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HLA - B8、DR3阳性个体中T淋巴细胞活化标志物

Markers of T lymphocyte activation in HLA-B8, DR3 positive individuals.

作者信息

Modica M A, Zambito A M, Candore G, Caruso C

机构信息

Servizio di Immunologia Tissutale, Università di Palermo, Italy.

出版信息

Immunobiology. 1990 Nov;181(4-5):257-66. doi: 10.1016/S0171-2985(11)80517-6.

Abstract

Many autoimmune diseases are associated in Caucasians with HLA-B8 and/or HLA-DR3 antigens. There is evidence that bearers of these antigens may display significant changes in immune parameters when compared to individuals not having these antigens. Recently, increased numbers of blood activated T lymphocytes have been reported in the majority of these diseases. The increase in activated blood T lymphocytes is paradoxically characterized by an in vitro impairment of T cell activation. Particularly, an inadequate production of interleukins has been observed. We have studied blood levels of activated T cells in HLA-typed, healthy subjects. The results show that the percentage of activated T cells, as recognized by monoclonal antibodies anti-CD25, anti-Ia and anti-MLR3, was more frequent in HLA-B8, DR3 positive individuals. On the other hand, in the 24 h, PHA stimulated cultures IL-2, IFN-gamma and the percentage of T cells CD25 positive were decreased. Thus, there was an apparent discrepancy between the increase of blood activated T cells and the in vitro impaired T cell activation. Since there is evidence that HLA-B8, DR3 positive subjects are genetically low responders, a possible reason for the discrepancy might be their relative inability to remove antigenic stimuli from the body. In this case, the increased number of activated blood T cells may reflect a cellular activation caused by persistent antigenic stimulation.

摘要

在高加索人中,许多自身免疫性疾病与HLA - B8和/或HLA - DR3抗原相关。有证据表明,与没有这些抗原的个体相比,这些抗原的携带者可能在免疫参数上表现出显著变化。最近,在大多数这些疾病中都报告了血液中活化T淋巴细胞数量增加。矛盾的是,活化血液T淋巴细胞的增加表现为T细胞活化在体外受损。特别是,已经观察到白细胞介素产生不足。我们研究了HLA分型的健康受试者血液中活化T细胞的水平。结果表明,通过抗CD25、抗Ia和抗MLR3单克隆抗体识别的活化T细胞百分比在HLA - B8、DR3阳性个体中更常见。另一方面,在24小时PHA刺激培养物中,IL - 2、IFN - γ和CD25阳性T细胞百分比降低。因此,血液中活化T细胞的增加与体外T细胞活化受损之间存在明显差异。由于有证据表明HLA - B8、DR3阳性受试者在遗传上是低反应者,这种差异的一个可能原因可能是他们相对无法从体内清除抗原刺激。在这种情况下,活化血液T细胞数量的增加可能反映了由持续抗原刺激引起的细胞活化。

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