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. 2022 Oct;52(10):1630-1639.
doi: 10.1002/eji.202250013. Epub 2022 Aug 16.

Improving naive B cell isolation by absence of CD45RB glycosylation and CD27 expression in combination with BCR isotype

Jana Koers  1 Sabrina Pollastro  1 Simon Tol  2 Ilse T G Niewold  3 Pauline A van Schouwenburg  4 Niek de Vries  3 Theo Rispens  1
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Free article

Improving naive B cell isolation by absence of CD45RB glycosylation and CD27 expression in combination with BCR isotype

Jana Koers et al. Eur J Immunol. 2022 Oct.
Free article

Abstract

In past years ex vivo and in vivo experimental approaches involving human naive B cells have proven fundamental for elucidation of mechanisms promoting B cell differentiation in both health and disease. For such studies, it is paramount that isolation strategies yield a population of bona fide naive B cells, i.e., B cells that are phenotypically and functionally naive, clonally non-expanded, and have non-mutated BCR variable regions. In this study different combinations of common as well as recently identified B cell markers were compared to isolate naive B cells from human peripheral blood. High-throughput BCR sequencing was performed to analyze levels of somatic hypermutation and clonal expansion. Additionally, contamination from mature mutated B cells intrinsic to each cell-sorting strategy was evaluated and how this impacts the purity of obtained populations. Our results show that current naive B cell isolation strategies harbor contamination from non-naive B cells, and use of CD27-IgD+ is adequate but can be improved by including markers for CD45RB glycosylation and IgM. The finetuning of naive B cell classification provided herein will harmonize research lines using naive B cells, and will improve B cell profiling during health and disease, e.g. during diagnosis, treatment, and vaccination strategies.

Keywords: B cell receptor; CD27; CD45RB glycosylation; Naive B cells; somatic hypermutation.

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