Human T-bet+ B cell development is associated with BTK activity and suppressed by evobrutinib
Liza Rijvers, Jamie van Langelaar, Laurens Bogers, Marie-José Melief, Steven C. Koetzier, Katelijn M. Blok, Annet F. Wierenga-Wolf, Helga E. de Vries, Jasper Rip, Odilia B.J. Corneth, Rudi W. Hendriks, Roland Grenningloh, Ursula Boschert, Joost Smolders, Marvin M. van Luijn
Liza Rijvers, Jamie van Langelaar, Laurens Bogers, Marie-José Melief, Steven C. Koetzier, Katelijn M. Blok, Annet F. Wierenga-Wolf, Helga E. de Vries, Jasper Rip, Odilia B.J. Corneth, Rudi W. Hendriks, Roland Grenningloh, Ursula Boschert, Joost Smolders, Marvin M. van Luijn
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Research Article Immunology

Human T-bet+ B cell development is associated with BTK activity and suppressed by evobrutinib

Abstract

Recent clinical trials have shown promising results for the next-generation Bruton’s tyrosine kinase (BTK) inhibitor evobrutinib in the treatment of multiple sclerosis (MS). BTK has a central role in signaling pathways that govern the development of B cells. Whether and how BTK activity shapes B cells as key drivers of MS is currently unclear. Compared with levels of BTK protein, we found higher levels of phospho-BTK in ex vivo blood memory B cells from patients with relapsing-remitting MS and secondary progressive MS compared with controls. In these MS groups, BTK activity was induced to a lesser extent after anti-IgM stimulation. BTK positively correlated with CXCR3 expression, both of which were increased in blood B cells from clinical responders to natalizumab (anti–VLA-4 antibody) treatment. Under in vitro T follicular helper–like conditions, BTK phosphorylation was enhanced by T-bet–inducing stimuli, IFN-γ and CpG-ODN, while the expression of T-bet and T-bet–associated molecules CXCR3, CD21, and CD11c was affected by evobrutinib. Furthermore, evobrutinib interfered with in vitro class switching, as well as memory recall responses, and disturbed CXCL10-mediated migration of CXCR3+ switched B cells through human brain endothelial monolayers. These findings demonstrate a functional link between BTK activity and disease-relevant B cells and offer valuable insights into how next-generation BTK inhibitors could modulate the clinical course of patients with MS.

Authors

Liza Rijvers, Jamie van Langelaar, Laurens Bogers, Marie-José Melief, Steven C. Koetzier, Katelijn M. Blok, Annet F. Wierenga-Wolf, Helga E. de Vries, Jasper Rip, Odilia B.J. Corneth, Rudi W. Hendriks, Roland Grenningloh, Ursula Boschert, Joost Smolders, Marvin M. van Luijn

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Figure 3

BTK activity is associated with IFN-γ– and CpG-mediated T-bet induction in human B cells.

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BTK activity is associated with IFN-γ– and CpG-mediated T-bet induction ...
(A) Representative histograms of phospho-BTK expression in healthy blood-derived B cells stimulated with IL-21+CD40L, IL-21+CD40L+IFN-γ, and IL-21+CD40L+IFN-γ+CpG for 10 minutes. (B) Donor-specific phospho-BTK induction in blood B cells under the same conditions for 5, 10, 20, and 40 minutes (n = 6). The blue arrows indicate time points at which phospho-BTK is upregulated by IFN-γ with and without CpG. These FACS data were collected in 4 independent experiments, with 1–2 donors per experiment. (C) Correlation between phospho-BTK and T-bet levels in B cells under IL-21/CD40L/IFN-γ–inducing conditions with and without CpG for 48 hours. (D) The effect of evobrutinib (Evo) on IFN-γ– and CpG-induced T-bet expression in B cells (48 hours). These data were collected in 3 independent experiments, with 2 –3 donors per experiment. (C) Spearman’s correlation and (D) repeated measures 1-way ANOVA with Fisher’s least significant difference post hoc test was performed. *P < 0.05, **P < 0.01, ****P < 0.0001.