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小鼠免疫记忆的特征。I. 介导对绵羊红细胞IgM和IgG记忆的细胞早期分别产生。

Characteristics of immunological memory in mice. I. Separate early generation of cells mediating IgM and IgG memory to sheep erythrocytes.

作者信息

Black S J, Inchley C J

出版信息

J Exp Med. 1974 Aug 1;140(2):333-48. doi: 10.1084/jem.140.2.333.

Abstract

The kinetics of the generation of primed IgM and IgG antibody-forming cell precursors, and of helper T-cell populations, were analyzed in mice whose primary responses to high and low doses of SRBC were arrested at intervals by the immunosuppressive agents cyclophosphamide monohydrate and specific antibody. The extent to which immunological memory was established in these animals before blockade of the primary response was assessed by the hemolytic plaque assay following challenge 12 wk after priming. The presence of IgG B-memory cells and T-memory cells in suppressed mice was further investigated by the transfer into these animals of syngeneic SRBC-stimulated thymocytes or anti-theta-treated spleen cells. It was found that the progenitors of secondary IgM-synthesizing cells were primed almost immediately after injection of antigen, and that early blockade of the primary response resulted in a raised IgM response after challenge. On the other hand, priming for a secondary IgG response took at least 4 days, and was dose-dependent, although helper T populations for a secondary IgG response appeared 3 days after antigen injection. It appeared that both IgM and IgG memory cells may be considered as Y cells in terms of the X-Y-Z scheme of lymphocyte activation, but that the two populations are generated at different times after exposure to antigen. The size of either Y-cell population at any given time is dependent upon the amount of antigen available to provoke differentiation to antibody-forming Z cells, and the IgM Y-cell population in particular is likely to be depleted during the course of a normal 1 degrees response. When IgM Y cells were maintained for long periods as a result of immunosuppression, their secondary antibody response was independent of the primed T cells necessary for a secondary IgG response.

摘要

在对高剂量和低剂量绵羊红细胞(SRBC)产生初次应答的小鼠中,通过免疫抑制剂一水合环磷酰胺和特异性抗体间歇性阻断其初次应答,分析了致敏IgM和IgG抗体形成细胞前体以及辅助性T细胞群体的生成动力学。在初次应答被阻断前,通过致敏12周后攻击的溶血空斑试验评估这些动物中建立免疫记忆的程度。通过将同基因SRBC刺激的胸腺细胞或抗θ处理的脾细胞转移到这些动物中,进一步研究了受抑制小鼠中IgG B记忆细胞和T记忆细胞的存在情况。发现二次IgM合成细胞的祖细胞在注射抗原后几乎立即被致敏,并且初次应答的早期阻断导致攻击后IgM应答增强。另一方面,二次IgG应答的致敏至少需要4天,并且呈剂量依赖性,尽管二次IgG应答的辅助性T细胞群体在抗原注射后3天出现。就淋巴细胞激活的X-Y-Z模式而言,似乎IgM和IgG记忆细胞都可被视为Y细胞,但这两个群体在接触抗原后的不同时间产生。在任何给定时间,任一Y细胞群体的大小取决于可用于诱导分化为抗体形成Z细胞的抗原量,尤其是IgM Y细胞群体在正常初次应答过程中可能会被耗尽。当由于免疫抑制使IgM Y细胞长期维持时,它们的二次抗体应答独立于二次IgG应答所需的致敏T细胞。

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