首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Antigen-specific suppression of human antibody responses by allogeneic T cells. I. Frequency and antigen specificity of allogeneic suppressor T cells and their role in major histocompatibility complex-controlled genetic restriction
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Antigen-specific suppression of human antibody responses by allogeneic T cells. I. Frequency and antigen specificity of allogeneic suppressor T cells and their role in major histocompatibility complex-controlled genetic restriction

机译:同种异体T细胞对人抗体反应的抗原特异性抑制。一同种异体抑制性T细胞的频率和抗原特异性及其在主要组织相容性复合物控制的遗传限制中的作用

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摘要

Specific antibody responses to influenza virus were obtained in vitro from human blood mononuclear cells (PBM). The addition of allogeneic T cells to responding PBM profoundly suppressed antigen-induced antibody responses, but had no effect on pokeweed mitogen (PWM)-induced polyclonal Ig formation. This raised the possibility that suppression by allogeneic T cells may result from the activation of antigen- specific T suppressor (Ts) cells rather than nonspecific allogeneic effects. The frequency of allogeneic Ts in PBM from a number of different donors, estimated in a series of limiting dilution analyses, was found to range from 0.8 X 10(-5) to 4.5 X 10(-5), which is more typical of antigen-specific than alloreactive T cells. By adding limiting numbers of allogeneic T cells to antibody-forming cultures stimulated simultaneously with two non-cross-reacting antigens (influenza A and B strain viruses A/X31 and B/HK), it was possible to demonstrate suppression of the response to one antigen, but not the other, in the same culture well. Moreover, the frequency of wells in which the response to both antigens was suppressed was not significantly different from that predicted from the calculated frequency of specific allogeneic Ts. These results show that allogeneic suppression was antigen specific, and was not due to non-specific allogeneic effects. By separating T cell preparations into Leu-3a+ (helper) and Leu-2a+ (suppressor/cytotoxic) T cell subsets, suppression was shown to be mediated by a radiosensitive Leu-2a+ T cell. The removal of Leu-2a+ cells from T cell preparations abrogated the suppressor effect and permitted T cell collaboration with B cells, across an HLA-A, -B, and -DR barrier. This result shows that in at least some combinations, suppression rather than major histocompatibility complex restriction is the reason for the failure of allogeneic T and B cells to collaborate in T cell-dependent antibody responses.
机译:从人血单核细胞(PBM)体外获得了针对流感病毒的特异性抗体反应。向反应性PBM中添加同种异体T细胞可显着抑制抗原诱导的抗体反应,但对商陆有丝分裂原(PWM)诱导的多克隆Ig的形成没有影响。这增加了同种异体T细胞抑制作用可能是由于抗原特异性T抑制物(Ts)细胞活化而不是非特异性同种异体作用引起的可能性。在一系列有限稀释分析中估计,来自许多不同供体的PBM中同种异体Ts的频率范围为0.8 X 10(-5)至4.5 X 10(-5),这在抗原中更为典型特异性高于同种反应性T细胞。通过将有限数量的同种异体T细胞添加到同时受两种非交叉反应抗原(甲型和乙型流感病毒A / X31和B / HK)刺激的抗体形成培养物中,可以证明对一种应答的抑制作用抗原,而不是其他抗原,可以在同一培养物中很好地进行。此外,对两种抗原的反应均被抑制的孔的频率与根据特定异体Ts的计算频率预测的频率没有显着差异。这些结果表明,同种异体抑制是抗原特异性的,而不是由于非特异性同种异体作用。通过将T细胞制剂分为Leu-3a +(辅助)和Leu-2a +(抑制剂/细胞毒性)T细胞亚群,抑制作用被证明是由放射敏感性Leu-2a + T细胞介导的。从T细胞制备物中除去Leu-2a +细胞消除了抑制作用,并允许T细胞与B细胞跨越HLA-A,-B和-DR屏障。该结果表明,至少在某些组合中,抑制而不是主要的组织相容性复合物限制是同种异体T细胞和B细胞未能参与T细胞依赖性抗体反应的原因。

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