首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Expression of HLA-DR molecules by keratinocytes and presence of Langerhans cells in the dermal infiltrate of active psoriatic plaques
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Expression of HLA-DR molecules by keratinocytes and presence of Langerhans cells in the dermal infiltrate of active psoriatic plaques

机译:角质形成细胞表达HLA-DR分子并且在活动性银屑病斑块的真皮浸润液中存在朗格汉斯细胞

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摘要

Immunoperoxidase staining of skin sections and immunofluorescence analysis of keratinocyte suspensions obtained from suction blisters of psoriatic plaques were performed using an mAb, Josh 524.4.1, and Fab'2 fragments of a rabbit antiserum, both of which are directed against nonpolymorphic determinants of HLA-DR molecules. HLA-DR+ keratinocytes were present in plaques, but not normal-appearing skin, from a significant portion of patients with active psoriasis. Double-labelling immunofluorescence experiments with either the monoclonal or polyclonal anti-HLA-DR antibody, in conjunction with the mAb OKT6, which identifies DR+ Langerhans cells, demonstrated that HLA-DR molecules were present on OKT6- keratinocytes. The dermal infiltrate of psoriatic plaques contained T cells expressing the activation antigens, IL-2 receptor (Tac) and HLA-DR, as well as macrophages and OKT6+ cells. There was little difference in the characteristics of the dermal infiltrate between the lesions with or without HLA-DR+ keratinocytes. OKT6+ presumptive Langerhans cells were also found in the dermal infiltrates of patients with lichen planus, contact dermatitis, spongiotic dermatitis, erythema multiforme, basal and squamous cell carcinoma. Studies of keratinocyte suspensions showed that 7-84% of keratinocytes were HLA-DR+. Flow cytometry experiments showed that keratinocytes at all stages of differentiation were HLA-DR+. However, the stem cell-enriched population contained the highest proportion of HLA-DR+ cells. HLA-DR expression by keratinocytes correlated with disease activity. The expression was reversible with successful medical therapy. HLA-DR+ keratinocytes may activate T cells directly or may present an as yet unknown antigen to T cells. These studies provide further support for the hypothesis that immunological mechanisms play an important role in the pathogenesis of psoriasis.
机译:使用mAb,Josh 524.4.1和兔抗血清的Fab'2片段对皮肤切片的免疫过氧化物酶染色和从牛皮癣斑块的吸水泡中获得的角质形成细胞悬液进行免疫荧光分析,这两个片段均针对HLA-的非多态决定簇DR分子。 HLA-DR +角质形成细胞存在于大部分活动性银屑病患者的斑块中,但不正常出现在皮肤中。使用单克隆或多克隆抗HLA-DR抗体与可鉴定DR + Langerhans细胞的mAb OKT6进行的双标记免疫荧光实验表明,HLA-DR分子存在于OKT6-角质形成细胞上。牛皮癣斑块的皮肤浸润含有表达激活抗原的T细胞,IL-2受体(Tac)和HLA-DR,以及巨噬细胞和OKT6 +细胞。有或没有HLA-DR +角质形成细胞的病灶之间的皮肤浸润特性差异不大。在扁平苔藓,接触性皮炎,海绵状皮炎,多形性红斑,基底和鳞状细胞癌患者的皮肤浸润中还发现了OKT6 +推测的Langerhans细胞。对角质形成细胞悬浮液的研究表明,7-84%的角质形成细胞为HLA-DR +。流式细胞仪实验表明,分化的各个阶段的角质形成细胞均为HLA-DR +。但是,富含干细胞的群体包含最高比例的HLA-DR +细胞。角质形成细胞的HLA-DR表达与疾病活动相关。该表达在成功的药物治疗中是可逆的。 HLA-DR +角质形成细胞可以直接激活T细胞,也可以向T细胞呈递未知抗原。这些研究为免疫机制在银屑病发病机理中起重要作用的假说提供了进一步的支持。

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