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抗原驱动的免疫反应中B细胞的体细胞突变和克隆性扩增。

Somatic mutation and clonal expansion of B cells in an antigen-driven immune response.

作者信息

Sablitzky F, Wildner G, Rajewsky K

出版信息

EMBO J. 1985 Feb;4(2):345-50. doi: 10.1002/j.1460-2075.1985.tb03635.x.

Abstract

The variable (V) regions of three closely related monoclonal antibodies produced by hybridomas which had been isolated from a single mouse were sequenced at the level of the mRNA. The sequences and the restriction analysis of the immunoglobulin loci carried by the hybridoma cells indicate that the antibodies are derived from cells belonging to a single B cell clone. The sequence data imply a high frequency and stepwise occurrence of somatic point mutations in the expressed V region genes and substantial clonal expansion of B cells in the mouse. The mutations appear to be randomly introduced into heavy and light chain V region genes. Mutations are also seen in the complementarity determining regions which may thus have been involved in the selection of the cells producing the three antibodies.

摘要

对从同一只小鼠分离得到的杂交瘤产生的三种密切相关单克隆抗体的可变(V)区进行了mRNA水平的测序。杂交瘤细胞携带的免疫球蛋白基因座的序列和限制性分析表明,这些抗体源自属于单个B细胞克隆的细胞。序列数据表明,在表达的V区基因中,体细胞点突变出现的频率很高且呈逐步发生,并且小鼠体内的B细胞发生了大量的克隆扩增。这些突变似乎是随机引入重链和轻链V区基因的。在互补决定区也观察到了突变,因此这些突变可能参与了产生这三种抗体的细胞的选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa2e/554192/368f8022b14a/emboj00267-0071-a.jpg

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