Positive and negative selection shape the human naive B cell repertoire
Jeff W. Chen, … , Laurence Menard, Eric Meffre
Jeff W. Chen, … , Laurence Menard, Eric Meffre
Published November 23, 2021
Citation Information: J Clin Invest. 2022;132(2):e150985. https://doi.org/10.1172/JCI150985.
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Research Article Autoimmunity Immunology

Positive and negative selection shape the human naive B cell repertoire

Abstract

Although negative selection of developing B cells in the periphery is well described, yet poorly understood, evidence of naive B cell positive selection remains elusive. Using 2 humanized mouse models, we demonstrate that there was strong skewing of the expressed immunoglobulin repertoire upon transit into the peripheral naive B cell pool. This positive selection of expanded naive B cells in humanized mice resembled that observed in healthy human donors and was independent of autologous thymic tissue. In contrast, negative selection of autoreactive B cells required thymus-derived Tregs and MHC class II–restricted self-antigen presentation by B cells. Indeed, both defective MHC class II expression on B cells of patients with rare bare lymphocyte syndrome and prevention of self-antigen presentation via HLA-DM inhibition in humanized mice resulted in the production of autoreactive naive B cells. These latter observations suggest that Tregs repressed autoreactive naive B cells continuously produced by the bone marrow. Thus, a model emerged, in which both positive and negative selection shaped the human naive B cell repertoire and that each process was mediated by fundamentally different molecular and cellular mechanisms.

Authors

Jeff W. Chen, Jean-Nicolas Schickel, Nikolaos Tsakiris, Joel Sng, Florent Arbogast, Delphine Bouis, Daniele Parisi, Ruchi Gera, Joshua M. Boeckers, Fabien R. Delmotte, Margaret Veselits, Catharina Schuetz, Eva-Maria Jacobsen, Carsten Posovszky, Ansgar S. Schulz, Klaus Schwarz, Marcus R. Clark, Laurence Menard, Eric Meffre

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Figure 3

Tregs are necessary for the establishment of the peripheral B cell tolerance checkpoint.

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Tregs are necessary for the establishment of the peripheral B cell toler...
(A) Schematic diagram depicting the Treg depletion strategy. NSG + thymus humanized mice were i.v. injected with 200 μg mouse anti–human CD25 Abs once a week for 4 weeks before analysis of B cell Ab reactivity. Recombinant Abs cloned from mature naive B cells from NSG (n = 7), NSG + thymus (n = 7), and anti–CD25 Ab–injected NSG + thymus (n = 3) humanized mice were tested by ELISA for (B) anti–HEp-2 cell reactivity and (E) polyreactivity. Reactivity curves are represented as in Figure 1. Frequencies of (C) HEp-2–reactive and (F) polyreactive mature naive B cells. Each symbol represents an individual or a humanized mouse. Solid lines indicate the mean. Frequencies of (D) HEp-2–reactive and (G) polyreactive B cells and their evolution between the new emigrant/transitional and mature naive B cell stages in NSG + thymus humanized mice injected or not with anti-CD25 Abs. ****P < 0.0001, by Kruskal-Wallis test.