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Natural killer and natural killer-T cells in psoriasis.

机译:牛皮癣中的自然杀手和自然杀手T细胞。

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Psoriasis is characterized by a dermal and epidermal infiltrate comprised predominantly of CD4(+) and CD8(+) T cells, respectively. These cells behave in an antigen-dependent manner, which suggests that psoriasis may be a T-cell-mediated autoimmune disease. Psoriasis shares certain immunological features with recognized autoimmune conditions such as type I diabetes mellitus and multiple sclerosis, in both of which a pathogenic role is postulated for natural killer (NK) cells and natural killer-like T (NK-T) cells. However, there are few studies assessing the role of NK and NK-T cells in psoriasis. We sought to determine whether NK and NK-T cells are present in psoriasis. Skin biopsies were taken from the active edge of a psoriasis plaque and from uninvolved skin at least 5 cm away from involved skin of ten patients with chronic plaque psoriasis. Skin from four normal subjects was used as controls. Using an immunoperoxidase technique, cryostat sections were stained using antibodies to T-cell markers CD2, CD3, CD4 and CD8; cutaneous leucocyte associated antigen; NK cell markers CD16, CD56, CD57, CD94 and CD158a; and the NK-T cell marker CD161. There were significantly more cells expressing T cell markers, NK cell markers CD16, CD57, CD94 and CD158a and NK-T cell marker CD161 in involved skin than in uninvolved or normal skin ( P<0.01). There was no difference in the number of cells expressing CD56. Cells expressing NK markers were found most commonly in the papillary dermis immediately subjacent to the dermoepidermal junction. Cells expressing CD57 were found in significantly higher numbers in the epidermis and reticular dermis of involved skin. This study demonstrates that cells expressing NK markers and NK-T cell markers are present in plaques of psoriasis. The exact roles of NK and NK-T cells in psoriasis are unclear, although they may modulate autoimmune inflammation and act as a source of Th(1) cytokines important in the psoriatic process.
机译:牛皮癣的特征是真皮和表皮浸润分别主要由CD4(+)和CD8(+)T细胞组成。这些细胞以抗原依赖性方式起作用,这表明牛皮癣可能是T细胞介导的自身免疫性疾病。牛皮癣与公认的自身免疫疾病(例如I型糖尿病和多发性硬化症)具有某些免疫学特征,在这两种疾病中均假定自然杀伤(NK)细胞和自然杀伤性T(NK-T)细胞具有致病作用。但是,很少有研究评估NK和NK-T细胞在牛皮癣中的作用。我们试图确定牛皮癣中是否存在NK和NK-T细胞。从牛皮癣斑块的活动边缘和距十名患有慢性斑块牛皮癣的患者的受累皮肤至少5 cm处的未累及皮肤中进行皮肤活检。来自四个正常受试者的皮肤用作对照。使用免疫过氧化物酶技术,使用针对T细胞标记CD2,CD3,CD4和CD8的抗体对低温恒温器切片进行染色;皮肤白细胞相关抗原NK细胞标记CD16,CD56,CD57,CD94和CD158a;和NK-T细胞标记CD161。受累皮肤中表达T细胞标志物,NK细胞标志物CD16,CD57,CD94和CD158a以及NK-T细胞标志物CD161的细胞明显多于未受累或正常的皮肤(P <0.01)。表达CD56的细胞数量没有差异。表达NK标记的细胞最常见于紧邻表皮表皮交界处的乳头状真皮中。在受累皮肤的表皮和网状真皮中发现表达CD57的细胞数量明显增加。这项研究表明牛皮癣斑块中存在表达NK标志物和NK-T细胞标志物的细胞。 NK和NK-T细胞在牛皮癣中的确切作用尚不清楚,尽管它们可能调节自身免疫炎症并充当银屑病过程中重要的Th(1)细胞因子的来源。

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