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T淋巴细胞在体液免疫反应中的作用。II. T细胞介导的抗体亲和力调节。

Role of t lymphocytes in the humoral immune response. II. T cell-mediated regulation of antibody avidity.

作者信息

Warren R W, Murphy S, Davie J M

出版信息

J Immunol. 1976 May;116(5):1385-90.

PMID:58032
Abstract

The effect of activated T lymphocytes (ATC) on the avidity distribution of PFC in the secondary response was studied in normal mice. The total PFC response was not significantly changed for either direct or indirect PFC by administration of ATC before secondary antigen challenge. However, marked suppression occurred of indirect PFC that secreted high avidity antibody; no suppression was seen of high avidity direct PFC. At the same time, significant stimulation was seen of relative and absolute frequencies of indirect PFC that secreted middle and low avidity antibody. These effects were dependent on Thy 1-bearing, nylon nonadherent cells which demonstrated carrier specificity. In further characterization of these effects, it was found that increasing the number of ATC transferred produced progressive loss of high avidity PFC and compensatory increase in lower avidity PFC. Moreover, in these experiments, suppression of the high avidity response was inducible with the administration of ATC 5 weeks before to 3 days after the secondary immunization. Thus, it is likely that the avidity-modifying effects are dependent on T lymphocytes which influence the late stages of B lymphocyte maturation.

摘要

在正常小鼠中研究了活化T淋巴细胞(ATC)对二次应答中PFC亲和力分布的影响。在二次抗原攻击前给予ATC,直接或间接PFC的总PFC应答均无显著变化。然而,分泌高亲和力抗体的间接PFC出现明显抑制;高亲和力直接PFC未见抑制。同时,分泌中低亲和力抗体的间接PFC的相对和绝对频率出现显著刺激。这些效应依赖于具有Thy 1、不黏附尼龙的细胞,这些细胞表现出载体特异性。在对这些效应的进一步表征中,发现增加转移的ATC数量会导致高亲和力PFC逐渐减少,低亲和力PFC代偿性增加。此外,在这些实验中,在二次免疫前5周直至免疫后3天给予ATC均可诱导高亲和力应答的抑制。因此,亲和力调节效应可能依赖于影响B淋巴细胞成熟后期的T淋巴细胞。

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