Spatiotemporal segregation of human marginal zone and memory B cell populations in lymphoid tissue

Yuan Zhao; Mohamed Uduman; Jacqueline H. Y. Siu; Thomas J Tull; Jeremy Sanderson; Bryan Wu; Julian Q. Zhou; Nedyalko Petrov; Richard J. Ellis; Katrina Todd; Konstantia-Maria Chavele; William Guesdon; Anna Vossenkämper; Wayel Jassem; David D’Cruz; David J. Fear; Susan John; Dagmar Scheel‐Toellner; Claire Hopkins; Estefanía Moreno; Natalie Woodman; Francesca D. Ciccarelli; Susanne Heck; Steven H. Kleinstein; Mats Bemark; Jo Spencer

doi:10.1038/s41467-018-06089-1

Spatiotemporal segregation of human marginal zone and memory B cell populations in lymphoid tissue

Yuan Zhao(King's College London), Mohamed Uduman(Yale University), Jacqueline H. Y. Siu(University of Cambridge), Thomas J Tull(King's College London), Jeremy Sanderson(King's College London), Bryan Wu(King's College London), Julian Q. Zhou(Yale University), Nedyalko Petrov(Guy's and St Thomas' NHS Foundation Trust), Richard J. Ellis(Guy's and St Thomas' NHS Foundation Trust), Katrina Todd(Guy's and St Thomas' NHS Foundation Trust), Konstantia-Maria Chavele(King's College London), William Guesdon(King's College London), Anna Vossenkämper(Queen Mary University of London), Wayel Jassem(King's College Hospital), David D’Cruz(King's College London), David J. Fear(King's College London), Susan John(King's College London), Dagmar Scheel‐Toellner(University of Birmingham), Claire Hopkins(King's College London), Estefanía Moreno(Queen Mary University of London), Natalie Woodman(King's College London), Francesca D. Ciccarelli(King's College London), Susanne Heck(Guy's and St Thomas' NHS Foundation Trust), Steven H. Kleinstein(Yale University), Mats Bemark(University of Gothenburg), Jo Spencer(King's College London)

Nature Communications

September 17, 2018

10.1038/s41467-018-06089-1

Cited by 103Open Access

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Abstract

Abstract Human memory B cells and marginal zone (MZ) B cells share common features such as the expression of CD27 and somatic mutations in their IGHV and BCL6 genes, but the relationship between them is controversial. Here, we show phenotypic progression within lymphoid tissues as MZ B cells emerge from the mature naïve B cell pool via a precursor CD27 − CD45RB MEM55+ population distant from memory cells. By imaging mass cytometry, we find that MZ B cells and memory B cells occupy different microanatomical niches in organised gut lymphoid tissues. Both populations disseminate widely between distant lymphoid tissues and blood, and both diversify their IGHV repertoire in gut germinal centres (GC), but nevertheless remain largely clonally separate. MZ B cells are therefore not developmentally contiguous with or analogous to classical memory B cells despite their shared ability to transit through GC, where somatic mutations are acquired.

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