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用于分析抗半抗原反应亲和力成熟的抗体工程。

Antibody engineering for the analysis of affinity maturation of an anti-hapten response.

作者信息

Allen D, Simon T, Sablitzky F, Rajewsky K, Cumano A

机构信息

Institut für Genetik der Universität zu Köln, FRG.

出版信息

EMBO J. 1988 Jul;7(7):1995-2001. doi: 10.1002/j.1460-2075.1988.tb03038.x.

Abstract

The influence of structural variation, previously observed in a panel of V186.2 VH/V lambda 1-expressing anti-NP antibodies from the secondary response, on the affinity of these antibodies was examined by site-specific mutagenesis and recombinant antibody construction. A tryptophan----leucine exchange at position 33 in the VH segment of all but one of the high-affinity antibodies is the most frequently observed somatic mutation and by itself leads to a 10-fold higher affinity; all other somatic exchanges are irrelevant for affinity selection. In the single case of a high-affinity antibody without this common exchange, high affinity is mediated by a combination of mutations (including a one-codon deletion) in VH and the particular D-JH rearrangement carried by this antibody. The data indicate that the pattern of somatic diversification through hypermutation is shaped by affinity selection, but that only a single point mutation is available in the VH and the VL gene of lambda 1 chain-bearing anti-NP antibodies which by itself leads to an increase of hapten-binding affinity. Based on the analysis of two secondary response antibodies from which somatic mutations in VH and VL have been eliminated, it is also concluded that the recruitment of B cell clones into the pathway of hypermutation involves a mechanism which is not based upon affinity differences towards the antigen.

摘要

通过位点特异性诱变和重组抗体构建,研究了先前在一组来自二次应答的表达V186.2 VH/Vλ1的抗NP抗体中观察到的结构变异对这些抗体亲和力的影响。除一种高亲和力抗体外,所有高亲和力抗体VH区段第33位的色氨酸→亮氨酸交换是最常观察到的体细胞突变,其本身可使亲和力提高10倍;所有其他体细胞交换与亲和力选择无关。在没有这种常见交换的高亲和力抗体的单个案例中,高亲和力由VH中的突变组合(包括一个密码子缺失)以及该抗体携带的特定D-JH重排介导。数据表明,通过超突变进行的体细胞多样化模式受亲和力选择的影响,但对于携带λ1链的抗NP抗体,VH和VL基因中只有单个点突变可导致半抗原结合亲和力增加。基于对两种已消除VH和VL体细胞突变的二次应答抗体的分析,还得出结论,B细胞克隆进入超突变途径涉及一种不基于对抗原亲和力差异的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8504/454473/5ba81ccc831c/emboj00144-0077-a.jpg

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