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对(4-羟基-3-硝基苯基)乙酰半抗原超免疫反应中独特型表达改变的遗传基础。

Genetic basis for altered idiotype expression in the hyperimmune response to (4-hydroxy-3-nitrophenyl)acetyl hapten.

作者信息

White-Scharf M E, Imanishi-Kari T

出版信息

J Immunol. 1986 Aug 1;137(3):887-96.

PMID:3088116
Abstract

To assess the significance of somatic point mutation in the hyperimmune response to the hapten NP, an in vivo enrichment procedure was followed. Mice that expressed high titers of B1-8 idiotopic determinants were selected as donors for serial transfer of small numbers of immune spleen cells into syngeneic irradiated recipient mice. Cells expressing B1-8 idiotopic determinants were chosen for enrichment because B1-8 cross-reactive determinants constitute a significant portion of the primary response. Furthermore, B1-8 is a monoclonal antibody derived from a primary response to NP, and its heavy and light chains are unmutated products of the germ-line genes VH186.2 and VL lambda 1, respectively. The germ-line sequence is thus available for comparison with the somatic mutants that arise during enrichment and hyperimmunization. The data show that serial transfer of spleen cells from mice with a high titer of idiotypic determinants results in a dramatic decrease in the titers of antibodies that bind antigen. Three lines of evidence indicate that progeny cells from the initial lambda-positive, idiotype-bearing, antigen-binding cells are successfully transferred and expanded during successive adoptive transfers. First, the proportion of lambda-bearing antibodies relative to NP-specific lambda-bearing antibodies increases with transfer, which is consistent with mutation away from antigen binding. Second, analysis of serum antibodies and hybridoma proteins derived from transfer-recipient mice confirm the presence of idiotype-positive antibodies that do not bind antigen. Third, RNA dot blot analysis of hybridomas constructed from a recipient mouse in the fourth transfer indicates a high frequency of expression of the VH gene predominantly used in the NP response. Many of the antibodies expressed by these hybridomas not only do not bind antigen, but have also lost the determinants recognized by the anti-idiotypic reagents. Most of these VH-positive hybridomas express lambda L chain. The most likely interpretation of the data is that somatic mutation is occurring during the hyperimmune response. Because we selected donor mice that expressed a high titer of idiotype-positive, antigen-specific antibody and immunized the recipient mice, we expected to observe a selective expansion of somatic variants that bound antigen. This was not the case. The observed loss of antigen binding suggests that the majority of mutations arising result in antibodies with lower affinity for the immunizing antigen.

摘要

为了评估体细胞点突变在对半抗原NP的超免疫反应中的意义,我们采用了一种体内富集程序。选择表达高滴度B1-8独特型决定簇的小鼠作为供体,将少量免疫脾细胞连续转移到同基因照射的受体小鼠体内。选择表达B1-8独特型决定簇的细胞进行富集,因为B1-8交叉反应决定簇构成了初次反应的很大一部分。此外,B1-8是一种源自对NP初次反应的单克隆抗体,其重链和轻链分别是种系基因VH186.2和VL lambda 1的未突变产物。因此,种系序列可用于与富集和超免疫过程中出现的体细胞突变体进行比较。数据显示,从高滴度独特型决定簇的小鼠连续转移脾细胞会导致结合抗原的抗体滴度急剧下降。三条证据表明,最初的λ阳性、携带独特型、结合抗原的细胞的后代细胞在连续的过继转移过程中成功转移并扩增。首先,携带λ的抗体相对于NP特异性携带λ的抗体的比例随着转移而增加,这与远离抗原结合的突变一致。其次,对来自转移受体小鼠的血清抗体和杂交瘤蛋白的分析证实了存在不结合抗原的独特型阳性抗体。第三,对第四次转移中受体小鼠构建的杂交瘤进行RNA点杂交分析表明,主要用于NP反应的VH基因表达频率很高。这些杂交瘤表达的许多抗体不仅不结合抗原,而且还失去了抗独特型试剂识别的决定簇。这些VH阳性杂交瘤大多表达λ轻链。对数据最可能的解释是,超免疫反应过程中发生了体细胞突变。因为我们选择了表达高滴度独特型阳性、抗原特异性抗体的供体小鼠并对受体小鼠进行免疫,我们预期会观察到结合抗原的体细胞变体的选择性扩增。但情况并非如此。观察到的抗原结合丧失表明,产生的大多数突变导致抗体对免疫抗原的亲和力降低。

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