Literature DB >> 25535378

B-cell repertoire responses to varicella-zoster vaccination in human identical twins.

Chen Wang1, Yi Liu2, Mary M Cavanagh3, Sabine Le Saux3, Qian Qi3, Krishna M Roskin1, Timothy J Looney1, Ji-Yeun Lee1, Vaishali Dixit1, Cornelia L Dekker4, Gary E Swan5, Jörg J Goronzy6, Scott D Boyd7.   

Abstract

Adaptive immune responses in humans rely on somatic genetic rearrangements of Ig and T-cell receptor loci to generate diverse antigen receptors. It is unclear to what extent an individual's genetic background affects the characteristics of the antibody repertoire used in responding to vaccination or infection. We studied the B-cell repertoires and clonal expansions in response to attenuated varicella-zoster vaccination in four pairs of adult identical twins and found that the global antibody repertoires of twin pair members showed high similarity in antibody heavy chain V, D, and J gene segment use, and in the length and features of the complementarity-determining region 3, a major determinant of antigen binding. These twin similarities were most pronounced in the IgM-expressing B-cell pools, but were seen to a lesser extent in IgG-expressing B cells. In addition, the degree of antibody somatic mutation accumulated in the B-cell repertoire was highly correlated within twin pair members. Twin pair members had greater numbers of shared convergent antibody sequences, including mutated sequences, suggesting similarity among memory B-cell clonal lineages. Despite these similarities in the memory repertoire, the B-cell clones used in acute responses to ZOSTAVAX vaccination were largely unique to each individual. Taken together, these results suggest that the overall B-cell repertoire is significantly shaped by the underlying germ-line genome, but that stochastic or individual-specific effects dominate the selection of clones in response to an acute antigenic stimulus.

Entities:  

Keywords:  B cell repertoire; Varicella Zoster vaccine; antibody; convergent; twin

Mesh:

Substances:

Year:  2014        PMID: 25535378      PMCID: PMC4299233          DOI: 10.1073/pnas.1415875112

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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