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人类IgM+IgD+B细胞是外周血中主要的B细胞亚群,其一生中表达的Vκ基因没有或仅有少量体细胞突变。

Human IgM+IgD+ B cells, the major B cell subset in the peripheral blood, express V kappa genes with no or little somatic mutation throughout life.

作者信息

Klein U, Küppers R, Rajewsky K

机构信息

Institute for Genetics, University of Cologne, FRG.

出版信息

Eur J Immunol. 1993 Dec;23(12):3272-7. doi: 10.1002/eji.1830231232.

Abstract

Peripheral blood B cells of a 67-year-old person were separated into IgM+IgD+, IgM+IgD-, and IgM-IgD- subsets, and nucleotide sequences of expressed immunoglobulin light chain variable (V) regions encoded by V kappa 3 and V kappa 4 gene family members were determined from amplified cDNA. V region sequences from IgM+IgD+ cells (the major B cell population in the blood) showed no or little somatic mutation (0.3%), in contrast to V kappa sequences from IgM+IgD- and IgM-IgD- B cells (2.0% and 3.9%, respectively). This suggests that in the human like in the mouse, and independently of age, somatically mutated memory B cells accumulate in the compartment of IgM-IgD- cells, whereas the IgM+IgD+ subpopulation consists of cells whose antibody repertoire is mainly determined by V region gene rearrangements and N-region insertion, at the molecular level. The somatically mutated IgM+IgD- cells may represent early descendants of IgM+IgD+ cells recruited into the memory cell compartment.

摘要

一名67岁个体的外周血B细胞被分离为IgM+IgD+、IgM+IgD-和IgM-IgD-亚群,并从扩增的cDNA中确定了由Vκ3和Vκ4基因家族成员编码的表达免疫球蛋白轻链可变(V)区的核苷酸序列。与IgM+IgD-和IgM-IgD-B细胞的Vκ序列(分别为2.0%和3.9%)相比,IgM+IgD+细胞(血液中的主要B细胞群体)的V区序列显示无或几乎没有体细胞突变(0.3%)。这表明,在人类中,与小鼠类似,且与年龄无关,体细胞突变的记忆B细胞在IgM-IgD-细胞区室中积累,而IgM+IgD+亚群由其抗体库主要在分子水平上由V区基因重排和N区插入决定的细胞组成。体细胞突变的IgM+IgD-细胞可能代表被招募到记忆细胞区室的IgM+IgD+细胞的早期后代。

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