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2型非胸腺依赖性抗原诱导长期的IgG相关网络记忆。

Thymus-independent type 2 antigen induces a long-term IgG-related network memory.

作者信息

Lange Hans, Zemlin Michael, Tanasa Radu Iulian, Trad Ahmad, Weiss Thomas, Menning Hauke, Lemke Hilmar

机构信息

Biochemical Institute of the Medical Faculty, Christian-Albrechts-Universität Kiel, Otto Meyerhof-Haus, Rudolf Höberstrasse 1, Kiel, Germany.

出版信息

Mol Immunol. 2008 May;45(10):2847-60. doi: 10.1016/j.molimm.2008.01.020. Epub 2008 Mar 10.

DOI:10.1016/j.molimm.2008.01.020
PMID:18329101
Abstract

Thymus-independent type 2 (TI-2) antigens occasionally induce long-lasting IgM memory, but do not prime for typical secondary IgG responses. However, contrary to current understanding, we detected several TI-2-induced long-term memory effects in subsequent thymus-dependent (TD) responses to the hapten 2-phenyloxazolone coupled to a protein carrier. The early primary TD response, even 3 months after TI-2 immunization, included non-mutated IgM as well as IgG antibodies exhibiting higher affinities than the Ox1 idiotype which dominates and has highest affinity in sole TD responses. The secondary exclusive IgG response 8 weeks later contained major hitherto non-observed clones. Somatic hypermutation on the normally dominant V(H)Ox1 gene was largely silenced while the associated VkappaOx1 exhibited the classical affinity-enhancing mutations, thus suggesting a separate regulation of this process for V(H) and V(L) genes. Mutations accumulated in genes which normally are rarely or non-expressed or non-mutating. First evidence is presented that receptor revision by V(H) replacement may occur during immune maturation in genetically non-engineered wildtype mice. We conclude that the TI-2 antigen-induced altered selection of TD Ag-inducible clones and its severe gene-specific influence on further somatic mutations and affinity maturation represents a network memory, which we hypothesize to be mediated by anti-idiotypic regulatory T cells.

摘要

2型非胸腺依赖性(TI-2)抗原偶尔会诱导产生持久的IgM记忆,但不会引发典型的继发性IgG反应。然而,与目前的认识相反,我们在随后对半抗原2-苯基恶唑酮与蛋白质载体偶联物的胸腺依赖性(TD)反应中检测到了几种TI-2诱导的长期记忆效应。即使在TI-2免疫后3个月,早期的原发性TD反应也包括未发生突变的IgM以及亲和力高于Ox1独特型的IgG抗体,Ox1独特型在单独的TD反应中占主导地位且具有最高亲和力。8周后的继发性特异性IgG反应包含了迄今为止主要未观察到的克隆。通常占主导地位的V(H)Ox1基因上的体细胞超突变在很大程度上被沉默,而相关的VkappaOx1则表现出经典的亲和力增强突变,因此表明该过程对V(H)和V(L)基因有单独的调控。突变积累在通常很少表达、不表达或不发生突变的基因中。首次有证据表明,在未经过基因工程改造的野生型小鼠的免疫成熟过程中,可能会发生通过V(H)替换进行的受体编辑。我们得出结论,TI-2抗原诱导的TD抗原诱导性克隆选择改变及其对进一步体细胞突变和亲和力成熟的严重基因特异性影响代表了一种网络记忆,我们假设这种记忆是由抗独特型调节性T细胞介导的。

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