Cruz P D, Bergstresser P R
Department of Dermatology, University of Texas Southwestern Medical Center, Dallas.
Dermatol Clin. 1990 Oct;8(4):633-47.
The seminal observation made 30 years ago that T cells do not discriminate between native and denatured proteins, whereas B cells generally do, can now be explained by the fact that T cells never see antigens in their native conformation and that intact proteins cannot associate simultaneously with MHC molecules and the TCR. This difference in the ability to recognize antigen based on conformational specificity appears to be a consequence of the fact that the T cell sees antigen not free in solution, but on the surface of an APC in association with MHC molecules. The metabolic events that protein antigens undergo within APC, prior to their presentation in an appropriately processed form to T cells, are called antigen processing. The end-product of antigen processing for CD4+ T cells is a relatively short peptide fragment bound to class II MHC molecules on the surface of an APC that can be recognized by the TCR on the T cells. Because this event is difficult to monitor directly, antigen processing can only be assayed in conjunction with the temporally distal event of T-cell activation, manifested ultimately as proliferative responses or lymphokine secretion. In addition to occupancy of the TCR by the peptide/class II complex, several other antigen-nonspecific receptor-ligand interactions between APC and T cells are required for optimal T-cell activation. M phi, B cells, and LC/DC comprise the principal APC for CD4+ T cells. M phi and B cells have been studied extensively with respect to their antigen processing and presenting capacities. Only recently, however, have such capacities been investigated in LC and DC; these studies now indicate freshly isolated LC (but not cultured LC and DC) to possess efficient antigen processing capabilities. In this respect, LC have been proposed to represent evolving (or "maturing") forms of DC: Freshly isolated LC (which retain morphologic and functional properties of epidermal LC in situ) are the equivalent of tissue forms of DC, whereas cultured LC resemble lymphoid or circulating DC. Cultured LC and DC appear to be the sole effective APC for inducing primary T-cell responses in vitro. Possibly underlying this property is the ability of cultured LC and DC (but not M phi, B cells, or freshly isolated LC) to induce formation of T-cell clusters during the course of such responses. The capacity of accessory cells to function as APC varies depending upon the type of APC and T cells examined.(ABSTRACT TRUNCATED AT 400 WORDS)
30年前有一项具有开创性的观察结果,即T细胞不会区分天然蛋白质和变性蛋白质,而B细胞通常会区分,现在这一现象可以这样解释:T细胞从未见过处于天然构象的抗原,而且完整的蛋白质无法同时与MHC分子和TCR结合。基于构象特异性识别抗原的能力差异,似乎是由于T细胞看到的抗原不是游离于溶液中,而是与MHC分子结合在抗原呈递细胞(APC)表面。蛋白质抗原在APC内经历代谢事件,然后以适当加工的形式呈递给T细胞,这些代谢事件称为抗原加工。CD4+ T细胞的抗原加工最终产物是一个相对较短的肽片段,它与APC表面的II类MHC分子结合,能够被T细胞上的TCR识别。由于这一过程难以直接监测,抗原加工只能与T细胞激活这一在时间上较晚发生的事件一起检测,最终表现为增殖反应或淋巴因子分泌。除了肽/II类复合物占据TCR外,APC与T细胞之间的其他几种非抗原特异性受体-配体相互作用对于最佳的T细胞激活也是必需的。巨噬细胞(M phi)、B细胞以及朗格汉斯细胞/树突状细胞(LC/DC)是CD4+ T细胞的主要APC。关于M phi和B细胞的抗原加工和呈递能力,已经进行了广泛研究。然而,直到最近才对LC和DC的这种能力进行研究;这些研究现在表明,新鲜分离的LC(但不是培养的LC和DC)具有高效的抗原加工能力。在这方面,有人提出LC代表DC的进化(或“成熟”)形式:新鲜分离的LC(保留了原位表皮LC的形态和功能特性)等同于DC的组织形式,而培养的LC类似于淋巴样或循环DC。培养的LC和DC似乎是体外诱导原发性T细胞反应的唯一有效APC。这种特性的潜在原因可能是培养的LC和DC(但不是M phi、B细胞或新鲜分离的LC)在这种反应过程中能够诱导T细胞簇的形成。辅助细胞作为APC发挥功能的能力因所检测的APC和T细胞类型而异。(摘要截选至400词)
