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流感血凝素抗体应答中的克隆间及克隆内多样性。

Inter- and intraclonal diversity in the antibody response to influenza hemagglutinin.

作者信息

Clarke S H, Huppi K, Ruezinsky D, Staudt L, Gerhard W, Weigert M

出版信息

J Exp Med. 1985 Apr 1;161(4):687-704. doi: 10.1084/jem.161.4.687.

Abstract

This study focuses on 10 BALB/c anti-influenza virus (A/PR/8/34) hemagglutinin antibodies that have light chains encoded by the same variable region kappa chain (V kappa) gene, V kappa 21C. A comparison of antibodies from lymphocytes of independent origin reveals the contribution of germline diversity (combinatorial joining and association) to this response. Although combinatorial joining and association contribute to sequence diversity, they appear to have little effect on the fine specificity of these antibodies. Somatic mutation, in addition to contributing to the sequence diversity of these antibodies, creates differences in their fine specificity. The extent of mutation and its effect on fine specificity can be seen by comparing antibodies of lymphocytes from the same clone. These intraclonal comparisons also indicate that somatic mutation is an ongoing process occurring at a high rate (estimated to be at least 10(-3) mutations per base pair per division) in the expressed V region heavy chain (VH) and V kappa genes. Furthermore, both the nature and distribution of these mutations suggest that amino acid replacement mutations in the light but not the heavy chain are selected for by antigen.

摘要

本研究聚焦于10种BALB/c抗流感病毒(A/PR/8/34)血凝素抗体,这些抗体的轻链由相同的可变区κ链(Vκ)基因Vκ21C编码。对来自独立来源淋巴细胞的抗体进行比较,揭示了种系多样性(组合连接和关联)对这种反应的贡献。尽管组合连接和关联有助于序列多样性,但它们似乎对这些抗体的精细特异性影响很小。体细胞突变除了有助于这些抗体的序列多样性外,还会造成它们精细特异性的差异。通过比较来自同一克隆的淋巴细胞抗体,可以看出突变程度及其对精细特异性的影响。这些克隆内比较还表明,体细胞突变是一个持续进行的过程,在表达的V区重链(VH)和Vκ基因中以高频率发生(估计每碱基对每次分裂至少有10^(-3)个突变)。此外,这些突变的性质和分布表明,抗原选择的是轻链而非重链中的氨基酸置换突变。

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