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Expression of adhesion molecules on infiltrating T cells in thyroid glands from patients with Graves disease.

机译:Graves病患者甲状腺中浸润性T细胞上粘附分子的表达。

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摘要

The present study was performed to elucidate the role of adhesion molecules in the pathogenesis of Graves' disease. Peripheral blood and intrathyroidal mononuclear cells were obtained from 14 patients with Graves' disease. The expression of adhesion molecules and HLA-DR antigen on CD4+ cells and CD4+ cell subpopulations was analysed by the two- or three-colour immunofluorescence method. The expression of adhesion molecules including LFA-1 alpha, LFA-1 beta, CD2, VLA-4 alpha and VLA-5 alpha on CD4+ cells in the thyroid gland was markedly higher than that in peripheral blood. In peripheral blood CD4+ cell subsets, the CD4+ CD45RO+ cell population had an enhanced expression of the adhesion molecules compared with the CD4+ CD45RA+ cell population. However, there was no significant difference in the expression of adhesion molecules by CD4+ cell populations and subsets between Graves' disease and healthy subjects. The thyroid gland from Graves' disease contained a higher percentage of CD4+ CD45RO+ cells and a lower percentage of CD4+ CD45RA+ cells. In intrathyroidal CD4+ cell subsets, the CD4+ CD45RO+ cell population had an increased expression of LFA-1 and CD2 compared with the CD4+ CD45RA+ cell population, but there was no significant difference in VLA-4 and VLA-5 expression between the two cell subsets. Furthermore, the expression of LFA-1 and CD2 on the CD4+ CD45RO+ cell population in the thyroid was significantly higher than that in matched peripheral blood. A similar finding was also observed for the CD4+ CD45RA+ cell population. The thyroid gland had an increased percentage of CD4+ HLA-DR+ cells compared with matched or healthy peripheral blood. However, there was no significant difference in the percentage of HLA-DR+ cells in the thyroid gland between CD4+ CD45RO+ cell and CD4+ CD45RA+ cell populations. These results suggest that increased expression of adhesion molecules on CD4+ cells may be responsible for the migration of these cells into thyroid glands and cellular interactions between these cells and thyroid epithelial cells.
机译:进行本研究以阐明粘附分子在格雷夫斯病发病机理中的作用。从14名Graves病患者中获得了外周血和甲状腺内单核细胞。通过两色或三色免疫荧光法分析了CD4 +细胞和CD4 +细胞亚群上粘附分子和HLA-DR抗原的表达。在甲状腺的CD4 +细胞上,包括LFA-1α,LFA-1β,CD2,VLA-4α和VLA-5α在内的粘附分子的表达明显高于外周血。在外周血CD4 +细胞亚群中,与CD4 + CD45RA +细胞群体相比,CD4 + CD45RO +细胞群体的粘附分子表达增强。然而,在Graves病和健康受试者之间,CD4 +细胞群体和亚群的粘附分子表达没有显着差异。格雷夫斯氏病甲状腺的CD4 + CD45RO +细胞百分比较高,而CD4 + CD45RA +细胞百分比较低。在甲状腺内CD4 +细胞亚群中,与CD4 + CD45RA +细胞群相比,CD4 + CD45RO +细胞群的LFA-1和CD2表达增加,但是在两个细胞亚群之间,VLA-4和VLA-5表达没有显着差异。此外,甲状腺中CD4 + CD45RO +细胞群体中LFA-1和CD2的表达明显高于匹配的外周血。对于CD4 + CD45RA +细胞群体也观察到了类似的发现。与匹配或健康的外周血相比,甲状腺的CD4 + HLA-DR +细胞百分比增加。但是,在CD4 + CD45RO +细胞和CD4 + CD45RA +细胞群体之间,甲状腺中HLA-DR +细胞的百分比没有显着差异。这些结果表明,粘附分子在CD4 +细胞上的表达增加可能是这些细胞迁移到甲状腺以及这些细胞与甲状腺上皮细胞之间细胞相互作用的原因。

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