Kindlin-3 maintains marginal zone B cells but confines follicular B cell 
activation and differentiation

Harzschel, Andrea; Li, Lixia; Krenn, Peter; Szenes-Nagy, Eva; Andrieux, Geoffroy; Bayer, Elisabeth; Pfeifer, Dietmar; Polcik, Laura; Denk, Ursula; Hopner, Jan P.; Karabatak, Elif; Danner, Danielle-Justine; Tangermann, Simone; Kenner, Lukas; Jumaa, Hassan; Greil, Richard; Borries, Melanie; Ruppert, Raphael; Maity, Palash C.; Hartmann, Tanja Nicole

doi:10.1002/JLB.1HI0621-313R

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Kindlin-3 maintains marginal zone B cells but confines follicular B cell activation and differentiation

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Krenn, Peter
Fässler, Reinhard / Molecular Medicine, Max Planck Institute of Biochemistry, Max Planck Society;

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Ruppert, Raphael
Fässler, Reinhard / Molecular Medicine, Max Planck Institute of Biochemistry, Max Planck Society;

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J Leukocyte Bio - 2021 - H rzschel - Kindlin‐3 maintains marginal zone B cells but confines follicular B cell activation.pdf
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Citation

Harzschel, A., Li, L., Krenn, P., Szenes-Nagy, E., Andrieux, G., Bayer, E., et al. (2021). Kindlin-3 maintains marginal zone B cells but confines follicular B cell activation and differentiation. Journal of Leukocyte Biology, 1-14. doi:10.1002/JLB.1HI0621-313R.

Cite as: https://hdl.handle.net/21.11116/0000-000A-11AF-E

Abstract

Integrin-mediated interactions between hematopoietic cells and their microenvironment are important for the development and function of immune cells. Here, the role of the integrin adaptor Kindlin-3 in B cell homeostasis is studied. Comparing the individual steps of B cell development in B cell-specific Kindlin-3 or alpha4 integrin knockout mice, we found in both conditions a phenotype of reduced late immature, mature, and recirculating B cells in the bone marrow. In the spleen, constitutive B cell-specific Kindlin-3 knockout caused a loss of marginal zone B cells and an unexpected expansion of follicular B cells. Alpha4 integrin deficiency did not induce this phenotype. In Kindlin-3 knockout B cells VLA-4 as well as LFA-1-mediated adhesion was abrogated, and short-term homing of these cells in vivo was redirected to the spleen. Upon inducible Kindlin-3 knockout, marginal zone B cells were lost due to defective retention within 2 weeks, while follicular B cell numbers were unaltered. Kindlin-3 deficient follicular B cells displayed higher IgD, CD40, CD44, CXCR5, and EBI2 levels, and elevated PI3K signaling upon CXCR5 stimulation. They also showed transcriptional signatures of spontaneous follicular B cell activation. This activation manifested in scattered germinal centers in situ, early plasmablasts differentiation, and signs of IgG class switch.