能。T细胞受体对抗原呈递细胞在主要组织相容性复合体分子上呈递的加工抗原的识别决定了扩增的T细胞克隆的特异性。一系列复杂的辅助受体和淋巴因子介导的相互作用决定了激活或抑制是否会发生,以及淋巴细胞将获得哪种效应表型。基于第一次抗原接触,CD4 T细胞在功能上被定义为初始细胞或记忆/效应细胞。在记忆/效应T细胞中,细胞因子产生的模式允许进一步分类为Th1或Th2细胞。Th1细胞主要产生IFN-γ,而Th2细胞主要产生IL-4。这些细胞亚群的功能特性源于它们产生的这些(和相关的)淋巴因子的生物活性。已有的大量数据支持这样的观点,即T淋巴细胞在初始T细胞和记忆/效应T细胞中的迁移明显不同。CD4和CD8记忆/效应T细胞通过外周血管外途径选择性迁移到非淋巴器官,如皮肤、肠道和肺,而幼稚T细胞通过高内皮小静脉迁移并进入淋巴组织,如淋巴结、佩耶斯斑块和扁桃体。此外,Th1或Th2基因谱的获得进一步暗示了一组相对选择性的受体的协调表达,这些受体能够以不同的方式重新路由它们。这些事件对免疫反应的结果有巨大的影响,并决定它是否具有保护作用。可以设想新的治疗策略,干扰在这些协调分化事件中发生的关键分子过程。
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