Immune tolerance against infused FVIII in hemophilia A is mediated by PD-L1+ Tregs
Janine Becker-Gotot, … , Johannes Oldenburg, Christian Kurts
Janine Becker-Gotot, … , Johannes Oldenburg, Christian Kurts
Published September 15, 2022
Citation Information: J Clin Invest. 2022;132(22):e159925. https://doi.org/10.1172/JCI159925.
View: Text | PDF
Research Article Hematology Immunology

Immune tolerance against infused FVIII in hemophilia A is mediated by PD-L1+ Tregs

Abstract

A major complication of hemophilia A therapy is the development of alloantibodies (inhibitors) that neutralize intravenously administered coagulation factor VIII (FVIII). Immune tolerance induction therapy (ITI) by repetitive FVIII injection can eradicate inhibitors, and thereby reduce morbidity and treatment costs. However, ITI success is difficult to predict and the underlying immunological mechanisms are unknown. Here, we demonstrated that immune tolerance against FVIII under nonhemophilic conditions was maintained by programmed death (PD) ligand 1–expressing (PD-L1–expressing) regulatory T cells (Tregs) that ligated PD-1 on FVIII-specific B cells, causing them to undergo apoptosis. FVIII-deficient mice injected with FVIII lacked such Tregs and developed inhibitors. Using an ITI mouse model, we found that repetitive FVIII injection induced FVIII-specific PD-L1+ Tregs and reengaged removal of inhibitor-forming B cells. We also demonstrated the existence of FVIII-specific Tregs in humans and showed that such Tregs upregulated PD-L1 in patients with hemophilia after successful ITI. Simultaneously, FVIII-specific B cells upregulated PD-1 and became killable by Tregs. In summary, we showed that PD-1–mediated B cell tolerance against FVIII operated in healthy individuals and in patients with hemophilia A without inhibitors, and that ITI reengaged this mechanism. These findings may impact monitoring of ITI success and treatment of patients with hemophilia A.

Authors

Janine Becker-Gotot, Mirjam Meissner, Vadim Kotov, Blanca Jurado-Mestre, Andrea Maione, Andreas Pannek, Thilo Albert, Chrystel Flores, Frank A. Schildberg, Paul A. Gleeson, Birgit M. Reipert, Johannes Oldenburg, Christian Kurts

×

Figure 6

High-dose FVIII induces immune tolerance via PD-1 and Tregs in mice with existing inhibitors.

Options: View larger image (or click on image) Download as PowerPoint
High-dose FVIII induces immune tolerance via PD-1 and Tregs in mice with...
(A) Experimental scheme for inhibitor induction prior to ITI. HemA mice were challenged 2 times at a weekly interval with 2 IU rhFVIII per mouse. FVIII-specific IgG titer was determined on day 14 and mice were distributed into the groups to achieve a comparable pretreatment status. Subsequently, HemA mice were immunized again with 2 IU/mouse of rhFVIII therapeutically once a week (red, n = 5) or according to the ITI protocol twice a week with 2 IU (blue triangle, n = 5) or 4 IU (light blue circle, n = 4) per mouse. (B) Ex vivo quantification of the number of FVIII-specific B cells in the spleen 22 days after start of ITI by flow cytometry. (C) Percentage of PD-1+ FVIII-specific B cells and (D) the MFI of PD-1 on FVIII-specific B cells analyzed ex vivo. (E) Early apoptotic cells are presented as percentage of annexin V+ and Hoechst FVIII-specific B cells after in vitro restimulation with 0.25 μg rhFVIII overnight. (F) Percentage of residual active FVIII in the plasma of HemA mice on day 22. *P < 0.05; **P < 0.01 by 1-way ANOVA with Bonferroni’s post hoc test. NS, not significant.