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High-throughput antibody sequencing reveals genetic evidence of global regulation of the naive and memory repertoires that extends across individuals

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GENES AND IMMUNITY
卷 13, 期 6, 页码 469-473

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NATURE PUBLISHING GROUP
DOI: 10.1038/gene.2012.20

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antibodies; binding sites; antibody; immunologic memory; antibody specificity

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Vast diversity in the antibody repertoire is a key component of the adaptive immune response. This diversity is generated centrally through the assembly of variable, diversity and joining gene segments, and peripherally by somatic hypermutation and class-switch recombination. The peripheral diversification process is thought to only occur in response to antigenic stimulus, producing antigen-selected memory B cells. Surprisingly, analyses of the variable, diversity and joining gene segments have revealed that the naive and memory subsets are composed of similar proportions of these elements. Lacking, however, is a more detailed study, analyzing the repertoires of naive and memory subsets at the level of the complete V(D)J recombinant. This report presents a thorough examination of V(D)1 recombinants in the human peripheral blood repertoire, revealing surprisingly large repertoire differences between circulating B-cell subsets and providing genetic evidence for global control of repertoire diversity in naive and memory circulating B-cell subsets.

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