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甲胎蛋白免疫调节活性中的细胞与遗传限制。I. 抗Ia相关增殖反应的选择性抑制

Cellular and genetic restrictions in the immunoregulatory activity of alpha-fetoprotein. I. Selective inhibition of anti-Ia-associated proliferative reactions.

作者信息

Peck A B, Murgita R A, Wigzell H

出版信息

J Exp Med. 1978 Mar 1;147(3):667-83. doi: 10.1084/jem.147.3.667.

Abstract

Alpha-fetoprotein (AFP), a major alpha-globulin component of fetal and newborn sera, has earlier been shown to exert significant immunosuppressive activity in vitro on T-dependent-immune responses. In the present investigation we have examined the effects of AFP on the recognition and proliferation of T lymphocytes responding in mixed leukocyte culture against histocompatibility-associated alloantigens. Fetal-derived AFP could be shown to exert differential effects on both primary and secondary responses ranging from strong inhibition to occasional enhancement, depending on the stimulating antigens. Proliferative responses against major histocompatibility complex (MHC) I region determinants, mediated predominantly by Ly 1 + cells, were markedly suppressed. Suppression was also observed in responses against Mls locus products, an antigenic system whose recognition requires concomitant recognition of I region gene products on the stimulating cells. In contrast, responses against MHC K or D region determinants, mediated predominantly by Ly 2 + cells, were generally unaffected by AFP. Similarly, non-MHC loci alloantigens distinct from Mls locus products also induced T-cell proliferation which was refractive to suppression by AFP. Because neither Ly 1 + nor Ly 2 + cells responding in this latter situation could be inhibited by AFP, we concluded that the mere fact that a T cell expresses a particular Ly phenotype does not predetermine sensitivity to AFP-induced suppression. In any case, AFP exerts a highly selective suppressive activity on I region-associated immune responses. These data may help to resolve the present controversy over the possibility that AFP has an in vivo relevance as an immunosuppressive agent by pointing out the importance of selecting proper genetic situations for study.

摘要

甲胎蛋白(AFP)是胎儿和新生儿血清中的一种主要α球蛋白成分,此前已表明它在体外对T细胞依赖性免疫反应具有显著的免疫抑制活性。在本研究中,我们检测了AFP对混合白细胞培养中针对组织相容性相关同种异体抗原作出反应的T淋巴细胞识别和增殖的影响。结果表明,来源于胎儿的AFP对初次和二次反应均可产生不同影响,从强烈抑制到偶尔增强不等,这取决于刺激抗原。针对主要组织相容性复合体(MHC)I区决定簇的增殖反应(主要由Ly 1 +细胞介导)受到明显抑制。在针对Mls位点产物的反应中也观察到抑制作用,Mls位点产物是一种抗原系统,其识别需要同时识别刺激细胞上的I区基因产物。相比之下,针对MHC K或D区决定簇的反应(主要由Ly 2 +细胞介导)通常不受AFP影响。同样,与Mls位点产物不同的非MHC位点同种异体抗原也可诱导T细胞增殖,且这种增殖不受AFP抑制。由于在上述后一种情况下作出反应的Ly 1 +和Ly 2 +细胞均不会被AFP抑制,我们得出结论,T细胞表达特定的Ly表型这一事实本身并不能预先决定其对AFP诱导抑制的敏感性。无论如何,AFP对I区相关免疫反应具有高度选择性的抑制活性。这些数据通过指出选择合适的遗传背景进行研究的重要性,可能有助于解决目前关于AFP作为免疫抑制剂在体内是否具有相关性的争议。

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