首页> 外文期刊>Autoimmunity >Peripheral blood lymphocytes analysis detects CD100/SEMA4D alteration in systemic sclerosis patients.
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Peripheral blood lymphocytes analysis detects CD100/SEMA4D alteration in systemic sclerosis patients.

机译:外周血淋巴细胞分析可检测系统性硬化症患者的CD100 / SEMA4D改变。

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摘要

It was suggested that the immune system plays an important role at least in the amplification of the main elements in systemic sclerosis (SSc), an autoimmune disease with an incompletely elucidated pathogenesis. Elucidation of the mechanisms involved in the interaction between T and B cells, major players of the immune system, could contribute to a better understanding of some of clinical and pathological manifestations of SSc. Recently, abnormalities in Semaphorin 4D (Sema4D/CD100) or CD72, two contrareceptors involved in T and B cells cooperation, were associated with autoimmunity. Therefore, we investigated CD100 and CD72 expression level on T and B cells in attempting to establish their role in SSc pathogenesis. The results revealed augmented percentages of CD100(high) T and B cells, significantly increased expression of CD100 on CD4(+) T cells and frequently detectable levels of soluble CD100 in SSc patient sera compared to healthy donors. In SSc, CD100 dysregulations were associated with anti-Scl70 antibodies production, disease type, thickening of skin, disease duration, or with active inflammation processes. In consequence, dysregulations in CD100 expression and release could play a role in SSc development and/or maintenance.
机译:提示免疫系统至少在系统性硬化症(SSc)的主要成分的扩增中起重要作用,系统性硬化症是一种自身免疫性疾病,发病机理尚未完全阐明。阐明免疫系统的主要参与者T细胞和B细胞之间的相互作用所涉及的机制,可能有助于更好地理解SSc的某些临床和病理表现。最近,Semaphorin 4D(Sema4D / CD100)或CD72(参与T细胞和B细胞合作的两个受体)异常与自身免疫有关。因此,我们调查了T细胞和B细胞上CD100和CD72的表达水平,以试图确定它们在SSc发病机理中的作用。结果显示与健康供体相比,SSc患者血清中CD100(高)T细胞和B细胞的百分比增加,CD4(+)T细胞上CD100的表达显着增加,可溶性CD100的水平经常可检测到。在SSc中,CD100失调与抗Scl70抗体的产生,疾病类型,皮肤增厚,疾病持续时间或活跃的炎症过程有关。因此,CD100表达和释放失调可能在SSc的发育和/或维持中起作用。

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