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人类自体混合淋巴细胞反应中诱导细胞亚群的反应性及T8细胞活化

Reactivity of inducer cell subsets and T8-cell activation during the human autologous mixed lymphocyte reaction.

作者信息

Romain P L, Morimoto C, Daley J F, Palley L S, Reinherz E L, Schlossman S F

出版信息

Clin Immunol Immunopathol. 1984 Jan;30(1):117-28. doi: 10.1016/0090-1229(84)90012-6.

Abstract

To characterize the responding T cells in the autologous mixed lymphocyte reaction (AMLR), T cells were fractionated into purified subpopulations employing monoclonal antibodies and a variety of separation techniques including fluorescence-activated cell sorting. It was found that isolated T4 cells, but not T8 cells, proliferated in response to autologous non-T cells. More importantly, within the T4 subset, the autoreactive population was greatly enriched in a fraction reactive with an autoantibody from patients with juvenile chronic arthritis (JRA) or the monoclonal antibody anti-TQ1. Although T8 cells themselves were unable to proliferate in the AMLR, they could be induced to respond in the presence of either T4 cells or exogenous IL-2 containing medium. This was demonstrated by direct measurement of tritiated thymidine uptake by T8 cells during the course of the AMLR as well as by analysis of their relative DNA content. Taken together, these data indicate that the AMLR represents a complex pattern of immune responsiveness distinct from that observed in response to soluble antigen or alloantigen. The precise function of this T-cell circuit remains to be determined.

摘要

为了表征自体混合淋巴细胞反应(AMLR)中产生应答的T细胞,利用单克隆抗体和包括荧光激活细胞分选在内的多种分离技术,将T细胞分离为纯化的亚群。结果发现,分离出的T4细胞而非T8细胞会对自体非T细胞产生增殖反应。更重要的是,在T4亚群中,自身反应性群体在与青少年慢性关节炎(JRA)患者的自身抗体或单克隆抗体抗-TQ1反应的部分中大量富集。虽然T8细胞本身在AMLR中无法增殖,但在T4细胞或含外源性白细胞介素-2的培养基存在的情况下,它们可以被诱导产生反应。这通过在AMLR过程中直接测量T8细胞对氚标记胸腺嘧啶核苷的摄取以及分析它们的相对DNA含量得到了证实。综上所述,这些数据表明AMLR代表了一种不同于对可溶性抗原或同种异体抗原反应所观察到的复杂免疫应答模式。这种T细胞回路的确切功能仍有待确定。

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