Suboptimal B-cell antigen receptor signaling activity in vivo elicits germina 
center counterselection mechanisms

Königsberger, Sebastian; Weis, Vanessa; Prodöhl, Jan; Stehling, Martin; Hobeika, Elias; Reth, M.; Kiefer, Friedemann

doi:DOI: 10.1002/eji.201444538

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Suboptimal B-cell antigen receptor signaling activity in vivo elicits germina center counterselection mechanisms

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Hobeika, Elias
Centre for Biological Signalling (BIOSS), Faculty of Biology, University of Freiburg;
Research Group and Chair of Molecular Immunology of the University of Freiburg, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

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Reth, M.
Centre for Biological Signalling (BIOSS), Faculty of Biology, University of Freiburg;
Research Group and Chair of Molecular Immunology of the University of Freiburg, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

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Zitation

Königsberger, S., Weis, V., Prodöhl, J., Stehling, M., Hobeika, E., Reth, M., et al. (2015). Suboptimal B-cell antigen receptor signaling activity in vivo elicits germina center counterselection mechanisms. European Journal of Immunology, 45, 603-611. doi:DOI: 10.1002/eji.201444538.

Zitierlink: https://hdl.handle.net/someHandle/test/escidoc:902512

Zusammenfassung

Syk and Zap-70 constitute a closely related nonreceptor protein tyrosine kinase family, of which both members are functionally indispensable for conferring their respective antigen receptors with enzymatic activity. In this study, we analyze the impact of altering BCR signaling output on B-cell germinal center (GC) fate selection by constitutive, as well as inducible, monoallelic Syk kinase loss in the presence of a Zap-70 knock-in rescue allele. Cre-mediated Syk deletion in Syk^flox/Zap-70 B cells lowers pErk, but not pAkt-mediated signaling. Surprisingly, the use of a B-cell-specific constitutive mb1-cre deleter mouse model showed that a small cohort of peripheral Syk(flox/Zap-70);mb1-cre B cells efficiently circumvents deletion, which ultimately favors these Syk-sufficient cells to contribute to the GC reaction. Using a developmentally unbiased Syk(flox/Zap-70);mb1-creER(T2) approach in combination with an inducible tdRFP allele, we further demonstrate that this monoallelic deletion escape is not fully explained by leakiness of Cre expression, but is possibly the result of differential Syk locus accessibility in maturing B cells. Altogether, this underscores the importance of proper Syk kinase function not only during central and peripheral selection processes, but also during GC formation and maintenance.