Shared B cell memory to coronaviruses and other pathogens varies in human age groups and tissues

Author:

Yang Fan,Nielsen Sandra C. A.,Hoh Ramona A.,Lee Ji-Yeun,Pham Tho D.,Jackson Katherine J. L.,Roskin Krishna M.,Liu Yi,Ohgami Robert S.,Osborne Eleanor M.,Niemann Claus U.,Parsonnet Julie,Boyd Scott D.ORCID

Abstract

AbstractVaccination and infection promote the formation, tissue distribution, and clonal evolution of B cells encoding humoral immune memory. We evaluated convergent antigen-specific antibody genes of similar sequences shared between individuals in pediatric and adult blood, and deceased organ donor tissues. B cell memory varied for different pathogens. Polysaccharide antigen-specific clones were not exclusive to the spleen. Adults’ convergent clones often express mutated IgM or IgD in blood and are class-switched in lymphoid tissues; in contrast, children have abundant class-switched convergent clones in blood. Consistent with serological reports, pre-pandemic children had class-switched convergent clones to SARS-CoV-2, enriched in cross-reactive clones for seasonal coronaviruses, while adults showed few such clones in blood or lymphoid tissues. These results extend age-related and anatomical mapping of human humoral pathogen-specific immunity.One Sentence SummaryChildren have elevated frequencies of pathogen-specific class-switched memory B cells, including SARS-CoV-2-binding clones.

Publisher

Cold Spring Harbor Laboratory

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