Schmitt D
INSERM Unité 346, Clinique Dermatologique, Hôpital Edouard-Herriot, Lyon, France.
C R Seances Soc Biol Fil. 1994;188(3):207-21.
The skin is not only a physico-mechanical barrier between the environment and the body, but it also functions as an immune organ. The immunological function of epidermis is principally linked to the presence in this tissue of a distinct subpopulation of dendritic cells: the Langerhans cells (LC). LC constitute 2-4% of epidermal cell population and within epidermis they are the only cells which express MHC class II antigens constitutively. LC play a key role in the initiation of T cell responses to cutaneous antigens by picking up the antigen and migrating to the draining lymph node where they trigger specific T cell activation. There is also evidence that keratinocytes participate in immune responses in the skin since these cells produce a wide variety of cytokines that can modulate T cell responses. Dendritic cells comprise a system of highly efficient antigen-presenting cells which initiate immune responses such as the sensitization of T cells restricted by major histocompatibility complex molecules, the rejection of organ transplants and the formation of T-cell-dependent antibodies. Dendritic cells are found in many non-lymphoid tissues, such as skin and mucosa (Langerhans cells), and they migrate after antigen capture through the afferent lymph or the bloodstream to lymphoid organs, where they efficiently present antigen to T cells. Dendritic cells are difficult to isolate and, although they originate from bone marrow their growth and differentiation are still poorly characterized. Granulocyte macrophage-colony stimulating factor (GM-CSF) favours the out-growth of dendritic cells from mouse peripheral blood. The cooperation between GM-CSF and tumour necrosis factor-alpha (TNF-alpha) is crucial for the generation of human dendritic/Langerhans cells from CD34+ haematopoietic progenitors. The availability of large numbers of these cells should now facilitate the understanding of their role in immunological regulation and disorder. Recent studies reported that after 2-3 days in vitro incubation, both murine and human LC undergo profound phenotypic changes, as an enhancement in the expression of MHC class I and II antigens, LFA-3 and ICAM-1 molecules, a concomitant decrease of CD1a antigens and a loss of Fc gamma RII. Furthermore, cultured LC (cLC) lose or markedly reduce their specific cytoplasmic organelles: the Birbeck granules. Therefore, after a 2-3 days in vitro incubation, LC seem to acquire most of the features of lymphoid dendritic cells.(ABSTRACT TRUNCATED AT 400 WORDS)
皮肤不仅是环境与身体之间的物理机械屏障,还起着免疫器官的作用。表皮的免疫功能主要与该组织中一种独特的树突状细胞亚群——朗格汉斯细胞(LC)的存在有关。LC占表皮细胞总数的2%-4%,在表皮内它们是唯一持续表达MHC II类抗原的细胞。LC通过摄取抗原并迁移至引流淋巴结,在那里触发特异性T细胞活化,从而在T细胞对皮肤抗原的反应启动中发挥关键作用。也有证据表明角质形成细胞参与皮肤的免疫反应,因为这些细胞能产生多种可调节T细胞反应的细胞因子。树突状细胞构成了一个高效的抗原呈递细胞系统,可启动免疫反应,如受主要组织相容性复合体分子限制的T细胞致敏、器官移植排斥以及T细胞依赖性抗体的形成。树突状细胞存在于许多非淋巴组织中,如皮肤和黏膜(朗格汉斯细胞),它们在捕获抗原后通过输入淋巴管或血流迁移至淋巴器官,在那里有效地将抗原呈递给T细胞。树突状细胞难以分离,尽管它们起源于骨髓,但其生长和分化仍未得到充分表征。粒细胞巨噬细胞集落刺激因子(GM-CSF)有利于小鼠外周血中树突状细胞的生长。GM-CSF与肿瘤坏死因子-α(TNF-α)之间的协同作用对于从CD34+造血祖细胞生成人树突状/朗格汉斯细胞至关重要。大量获得这些细胞现在应有助于理解它们在免疫调节和疾病中的作用。最近的研究报道,在体外培养2-3天后,小鼠和人LC都会发生深刻的表型变化,如MHC I类和II类抗原、淋巴细胞功能相关抗原-3(LFA-3)和细胞间黏附分子-1(ICAM-1)分子表达增强,CD1a抗原同时减少以及FcγRII丧失。此外,培养的LC(cLC)会丢失或显著减少其特定的细胞质细胞器:伯贝克颗粒。因此,在体外培养2-3天后,LC似乎获得了淋巴样树突状细胞的大部分特征。(摘要截选至400字)
