Your search keyword '"Factor VIII immunology"' showing total 3,494 results

1. Evaluating clinically translatable conditioning for platelet gene therapy in murine hemophilia A with inhibitors.

Author

Chen Y, Li J, Schroeder JA, Jing W, and Shi Q

Subjects

Animals, Mice, Humans, Hematopoietic Stem Cell Transplantation, Vidarabine analogs & derivatives, Vidarabine pharmacology, Transplantation Conditioning methods, Disease Models, Animal, Lentivirus genetics, Mice, Inbred C57BL, Hemophilia A blood, Hemophilia A genetics, Hemophilia A therapy, Genetic Therapy methods, Blood Platelets metabolism, Blood Platelets drug effects, Busulfan pharmacology, Factor VIII genetics, Factor VIII immunology

Abstract

Background: Platelet gene therapy is effective in hemophilia A (HA) mice even with inhibitors. Fludarabine (Flu), along with busulfan (Bu) or melphalan (Mel), preconditioning has been shown to be highly effective for hematopoietic stem cell transplantation in the clinic., Objectives: To evaluate the efficacy of Bu-Flu and Mel-Flu preconditioning in platelet gene therapy of HA with inhibitors., Methods: Bu-Flu and Mel-Flu were used to condition HA mice preimmunized with recombinant human factor (F)VIII. An optimal 660 centigray total body irradiation was used as a control regimen in parallel. Platelet-FVIII expression was introduced by transplantation of 2bF8 lentivirus (LV)-transduced hematopoietic stem cells. Animals were analyzed by fluorescence-activated cell sorting, quantitative polymerase chain reaction, FVIII assays, and tail bleeding tests., Results: Bu-Flu, but not Mel-Flu, enabled successful 2bF8 gene therapy. All recipients achieved >55% chimerism post hematopoietic stem cell transplantation in both Bu-Flu and 660 centigray groups, with comparable copy numbers of 2bF8 cassette and the platelet-FVIII levels. The bleeding phenotype was rescued in 2bF8LV-transduced recipients. FVIII inhibitor titers declined with time, with comparable disappearance time of inhibitors between the 2 groups. When animals were rechallenged with recombinant human FVIII after the titers dropped to undetectable levels, no inhibitors were detected in 2bF8LV-transduced recipients. In contrast, all untransduced transplanted control mice produced inhibitors. These data demonstrate that immune tolerance was established in 2bF8LV-transduced primed HA mice under Bu-Flu conditioning., Conclusion: Bu-Flu preconditioning allows for successfully introducing platelet-FVIII expression to restore hemostasis and induce immune tolerance in primed HA mice, suggesting that this approach is a promising clinically translatable strategy for gene therapy of HA with inhibitors., Competing Interests: Declaration of competing interests There are no competing interests to disclose., (Copyright © 2024 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2024

2. Blunting specific T-dependent antibody responses with engineered "decoy" B cells.

Author

Pitner RA, Chao JL, Dahl NP, Fan MN, Cai X, Avery NG, Roe K, Spiegel PC Jr, Miao CH, Gerner MY, James RG, and Rawlings DJ

Subjects

Animals, Mice, T-Lymphocytes immunology, T-Lymphocytes metabolism, Factor VIII immunology, Factor VIII genetics, CRISPR-Cas Systems, Immunoglobulin G immunology, Adoptive Transfer, Humans, Germinal Center immunology, Germinal Center metabolism, B-Lymphocytes immunology, B-Lymphocytes metabolism, Mice, Knockout, Antibody Formation immunology, Positive Regulatory Domain I-Binding Factor 1 genetics, Positive Regulatory Domain I-Binding Factor 1 metabolism, Positive Regulatory Domain I-Binding Factor 1 immunology

Abstract

Antibody inhibitors pose an ongoing challenge to the treatment of subjects with inherited protein deficiency disorders, limiting the efficacy of both protein replacement therapy and corrective gene therapy. Beyond their central role as producers of serum antibody, B cells also exhibit many unique properties that could be exploited in cell therapy applications, notably including antigen-specific recognition and the linked capacity for antigen presentation. Here we employed CRISPR-Cas9 to demonstrate that ex vivo antigen-primed Blimp1-knockout "decoy" B cells, incapable of differentiation into plasma cells, participated in and downregulated host antigen-specific humoral responses after adoptive transfer. Following ex vivo antigen pulse, adoptively transferred high-affinity antigen-specific decoy B cells were diverted into germinal centers en masse, thereby reducing participation by endogenous antigen-specific B cells in T-dependent humoral responses and suppressing both cognate and linked antigen-specific immunoglobulin (Ig)G following immunization with conjugated antigen. This effect was dose-dependent and, importantly, did not impact concurrent unrelated antibody responses. We demonstrated the therapeutic potential of this approach by treating factor VIII (FVIII)-knockout mice with antigen-pulsed decoy B cells prior to immunization with an FVIII conjugate protein, thereby blunting the production of serum FVIII-specific IgG by an order of magnitude as well as reducing the proportion of animals exhibiting functional FVIII inhibition by 6-fold., Competing Interests: Declaration of interests R.A.P., R.G.J., and D.J.R. are credited as inventors on a provisional patent application (Application No. 63/584,432) filed by Seattle Children’s Research Institute with the United States Patent and Trademark Office regarding the materials described in this article. This patent application covers aspects of the synthesis, characterization, and applications of the materials discussed herein. C.H.M. is a member of the Editorial Board for Molecular Therapy., (Copyright © 2024 The American Society of Gene and Cell Therapy. Published by Elsevier Inc. All rights reserved.)

Published

2024

3. Efficacy and safety of recombinant porcine factor VIII in Japanese patients with acquired hemophilia A.

Author

Seki Y, Ogawa Y, Kikuchi T, Sakaida E, Mizuta Y, Kitagawa T, Takemura K, Miyaguchi Y, Nogami K, and Matsushita T

Subjects

Humans, Middle Aged, Aged, Swine, Animals, Japan, Male, Aged, 80 and over, Treatment Outcome, Female, Hemorrhage etiology, East Asian People, Hemophilia A drug therapy, Hemophilia A immunology, Factor VIII immunology, Factor VIII adverse effects, Factor VIII therapeutic use, Factor VIII administration & dosage, Recombinant Proteins therapeutic use, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects

Abstract

Acquired hemophilia A (AHA) is a rare bleeding disorder caused by autoantibodies inhibiting human factor VIII (hFVIII). This phase II/III open-label study evaluated the safety and efficacy of recombinant porcine factor VIII (rpFVIII, susoctocog alfa) in adults with AHA and severe bleeding episodes in Japan (NCT04580407). The initial rpFVIII dose was 200 U/kg, with subsequent doses based on clinical measures including plasma FVIII activity. The primary efficacy endpoint was the proportion of severe bleeding episodes with a positive response to rpFVIII therapy 24 h after treatment initiation. Five patients were eligible for, and completed, rpFVIII treatment (age group: 60s-80s; median hFVIII inhibitor: 52 BU/mL; porcine FVIII [pFVIII] inhibitor: 3/5 patients). The median (range) total dose/patient was 548.4 (198-1803) U/kg with a median 3.0 infusions/patient. All patients responded positively to rpFVIII therapy at 24 h regardless of baseline pFVIII inhibitor status. rpFVIII treatment was well tolerated with no adverse events of special interest such as thromboembolic events or de novo pFVIII inhibitors. This study supports the use of rpFVIII as a novel therapy in the clinical management of patients with AHA in Japan. rpFVIII was approved for treating bleeding episodes in adults with AHA in Japan in 2024., (© 2024. Takeda Pharmaceutical Company Limited.)

Published

2024

4. Emicizumab versus immunosuppressive therapy for the management of acquired hemophilia A.

Author

Hart C, Klamroth R, Sachs UJ, Greil R, Knoebl P, Oldenburg J, Miesbach W, Pfrepper C, Trautmann-Grill K, Pekrul I, Holstein K, Eichler H, Weigt C, Schipp D, Werwitzke S, and Tiede A

Subjects

Humans, Aged, Male, Female, Treatment Outcome, Aged, 80 and over, Middle Aged, Time Factors, Propensity Score, Hemophilia A drug therapy, Hemophilia A blood, Hemophilia A immunology, Hemophilia A diagnosis, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized adverse effects, Antibodies, Bispecific therapeutic use, Antibodies, Bispecific adverse effects, Immunosuppressive Agents therapeutic use, Immunosuppressive Agents adverse effects, Hemorrhage chemically induced, Factor VIII immunology

Abstract

Background: Acquired hemophilia A (AHA) is an autoimmune bleeding disorder caused by neutralizing antibodies against coagulation factor VIII. Immunosuppressive therapy (IST) is standard of care to eradicate autoantibody production and protect from further bleeding but carries a risk of severe infection and mortality in frail patients with AHA. Recently, emicizumab has been studied for its potential to reduce the need for early and aggressive IST., Objectives: To compare outcomes of 2 studies that used either IST (GTH-AH 01/2010; N = 101) or prophylaxis with emicizumab (GTH-AHA-EMI; N = 47) early after diagnosis of AHA., Methods: Baseline characteristics were balanced by propensity score matching. Primary endpoint was the rate of clinically relevant new bleeds during the first 12 weeks; secondary endpoints were adverse events and overall survival., Results: The negative binominal model-based bleeding rate was 68% lower with emicizumab as compared with IST (incident rate ratio, 0.325; 95% CI, 0.182-0.581). No difference was apparent in the overall frequency of infections (emicizumab 21%, IST 29%) during the first 12 weeks, but infections were less often fatal in emicizumab-treated patients (0%) compared with IST-treated patients (11%). Thromboembolic events occurred less often with emicizumab (2%) than with IST (7%). Overall survival after 24 weeks was better with emicizumab (90% vs 76%; hazard ratio, 0.44; 95%, CI, 0.24-0.81)., Conclusion: Using emicizumab instead of IST in the early phase after initial diagnosis of AHA reduced bleeding and fatal infections and improved overall survival., Competing Interests: Declaration of competing interests C.H. reports honoraria for lectures or consultancy from Bayer, BMS, SOBI, Daiichi Sankyo, Roche/Chugai, Pfizer, Sanofi, and Takeda. R.K. reports institutional grants for research and studies from Bayer, CSL Behring, Novo Nordisk, Octapharma, and SOBI, and honoraria for lectures or consultancy from Bayer, Biotest, BioMarin, CSL Behring, Grifols, LFB, Novo Nordisk, Octapharma, Pfizer, Roche/Chugai, Sanofi, SOBI, and Takeda. U.J.S. reports institutional grants for research and studies from Octapharma and honoraria for lectures or consultancy from Bayer, SOBI, CSL Behring, and Pfizer. R.G. reports institutional grants for research and studies from Celgene, Roche, Merck, Takeda, AstraZeneca, Novartis, Amgen, BMS, MSD, Sandoz, Abbvie, Gilead, and Daiichi Sankyo, and honoraria for lectures or consultancy from Celgene, Roche, Merck, Takeda, AstraZeneca, Novartis, Amgen, BMS, MSD, Sandoz, Abbvie, Gilead, Daiichi Sankyo, and Sanofi. P.K. reports institutional grants for research and studies from Ablynx/Sanofi, Novo Nordisk, Roche, and Takeda, and honoraria for lectures or consultancy from Ablynx/Sanofi, Alexion, Biotest, CSL Behring, Novo Nordisk, Roche, Takeda, and Technoclone. J.O. reports institutional grants for research and studies from Bayer, Biotest, CSL Behring, Octapharma, Pfizer, SOBI, and Takeda, and honoraria for lectures or consultancy from Bayer, Biogen Idec, BioMarin, Biotest, CSL Behring, Chugai, Freeline, Grifols, Novo Nordisk, Octapharma, Pfizer, Roche, Sparks, SOBI, and Takeda. W.M. reports institutional grants for research and studies from Bayer, Biotest, CSL Behring, LFB, Novo Nordisk, Octapharma, Pfizer, and Takeda/Shire, and honoraria for lectures or consultancy from Bayer, BioMarin, Biotest, CSL Behring, Chugai, Freeline, LFB, Novo Nordisk, Octapharma, Pfizer, Regeneron, Roche, Sanofi, Takeda/Shire, and uniQure. C.P. reports institutional grants for research and studies from Chugai/Roche, Takeda, Zacros, and LeoPharma, and honoraria for lectures or consultancy from Bayer, BioMarin, Chugai/Roche, CSL Behring, Novo Nordisk, Pfizer, BMS, SOBI, and Takeda. K.T.G. reports honoraria for lectures or consultancy from Takeda, Roche, Grifols, and SOBI. I.P. reports institutional grants for research and studies from Takeda and honoraria for lectures or consultancy from BMS and Novo Nordisk. K.H. reports institutional grants for research and studies from Bayer, CSL Behring, Novo Nordisk, Pfizer, and SOBI, and honoraria for lectures or consultancy from Bayer, Biotest, Chugai, CSL Behring, LFB, Novo Nordisk, Pfizer, Roche, SOBI, and Takeda. H.E. reports institutional grants for research and studies from Bayer Vital and CSL Behring and honoraria for lectures or consultancy from Bayer Vital, BioMarin, CSL Behring, Novo Nordisk, Pfizer, Roche, and SOBI. C.W. has nothing to disclose. D.S. has nothing to disclose. S.W. reports institutional grants for research and studies from Biotest and Octapharma, and honoraria for lectures or consultancy from Biotest and Stago. A.T. reports institutional grants for research and studies from Bayer, Biotest, Chugai, Novo Nordisk, Octapharma, Pfizer, Roche, SOBI, and Takeda, and honoraria for lectures or consultancy from Bayer, BioMarin, Biotest, Chugai, CSL Behring, Novo Nordisk, Octapharma, Pfizer, Roche, SOBI, and Takeda., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

5. Large deletions and small insertions and deletions in the factor VIII gene predict unfavorable immune tolerance induction outcome in people with severe hemophilia A and high-responding inhibitors.

Author

Zuccherato LW, Souza RP, Camelo RM, Dias MM, Jardim LL, Santana MAP, Oliveira AG, Lorenzato CS, Cerqueira MH, Franco VKB, Ribeiro RA, Etto LY, Roberti MDRF, Callado FMA, de Cerqueira MAF, Pinto ISS, Garcia AA, Anegawa TH, Neves DCF, Tan DM, Tou RP, Chaves DG, van der Bom J, and Rezende SM

Subjects

Humans, Male, Child, Child, Preschool, Adult, Adolescent, Female, Young Adult, Isoantibodies immunology, Isoantibodies blood, INDEL Mutation, Hemophilia A genetics, Hemophilia A immunology, Hemophilia A drug therapy, Factor VIII immunology, Factor VIII genetics, Factor VIII therapeutic use, Immune Tolerance genetics

Abstract

Introduction: Hemophilia A is an inherited bleeding disorder caused by pathogenic variants in the factor VIII gene (F8), which leads to factor VIII (FVIII) deficiency. Immune tolerance induction (ITI) is a therapeutic approach to eradicate alloantibodies (inhibitors) against exogenous FVIII in people with inherited hemophilia A. Few studies have evaluated the role of F8 variants on ITI outcome., Material and Methods: We included people with severe hemophilia A (FVIII ˂ 1 international units/dL) and high-responding inhibitors (≥ 5 Bethesda units/mL lifelong) who underwent a first course of ITI. Socio-demographic, clinical and laboratory data were collected. ITI outcomes were defined as total, partial successes, and failure. Detection of intron 1 and 22 inversions was performed by polymerase-chain reaction, followed by F8 sequencing., Results: We included 168 people with inherited hemophilia A and high-responding inhibitors, median age 6 years at ITI start. Intron 22 inversion was the most prevalent variant (53.6 %), followed by nonsense (16.1 %), small insertion/deletion (11.3 %), and large deletion (10.7 %). In comparison with intron 22 inversion, the odds of ITI failure were 15.5 times higher (odds ratio [OR] 15.50; 95 % confidence interval [95 % CI] 4.59-71.30) and 4.25 times higher (95 % CI, 1.53-12.3) among carriers of F8 large deletions and small insertions and deletions, respectively., Conclusion: F8 large deletions and small insertions/deletions predicted ITI failure after a first course of ITI in patients with severe hemophilia A and high-responding inhibitors. This is the first study to show F8 large deletions and small insertions/deletions as predictors of ITI failure., Competing Interests: Declaration of competing interest RMC received speaker fees from Bayer, NovoNordisk, Hoffman-La Roche, and Takeda, consultancy fees from Hoffman-La Roche and Takeda, and sponsorship to attend scientific event grants from Bayer, NovoNordisk, Hoffman-La Roche, and Takeda. AGO received speaker fees and scientific event grants from NovoNordisk and Takeda. MRFR received speaker fees from NovoNordisk, scientific event grants from Hoffman-La Roche, Takeda and NovoNordisk, and consultancy fees from the Brazilian Ministry of Health. FMRAC received sponsorship to attend scientific event grants from Hoffman-La Roche and NovoNordisk. LYE received scientific event grants from Hoffman-La Roche. MAFC received sponsorship to attend scientific event grants from Hoffman-La Roche and NovoNordisk. ISSP received speaker fees from Hoffman-La Roche, NovoNordisk and Takeda, sponsorship to attend scientific event grants from Hoffman-La Roche, Takeda and NovoNordisk, consultancy fees from the Hoffman-La Roche, NovoNordisk, Bayer and Biomarin, and grants for scientific publication from Takeda. AAG received speaker fees from Takeda and NovoNordisk, sponsorship to attend scientific event grants from Takeda and NovoNordisk, and consultancy fees from NovoNordisk. THA received sponsorship to attend scientific event grants from Hoffman-La Roche and Takeda. DCFN received sponsorship to attend scientific event grants from Takeda. LWZ, RPS, MMD, MAPS, LLJ, RAR, MHC, CSL, DMT, VKBF, RPT, DGC, JVDB and SMR declare they have no competing interests which might be perceived as posing as a conflict., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

6. Acid Treatment of FVIII-Containing Plasma Samples Unmasks a Broad Spectrum of FVIII-Specific Antibodies in ELISA.

Author

Schmidt A, Stichel D, Salzmann-Manrique E, and Königs C

Subjects

Humans, Antibodies blood, Factor VIII immunology, Factor VIII therapeutic use, Hemophilia A blood, Hemophilia A drug therapy, Enzyme-Linked Immunosorbent Assay methods

Abstract

During routine treatment, plasma samples of patients with hemophilia A or acquired hemophilia A are frequently analyzed for the presence of FVIII-specific antibodies. While only inhibitory antibodies can be detected by the Bethesda assay, inhibitory and non-inhibitory antibodies can be detected by ELISA. However, plasma samples of patients frequently contain endogenous or substituted FVIII, hence interfering with both types of analyses. One option for the inactivation of FVIII is heat denaturation, which unfortunately has been shown to lead to high background signals complicating the discrimination of negative and positive plasma samples. In the current study, we developed a method of acid denaturation for FVIII-containing plasma samples that can help identify samples containing FVIII-specific antibodies and compared the effects of heat and acid denaturation on the detection of FVIII-antibody interactions in a monoclonal setting. The aim of our study was to establish an analysis that allows safer treatment decisions in the context of tolerance to FVIII., Competing Interests: None declared., (Thieme. All rights reserved.)

Published

2024

7. Anti-mCD20 in combination with α-mCXCL13 monoclonal antibody inhibits anti-FVIII antibody development in hemophilia A mice.

Author

Zheng Q, Lin K, Zhang N, Shi Q, Wu Y, and Chen Y

Subjects

Animals, Mice, Humans, Antigens, CD20 immunology, Disease Models, Animal, Mice, Inbred C57BL, Male, Hemophilia A drug therapy, Hemophilia A immunology, Factor VIII immunology, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal pharmacology, Antibodies, Monoclonal immunology, Chemokine CXCL13 immunology, Chemokine CXCL13 metabolism

Abstract

Anti-factor VIII (FVIII) antibody development poses a significant challenge in hemophilia A (HA) patients receiving FVIII protein replacement therapy. There is an urgent need for novel therapeutic strategies to inhibit the production of anti-FVIII inhibitory antibodies (inhibitors) in HA. This study aimed to investigate a combination monoclonal antibody (mAb) therapy targeting CXCL13 and CD20 on the development of anti-FVIII antibodies in a HA murine model, along with the underlying mechanisms involved. Specifically, mAbs targeting mouse CD20 (18B12) with an IgG2a backbone and mouse CXCL13 (2C4) with an IgG1 backbone were synthesized. HA mice with FVIII inhibitors were established, and the results revealed that the combination therapy of anti-mCD20 with α-mCXCL13 significantly suppressed anti-FVIII antibody development and induced FVIII tolerance. Furthermore, this combination therapy led to a marked reduction of peripheral and splenic follicular helper T cells and an enhancement of regulatory T cell induction, along with sustained depletion of bone marrow and splenic plasma cells in HA mice with preexisting FVIII immunity. Thus, the concurrence of blockage of CD20 and neutralization of CXCL13 hold promise as a therapeutic strategy for HA patients with inhibitors., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

8. Pathogenic but sweet: factor VIII inhibitor hits the hot spot.

Author

Kolyadko VN

Subjects

Humans, Blood Coagulation drug effects, Animals, Blood Coagulation Factor Inhibitors blood, Blood Coagulation Factor Inhibitors immunology, Factor VIII immunology, Factor VIII antagonists & inhibitors, Hemophilia A drug therapy, Hemophilia A blood, Hemophilia A immunology

Abstract

Competing Interests: Declaration of competing interests The author declares no competing interests.

Published

2024

9. Marginal Zone B Cells Represent a Conserved Initiating Player in the Immune Response to Factor VIII in Hemophilia A Mice.

Author

Maarouf M, Patel SR, Baldwin WH, Zerra PE, Cox C, Parker ET, Stowell SR, and Meeks SL

Subjects

Animals, Mice, Mice, Knockout, Mice, Inbred C57BL, Hemophilia A immunology, Hemophilia A blood, Factor VIII immunology, Factor VIII metabolism, B-Lymphocytes immunology, Disease Models, Animal

Abstract

Competing Interests: S.L.M. has served as a paid consultant or advisory board member for Bayer, Takeda, Biomarin, Sanofi, CSL Behring, Genentech, NovoNordisk, Octapharma, Pfizer, Sangamo, Spark/Roche, Sobi, and receives research support from Octapharma and Genentech. S.R.S. has consulted for Novartis, Cellics, Argenx, and Alexion, and has received speaking honoraria from Grifols and research support from Alexion. S.R.P., W.H.B., P.Z., E.T.P., and C.C. declare no conflict of interests.

Published

2024

10. Structural basis for inhibition of coagulation factor VIII reveals a shared antigenic hotspot on the C1 domain.

Author

Childers KC, Cowper B, Vaughan JD, McGill JR, Davulcu O, Lollar P, Doering CB, Coxon CH, and Spiegel PC Jr

Subjects

Humans, Animals, Protein Domains, von Willebrand Factor metabolism, von Willebrand Factor chemistry, Cryoelectron Microscopy, Models, Molecular, Structure-Activity Relationship, Mice, Binding Sites, Protein Conformation, Blood Coagulation, Factor VIII immunology, Factor VIII chemistry, Factor VIII metabolism, Hemophilia A immunology, Hemophilia A drug therapy, Epitopes chemistry, Protein Binding

Abstract

Background: Hemophilia A arises from dysfunctional or deficient coagulation factor (F)VIII and leads to inefficient fibrin clot formation and uncontrolled bleeding events. The development of antibody inhibitors is a clinical complication in hemophilia A patients receiving FVIII replacement therapy. LE2E9 is an anti-C1 domain inhibitor previously isolated from a mild/moderate hemophilia A patient and disrupts FVIII interactions with von Willebrand factor and FIXa, though the intermolecular contacts that underpin LE2E9-mediated FVIII neutralization are undefined., Objectives: To determine the structure of the complex between FVIII and LE2E9 and characterize its mechanism of inhibition., Methods: FVIII was bound to the antigen binding fragment (Fab) of NB2E9, a recombinant construct of LE2E9, and its structure was determined by cryogenic electron microscopy., Results: This report communicates the 3.46 Å structure of FVIII bound to NB2E9, with its epitope comprising FVIII residues S2040 to Y2043, K2065 to W2070, and R2150 to H2155. Structural analysis reveals that the LE2E9 epitope overlaps with portions of the epitope for 2A9, a murine-derived inhibitor, suggesting that these residues represent a shared antigenic region on the C1 domain between FVIII -/- mice and hemophilia A patients. Furthermore, the FVIII:NB2E9 structure elucidates the orientation of the LE2E9 glycan, illustrating how the glycan sterically blocks interactions between the FVIII C1 domain and the von Willebrand factor D' domain. A putative model of the FVIIIa:FIXa complex suggests potential clashing between the NB2E9 glycan and FIXa light chain., Conclusion: These results describe an antigenic "hotspot" on the FVIII C1 domain and provide a structural basis for engineering FVIII replacement therapeutics with reduced antigenicity., Competing Interests: Declaration of competing interests P.L. is listed as an inventor on a patent application describing ET3i and on patents owned by Emory University claiming compositions of matter that include modified FVIII proteins with reduced reactivity with anti-FVIII antibodies. C.B.D. and P.L. are cofounders of Expression Therapeutics and own equity in the company. Expression Therapeutics owns the intellectual property associated with ET3i. The terms of this arrangement have been reviewed and approved by Emory University in accordance with its conflict-of-interest policies. The remaining authors have no competing interests to disclose., (Copyright © 2024 International Society on Thrombosis and Haemostasis. All rights reserved.)

Published

2024

11. The use of Bacillus subtilis as a cost-effective expression system for production of Cholera Toxin B fused factor VIII epitope regions applicable for inducing oral immune tolerance.

Author

Vijayakumar VE, Vijayalakshmi MA, Lacroix-Desmazes S, and Venkataraman K

Subjects

Humans, Gene Expression, Administration, Oral, Bacillus subtilis genetics, Bacillus subtilis immunology, Bacillus subtilis metabolism, Cholera Toxin genetics, Cholera Toxin immunology, Factor VIII immunology, Factor VIII genetics, Epitopes immunology, Epitopes genetics, Recombinant Fusion Proteins immunology, Recombinant Fusion Proteins genetics, Immune Tolerance

Abstract

Coagulation factor replacement therapy for the X-linked bleeding disorder Haemophilia, characterized by a deficiency of coagulation protein factor VIII (FVIII), is severely complicated by antibody (inhibitors) formation. The development of FVIII inhibitors drastically alters the quality of life of the patients and is associated with a tremendous increase in morbidity as well as treatment costs. The ultimate goal of inhibitor control is antibody elimination. Immune tolerance induction (ITI) is the only clinically established approach for developing antigen-specific tolerance to FVIII. This work aims to establish a novel cost-effective strategy to produce FVIII molecules in fusion with cholera toxin B (CTB) subunit at the N terminus using the Bacillus subtilis expression system for oral tolerance, as the current clinical immune tolerance protocols are expensive. Regions of B-Domain Deleted (BDD)-FVIII that have potential epitopes were identified by employing Bepipred linear epitope prediction; 2 or more epitopes in each domain were combined and cDNA encoding these regions were fused with CTB and cloned in the Bacillus subtilis expression vector pHT43 and expression analysis was carried out. The expressed CTB-fused FVIII epitope domains showed strong binding affinity towards the CTB-receptor GM1 ganglioside. To conclude, Bacillus subtilis expressing FVIII molecules might be a promising candidate for exploring for the induction of oral immune tolerance., (© 2024. Institute of Microbiology, Academy of Sciences of the Czech Republic, v.v.i.)

Published

2024

12. [Acquired hemophilia A and emicizumab for the treatment of bleeding: two case report and a literature review].

Author

Launois A, Martin-Toutain I, Devaux F, Lambert J, Longval T, Merabet F, Jaidi R, Le Dore S, Ferre E, Rousselot P, De Raucourt E, and Flaujac C

Subjects

Humans, Male, Aged, Treatment Outcome, Factor VIII immunology, Factor VIII therapeutic use, Factor VIII antagonists & inhibitors, Middle Aged, Antibodies, Bispecific therapeutic use, Hemophilia A drug therapy, Hemophilia A complications, Hemophilia A diagnosis, Hemophilia A blood, Hemophilia A immunology, Antibodies, Monoclonal, Humanized therapeutic use, Hemorrhage

Abstract

Emicizumab is a bispecific antibody that mimics the function of factor VIII (FVIII) and is indicated for prophylactic use in patients with congenital hemophilia A with or without inhibitors. Acquired hemophilia A (AHA) is a rare and severe disorder causes by autoantibodies that inhibit FVIII. In AHA, acute bleeding are managed with bypassing agents but several reports described the off-label use of emicizumab. The aim of this article is to describe two cases of AHA treated with emicizumab and a review of the scientific littérature. Reports indicate that the use of emicizumab is efficacious to treat acute bleeding with less thrombotic events thant with bypassing agents and with a reduced hospitalisation duration. Nevertheless biological monitoring is more complicated with assay interferences and a persistent circulation more than 6 months after the last injection was observed for our two patients.

Published

2024

13. Efanesoctocog alfa: the renaissance of Factor VIII replacement therapy.

Author

Dargaud Y, Leuci A, Ruiz AR, and Lacroix-Desmazes S

Subjects

Humans, von Willebrand Factor therapeutic use, von Willebrand Factor chemistry, von Willebrand Factor metabolism, Animals, Clinical Trials as Topic, Factor VIII therapeutic use, Factor VIII immunology, Hemophilia A drug therapy

Abstract

Efanesoctocog alfa (Altuviiio,TM Sanofi-SOBI) is a B domain-deleted single-chain Factor VIII (FVIII) connected to D'D3 domain of von Willebrand Factor (vWF). Its ingenious design allows efanesoctocog alfa to operate independently of endogenous vWF and results in an outstanding 3-4 times longer half-life compared to standard and extended half-life (EHL) FVIII products. The prolonged half-life ensures sustained high levels of factor activity, maintaining normal to near-normal ranges for the majority of the week, facilitating the convenience of once-weekly administration. Efanesoctocog alfa received regulatory approval in 2023 for application in both adults and children with inherited hemophilia A in the United States and Japan. Its sanctioned use encompasses both prophylaxis and 'on demand' treatment for bleeding episodes. The European Medicines Agency (EMA) is currently undertaking a comprehensive review of Altuviiio. TM This comprehensive review focuses on the immunological profile of efanesoctocog alfa, a highly sophisticated new class of EHL FVIII molecule. The integration of the vWF D'D3 domain, XTEN polypeptides, and potential regulatory T-cell epitopes within various segments of efanesoctocog alfa collectively serves as a mitigating factor against the development of a neutralizing T-cell-mediated immune response. We hypothesize that such distinctive attribute may significantly reduce the risk of neutralizing antibodies, particularly in previously untreated patients. The discussion extends beyond regulatory approval to encompass the preclinical and clinical development of efanesoctocog alfa, including considerations for laboratory monitoring. The review also highlights areas that warrant further investigation to deepen our understanding of this groundbreaking therapeutic agent.

Published

2024

14. Efanesoctocog Alfa Prophylaxis for Children with Severe Hemophilia A.

Author

Malec L, Peyvandi F, Chan AKC, Königs C, Zulfikar B, Yuan H, Simpson M, Álvarez Román MT, Carcao M, Staber JM, Dunn AL, Chou SC, d'Oiron R, Albisetti M, Demissie M, Santagostino E, Yarramaneni A, Wong N, Abad-Franch L, Gunawardena S, and Fijnvandraat K

Subjects

Child, Child, Preschool, Humans, Infant, Male, Antibodies, Neutralizing blood, Antibodies, Neutralizing immunology, Drug Administration Schedule, Joint Diseases etiology, Quality of Life, Factor VIII administration & dosage, Factor VIII adverse effects, Factor VIII immunology, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemophilia A complications, Hemorrhage etiology, Hemorrhage prevention & control, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects, Recombinant Proteins immunology, Recombinant Proteins therapeutic use

Abstract

Background: Once-weekly efanesoctocog alfa provides high sustained factor VIII activity with superior bleeding prevention as compared with prestudy factor VIII prophylaxis in previously treated patients 12 years of age or older with severe hemophilia A. Data on outcomes of efanesoctocog alfa treatment in children younger than 12 years of age with severe hemophilia A are limited., Methods: We conducted a phase 3, open-label study involving previously treated patients younger than 12 years of age with severe hemophilia A. Patients received prophylaxis with once-weekly efanesoctocog alfa (50 IU per kilogram of body weight) for 52 weeks. The primary end point was the occurrence of factor VIII inhibitors (neutralizing antibodies against factor VIII). Secondary end points included annualized rates of treated bleeding episodes, bleeding treatment, safety, and pharmacokinetics., Results: A total of 74 male patients were enrolled (38 with an age of <6 years and 36 with an age of 6 to <12 years). No factor VIII inhibitors developed. Most adverse events were nonserious. No serious adverse events that were assessed by the investigator as being related to efanesoctocog alfa were reported. In the 73 patients treated according to the protocol, the median and model-based mean annualized bleeding rates were 0.00 (interquartile range, 0.00 to 1.02) and 0.61 (95% confidence interval, 0.42 to 0.90), respectively. A total of 47 patients (64%) had no treated bleeding episodes, 65 (88%) had no spontaneous bleeding episodes, and 61 (82%) had no episodes of bleeding into joints. A total of 41 of 43 bleeding episodes (95%) resolved with one injection of efanesoctocog alfa. Mean factor VIII activity at steady state was more than 40 IU per deciliter for 3 days and more than 10 IU per deciliter for almost 7 days after dose administration. The geometric mean terminal half-life was 40.0 hours., Conclusions: In children with severe hemophilia A, once-weekly prophylaxis with efanesoctocog alfa provided high sustained factor VIII activity in the normal to near-normal range (>40 IU per deciliter) for 3 days and more than 10 IU per deciliter for almost 7 days after administration, leading to effective bleeding prevention. Efanesoctocog alfa was associated with mainly nonserious adverse events. (Funded by Sanofi and Sobi; XTEND-Kids ClinicalTrials.gov number, NCT04759131.)., (Copyright © 2024 Massachusetts Medical Society.)

Published

2024

15. Clinical immunogenicity outcomes from GENEr8-1, a phase 3 study of valoctocogene roxaparvovec, an AAV5-vectored gene therapy for hemophilia A.

Author

Long BR, Robinson TM, Day JRS, Yu H, Lau K, Imtiaz U, Patton KS, de Hart G, Henshaw J, Agarwal S, Vettermann C, Zoog SJ, and Gupta S

Subjects

Humans, Male, Adult, Treatment Outcome, Transgenes, Young Adult, Antibodies, Viral immunology, Antibodies, Viral blood, Middle Aged, Hemophilia A therapy, Hemophilia A immunology, Hemophilia A genetics, Dependovirus genetics, Dependovirus immunology, Genetic Therapy methods, Genetic Vectors genetics, Genetic Vectors administration & dosage, Factor VIII genetics, Factor VIII immunology

Abstract

Gene transfer therapies utilizing adeno-associated virus (AAV) vectors involve a complex drug design with multiple components that may impact immunogenicity. Valoctocogene roxaparvovec is an AAV serotype 5 (AAV5)-vectored gene therapy for the treatment of hemophilia A that encodes a B-domain-deleted human factor VIII (FVIII) protein controlled by a hepatocyte-selective promoter. Following previous results from the first-in-human phase 1/2 clinical trial, we assessed AAV5-capsid- and transgene-derived FVIII-specific immune responses with 2 years of follow-up data from GENEr8-1, a phase 3, single-arm, open-label study in 134 adult men with severe hemophilia A. No FVIII inhibitors were detected following administration of valoctocogene roxaparvovec. Immune responses were predominantly directed toward the AAV5 capsid, with all participants developing durable anti-AAV5 antibodies. Cellular immune responses specific for the AAV5 capsid were detected in most participants by interferon-γ enzyme-linked immunosorbent spot assay 2 weeks following dose administration and declined or reverted to negative over the first 52 weeks. These responses were weakly correlated with alanine aminotransferase elevations and showed no association with changes in FVIII activity. FVIII-specific cellular immune responses were less frequent and more sporadic compared with those specific for AAV5 and showed no association with safety or efficacy parameters., Competing Interests: Declaration of interests All authors are current or former employees and shareholders of BioMarin Pharmaceutical Inc. BioMarin Pharmaceutical Inc. has patents and/or patent applications covering ROCTAVIAN (valoctocogene roxaparvovec) and methods for treating hemophilia A., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

16. Pre-Existing Immunity to a Nucleic Acid Contaminant-Derived Antigen Mediates Transaminitis and Resultant Diminished Transgene Expression in a Mouse Model of Hepatic Recombinant Adeno-Associated Virus-Mediated Gene Transfer.

Author

Brimble MA, Morton CL, Winston SM, Reeves IL, Spence Y, Cheng PH, Zhou J, Nathwani AC, Thomas PG, Souquette A, and Davidoff AM

Subjects

Animals, Mice, Disease Models, Animal, Gene Transfer Techniques, Factor VIII genetics, Factor VIII immunology, Liver metabolism, Liver pathology, Liver immunology, Mice, Inbred BALB C, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes metabolism, Gene Expression, Humans, Hepatitis therapy, Hepatitis immunology, Dependovirus genetics, Dependovirus immunology, Transgenes, Genetic Vectors genetics, Genetic Vectors administration & dosage, Genetic Therapy methods

Abstract

Liver injury with concomitant loss of therapeutic transgene expression can be a clinical sequela of systemic administration of recombinant adeno-associated virus (rAAV) when used for gene therapy, and a significant barrier to treatment efficacy. Despite this, it has been difficult to replicate this phenotype in preclinical models, thereby limiting the field's ability to systematically investigate underlying biological mechanisms and develop interventions. Prior animal models have focused on capsid and transgene-related immunogenicity, but the impact of concurrently present nontransgene or vector antigens on therapeutic efficacy, such as those derived from contaminating nucleic acids within rAAV preps, has yet to be investigated. In this study, using Ad5-CMV&#95;GFP-immunized immunocompetent BALB/cJ mice, and a coagulation factor VIII expressing rAAV preparation that contains green flourescent protein (GFP) cDNA packaged as P5-associated contaminants, we establish a model to induce transaminitis and observe concomitant therapeutic efficacy reduction after rAAV administration. We observed strong epitope-specific anti-GFP responses in splenic CD8+ T cells when GFP cDNA was delivered as a P5-associated contaminant of rAAV, which coincided and correlated with alanine and aspartate aminotransferase elevations. Furthermore, we report a significant reduction in detectable circulating FVIII protein, as compared with control mice. Lastly, we observed an elevation in the detection of AAV8 capsid-specific T cells when GFP was delivered either as a contaminant or transgene to Ad5-CMV&#95;GFP-immunized mice. We present this model as a potential tool to study the underlying biology of post-AAV hepatotoxicity and demonstrate the potential for T cell responses against proteins produced from AAV encapsidated nontherapeutic nucleic acids, to interfere with efficacious gene transfer.

Published

2024

17. Immunogenicity profile of rurioctocog alfa pegol in previously treated patients with severe congenital hemophilia A.

Author

Horling FM, Reipert BM, Allacher P, Engl W, Pan L, and Tangada S

Subjects

Humans, Male, Antibodies, Neutralizing immunology, Adult, Adolescent, Animals, Recombinant Proteins therapeutic use, Recombinant Proteins immunology, Child, Young Adult, Factor VIII immunology, Factor VIII therapeutic use, Factor VIII adverse effects, Hemophilia A drug therapy, Hemophilia A immunology, Hemophilia A blood, Polyethylene Glycols therapeutic use

Abstract

Abstract: Rurioctocog alfa pegol is an extended-half-life full-length recombinant factor VIII (FVIII) bound to 20-kDa polyethylene glycol (PEG) that has been shown to be well tolerated and efficacious in the treatment and prevention of bleeding events in previously treated patients with severe hemophilia A. Here, we present a comprehensive analysis of immunogenicity data collected during 6 clinical studies of rurioctocog alfa pegol, including a total of 360 unique previously treated patients with severe hemophilia A. The analysis included treatment-emerging FVIII-neutralizing antibodies (FVIII inhibitors); preexisting and treatment-emerging antibodies binding to FVIII, PEG-FVIII, or PEG; and treatment-emerging antibodies binding to Chinese hamster ovary host cell proteins. Moreover, the potential association between the presence of these binding antibodies and adverse events (AEs) observed in patients was investigated, and the potential impact of these antibodies on the incremental recovery of rurioctocog alfa pegol in patients was analyzed. Overall, the data indicate that rurioctocog alfa pegol is not associated with any unexpected immunogenicity characteristics. Of 360 patients, 1 patient developed a transient FVIII inhibitor with a titer of 0.6 Bethesda units per mL, which was not associated with any serious AEs. Antibodies binding to FVIII, PEG-FVIII, or PEG were not detected at the time when the inhibitor was present. Moreover, 54 of 360 patients either entered the clinical studies with preexisting binding antibodies or developed these antibodies after exposure to rurioctocog alfa pegol. These antibodies were transient in most patients and did not show any causal relationship to either AEs or spontaneous bleeding episodes., (© 2024 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2024

18. Predicting inhibitor development using a random peptide phage-display library approach in the SIPPET cohort.

Author

Hassan S, Baselli G, Mollica L, Rossi RL, Chand H, El-Beshlawy A, Elalfy M, Ramanan V, Eshghi P, Karimi M, Palla R, Rosendaal FR, and Peyvandi F

Subjects

Humans, Epitope Mapping, Male, Cohort Studies, Epitopes immunology, Hemophilia A, Factor VIII immunology, Peptide Library

Abstract

Abstract: Inhibitor development is the most severe complication of hemophilia A (HA) care and is associated with increased morbidity and mortality. This study aimed to use a novel immunoglobulin G epitope mapping method to explore the factor VIII (FVIII)-specific epitope profile in the SIPPET cohort population and to develop an epitope mapping-based inhibitor prediction model. The population consisted of 122 previously untreated patients with severe HA who were followed up for 50 days of exposure to FVIII or 3 years, whichever occurred first. Sampling was performed before FVIII treatment and at the end of the follow-up. The outcome was inhibitor development. The FVIII epitope repertoire was assessed by means of a novel random peptide phage-display assay. A least absolute shrinkage and selection operator (LASSO) regression model and a random forest model were fitted on posttreatment sample data and validated in pretreatment sample data. The predictive performance of these models was assessed by the C-statistic and a calibration plot. We identified 27 775 peptides putatively directed against FVIII, which were used as input for the statistical models. The C-statistic of the LASSO and random forest models were good at 0.78 (95% confidence interval [CI], 0.69-0.86) and 0.80 (95% CI, 0.72-0.89). Model calibration of both models was moderately good. Two statistical models, developed on data from a novel random peptide phage display assay, were used to predict inhibitor development before exposure to exogenous FVIII. These models can be used to set up diagnostic tests that predict the risk of inhibitor development before starting treatment with FVIII., (© 2024 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2024

19. Comprehensive domain-specific analysis and immunoglobulin G profiling of anti-factor VIII antibodies using a bead-based multiplex immunoassay.

Author

Pezeshkpoor B, Berkemeier AC, Herbst K, Albert T, Müller J, and Oldenburg J

Subjects

Humans, Immunoassay methods, Predictive Value of Tests, Reproducibility of Results, Male, Protein Domains, Antibodies, Neutralizing blood, Antibodies, Neutralizing immunology, Adolescent, Microspheres, Factor VIII immunology, Hemophilia A immunology, Hemophilia A blood, Hemophilia A diagnosis, Immunoglobulin G blood, Immunoglobulin G immunology, Enzyme-Linked Immunosorbent Assay methods

Abstract

Background: Antibodies against factor (F)VIII are a major complication in the treatment of patients with severe hemophilia A. The Nijmegen-Bethesda assay (NBA) is the gold standard for detection of neutralizing antibodies (inhibitors), whereas both inhibitors and nonneutralizing antibodies can be detected by immunoassays such as enzyme-linked immunosorbent assay (ELISA) and multiplex bead-based assays., Objectives: Evaluation of an in-house Luminex bead-based assay (LumiTope) compared with a commercially available ELISA and NBA., Methods: The LumiTope method comprised full-length and B-domain-deleted FVIII as well as 9 purified FVIII single or multidomains. The respective proteins were coupled to magnetic beads to detect domain-specific immunoglobulin (IgG; IgG 1-4 ) anti-FVIII antibodies in a large cohort of patients with hemophilia A with and without inhibitors., Results: Overall, LumiTope assay had a high sensitivity (94.9%) and specificity (91.2%), particularly in patients with low-titer inhibitors compared with ELISA (sensitivity of 72.2% vs 27.7%). IgG 4 was the most abundant IgG subclass in NBA-positive patients. NBA-positive and -negative patients showed different domain profiles. Patients with genetic variants in the heavy chain predominantly exhibited antibodies specific to this chain, while those with a light-chain variant showed a more diverse distribution of antibody specificities. Patients with an intron 22 inversion resembled those with a light-chain defect, with a majority of antibodies targeting the light chain., Conclusion: LumiTope assay provides a sensitive and specific method for not only detection but also domain specification of anti-FVIII-antibodies. Implementation of bead-based assays could improve antibody detection, profiling, and comparability of results and complement NBA., Competing Interests: Declaration of competing interests B.P. reports having received grants for research from Biotest and Octapharma as well as personal fees for lectures and advisory board meetings from Novo Nordisk and Octapharma. A.-C.B. and K.H. report no conflict of interest. T.A. reports having received grants for a patient support association from Bayer, Biotest, Chugai, CSL Behring, Grifols, Novo Nordisk, Octapharma, Roche, Swedish Orphan Biovitrum, and Takeda, as well as personal fees for advisory board meetings, consulting and/or travel support from Bayer, BioMarin, Biotest, CSL Behring, Grifols, Novo Nordisk, Octapharma, Pfizer, Swedish Orphan Biovitrum, and Takeda. J.M. received honoraria from Siemens Healthineers and Octapharma. J.O. reports having received grants for studies and research from Bayer, Biotest, CSL Behring, Octapharma, Pfizer, Sobi, and Takeda and travel support as well as personal fees for lectures and advisory board meetings from Bayer, Biogen Idec, BioMarin, Biotest, CSL Behring, Chugai, Freeline, Grifols, Novo Nordisk, Octapharma, Pfizer, Roche, Sanofi, Sparks, Swedish Orphan Biovitrum, and Takeda., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

20. Inhibitor eradication and treatment for acquired hemophilia A.

Author

Franchini M and Focosi D

Subjects

Humans, Autoantibodies immunology, Rituximab therapeutic use, Disease Management, Hemophilia A drug therapy, Hemophilia A therapy, Hemophilia A immunology, Factor VIII therapeutic use, Factor VIII immunology, Immunosuppressive Agents therapeutic use

Abstract

Introduction: Acquired hemophilia A (AHA) is a rare hemorrhagic autoimmune disorder characterized by autoantibodies against coagulation factor VIII (FVIII). In approximately half of the cases AHA does not recognize any cause (idiopathic form), while in the other cases it may be triggered by autoimmune disorders, cancers, drugs, infections, or pregnancy. Besides treating the underlying disorder, specific AHA treatment includes management of bleeding, if necessary, and inhibitor eradication., Areas Covered: This narrative review summarizes the main epidemiological, clinical, laboratory, and therapeutic characteristics of AHA. In particular, it is focused on the current therapeutic options for the inhibitor eradication, also showing the latest findings on the innovative therapies. A literature search strategy was performed, without temporal limits, through Medline and PubMed electronic databases., Expert Opinion: Various first-line and second-line immunosuppressive agents are currently available for the management of AHA. Among the latter, the anti-CD20 monoclonal antibody rituximab has been the object of intense research during the last years from investigators as innovative promising eradicating therapy for AHA. Preliminary data from the studies support the use of this drug as a first-line option for newly diagnosed AHA cases.

Published

2024

21. Association of bullous pemphigoid with acquired hemophilia A: a case report.

Author

Abakarim O, Lahlimi FE, and Tazi I

Subjects

Humans, Female, Adult, Hemorrhage etiology, Factor VIII immunology, Partial Thromboplastin Time, Adrenal Cortex Hormones administration & dosage, Glucocorticoids administration & dosage, Autoantibodies blood, Hemophilia A complications, Pemphigoid, Bullous diagnosis

Abstract

Acquired hemophilia A, a rare condition resulting in spontaneous bleeding without prior bleeding disorders, arises due to autoantibody-mediated inhibition of coagulation factor VIII and is typically associated with autoimmune, neoplastic, drug, or obstetric factors. We present the case of a 31-year-old woman with bullous pemphigoid, managed with corticosteroids since 2013, who presented spontaneous hemorrhagic manifestations. Upon admission, laboratory tests revealed hypochromic microcytic anemia, prolonged activated partial thromboplastin time, and a factor VIII level < 1%, indicative of acquired hemophilia A. Further assessments showed elevated Ristocetin cofactor activity, von Willebrand factor antigen, and a factor VIII inhibitor level of 665 BU. This underscores the importance of considering acquired hemophilia A in autoimmune dermatological conditions like bullous pemphigoid, highlighting the association between autoimmune disorders and coagulation abnormalities, particularly in cases of spontaneous hemorrhagic events., Competing Interests: The authors declare no competing interests., (Copyright: Ouadii Abakarim et al.)

Published

2024

22. Clinical and economic burden of immune tolerance induction in entire patients with hemophilia A: Insights from a real-world Korean setting.

Author

Kim AY, Baek HJ, Lee S, Choo E, Park YS, and Lee H

Subjects

Humans, Republic of Korea, Male, Child, Adult, Adolescent, Child, Preschool, Factor VIII therapeutic use, Factor VIII immunology, Factor VIII economics, Cost of Illness, Young Adult, Female, Infant, Health Care Costs, Hemophilia A economics, Hemophilia A immunology, Hemophilia A drug therapy, Immune Tolerance

Abstract

Introduction: The most notable challenge facing hemophilia A treatment is the development of inhibitors against factor VIII, resulting in increased clinical and socioeconomic burdens due to the need for expensive bypassing agents (BPAs). Although immune tolerance induction (ITI) is currently the primary approach for inhibiting and reducing the inhibitors, the lengthy duration of ITI necessitates the continued use of BPA to manage bleeding episodes. In this study, we aimed to obtain real-world evidence on the clinical and economic aspects and associated burdens experienced by patients with hemophilia A with inhibitors undergoing ITI in Korea., Methods: Claims data from January 1, 2007, to December 31, 2020, were used in this study. The study cohort comprised patients with hemophilia A undergoing ITI, who were categorized into three groups: successful, failed, or continuation of ITI. We evaluated clinical and economic burdens, including monthly healthcare visits, medication costs, and total medical expenses., Results: The study involved 33 cases of ITI across 32 patients. Excluding seven continuation cases where success could not be determined at the observation point, the estimated success rate of ITI was 80.8 %. The median duration of ITI for all patients was 25.7 months. While no significant disparities were noted in the ITI duration between successful and unsuccessful cases (24.51 vs. 25.66 months), substantial discrepancies were observed in the duration of BPA usage (11.10 vs. 25.66 months) and the number of prescribed BPAs (1.79 vs. 2.97)., Conclusion: Successful ITI reduced both clinical and economic burdens, resulting in decreased monthly medication expenses and overall medical costs., Competing Interests: Declaration of competing interest All authors declare that they have no conflicts of interest., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

23. Cyclophosphamide vs rituximab for eradicating inhibitors in acquired hemophilia A: A randomized trial in 108 patients.

Author

Lévesque H, Viallard JF, Houivet E, Bonnotte B, Voisin S, Le Cam-Duchez V, Maillot F, Lambert M, Liozon E, Hervier B, Fain O, Guillet B, Schmidt J, Luca LE, Ebbo M, Ferreira-Maldent N, Babuty A, Sailler L, Duffau P, Barbay V, Audia S, Benichou J, Graveleau J, and Benhamou Y

Subjects

Humans, Male, Female, Middle Aged, Aged, Immunosuppressive Agents therapeutic use, Adult, Factor VIII therapeutic use, Factor VIII immunology, Aged, 80 and over, Rituximab therapeutic use, Hemophilia A drug therapy, Cyclophosphamide therapeutic use

Abstract

Background: Acquired hemophilia A (AHA) is a rare autoimmune disorder due to autoantibodies against Factor VIII, with a high mortality risk. Treatments aim to control bleeding and eradicate antibodies by immunosuppression. International recommendations rely on registers and international expert panels., Methods: CREHA, an open-label randomized trial, compared the efficacy and safety of cyclophosphamide and rituximab in association with steroids in patients with newly diagnosed AHA. Participants were treated with 1 mg/kg prednisone daily and randomly assigned to receive either 1.5-2 mg/kg/day cyclophosphamide orally for 6 weeks, or 375 mg/m 2 rituximab once weekly for 4 weeks. The primary endpoint was complete remission over 18 months. Secondary endpoints included time to achieve complete remission, relapse occurrence, mortality, infections and bleeding, and severe adverse events., Results: Recruitment was interrupted because of new treatment recommendations after 108 patients included (58 cyclophosphamide, 50 rituximab). After 18 months, 39 cyclophosphamide patients (67.2 %) and 31 rituximab patients (62.0 %) were in complete remission (OR 1.26; 95 % CI, 0.57 to 2.78). In the poor prognosis group (FVIII < 1 IU/dL, inhibitor titer > 20 BU mL -1 ), significantly more remissions were observed with cyclophosphamide (22 patients, 78.6 %) than with rituximab (12 patients, 48.0 %; p = 0.02). Relapse rates, deaths, severe infections, and bleeding were similar in the 2 groups. In patients with severe infection, cumulative doses of steroids were significantly higher than in patients without infection (p = 0.03)., Conclusion: Cyclophosphamide and rituximab showed similar efficacy and safety. As first line, cyclophosphamide seems preferable, especially in poor prognosis patients, as administered orally and less expensive., Funding: French Ministry of Health., Clinicaltrials: gov number: NCT01808911., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

24. Emicizumab: the hemophilia A game-changer.

Author

Alcedo Andrade PE, Mannucci PM, and Kessler CM

Subjects

Humans, Hemorrhage etiology, Factor VIII therapeutic use, Factor VIII immunology, Hemophilia A drug therapy, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized adverse effects, Antibodies, Monoclonal, Humanized administration & dosage, Antibodies, Bispecific therapeutic use, Antibodies, Bispecific adverse effects

Abstract

In hemophilia, the unmet needs regarding adherence to prophylaxis and lack of effective long-term prophylaxis regimens, especially in patients with inhibitors, led to the production of emicizumab, the first non-factor medicine for subcutaneous administration in patients with severe and moderate hemophilia A with or without factor VIII inhibitors. This review describes the research steps behind the development of this game-changing medication as well as its success in the prophylaxis of bleeding episodes, as witnessed by the results of pivotal clinical trials but also by real-life use in the frame of a still expanding global market. We also discuss potential and actual adverse events and the nuances related to clinical use, such as laboratory monitoring, development of neutralizing antidrug antibodies, risk of thrombosis/hypercoagulability and role in the management of surgical operations. The potential of emicizumab to prevent bleeding in other congenital and acquired coagulation disorders is also outlined.

Published

2024

25. The effects of emicizumab on in vitro coagulation and fibrinolysis parameters in patients with disseminated intravascular coagulation with and without addition of anti-FVIII antibody.

Author

Onishi T, Shimo H, Harada S, and Nogami K

Subjects

Female, Humans, Male, Factor VIII therapeutic use, Factor VIII pharmacology, Factor VIII immunology, Antibodies, Bispecific therapeutic use, Antibodies, Bispecific pharmacology, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized pharmacology, Blood Coagulation drug effects, Disseminated Intravascular Coagulation drug therapy, Disseminated Intravascular Coagulation etiology, Disseminated Intravascular Coagulation blood, Fibrinolysis drug effects

Abstract

Background: Emicizumab (Emi) is used as haemostatic prophylaxis for patients with haemophilia A (PwHA). Disseminated intravascular coagulation (DIC) is a condition characterized by persistent systemic activation of coagulation, but there is yet no information on coagulation and fibrinolysis potentials in Emi-treated PwHA with DIC., Aim: To examine the effect of Emi on coagulation and fibrinolysis potentials in HA-model DIC plasmas., Methods: Plasma from a patient with sepsis-DIC (seven patients) was treated with anti-factor (F)VIII monoclonal antibody (HA-model DIC plasma) and incubated with Emi (50 µg/mL). The plasma was then assessed using clot-fibrinolysis waveform analysis (CFWA). Coagulation and fibrinolysis parameters were expressed as ratios relative to normal plasma (|min1|-ratio and |FL-min1|-ratio, respectively)., Patients and Results: In case 1, coagulant potential was slightly high and fibrinolytic potential was extremely low, presenting a coagulant-dominant state (|min1|-ratio/|FL-min1|-ratio: 1.1/.38). In cases 2-5, fibrinolytic potential was not suppressed, but there were marked hypercoagulant potentials, indicating relative coagulant-dominant states. In case 6, coagulant and fibrinolytic potentials were increased but well balanced (|min1|-ratio/|FL-min1|-ratio: 1.38/1.28). In case 7, both potentials were severely deteriorated in not only CFWA but also the thrombin/plasmin generation assay. The addition of Emi into the HA-model DIC plasmas increased |min1|-ratio values in all cases, but the coagulant potentials did not exceed the initial ones (DIC plasma before treatment with anti-FVIII antibody)., Conclusions: The presence of Emi in the HA-model DIC plasma improved coagulation potentials, but did not increase coagulation potentials beyond those of DIC plasma in non-HA states., (© 2024 John Wiley & Sons Ltd.)

Published

2024

26. Factor VIII moiety of recombinant Factor VIII Fc fusion protein impacts Fc effector function and CD16 + NK cell activation.

Author

Lagassé HAD, Ou J, Sauna ZE, and Golding B

Subjects

Humans, Cell Degranulation immunology, Hemophilia A immunology, Hemophilia A drug therapy, Interferon-gamma metabolism, Protein Binding, Factor VIII chemistry, Factor VIII immunology, GPI-Linked Proteins immunology, GPI-Linked Proteins metabolism, Immunoglobulin Fc Fragments immunology, Killer Cells, Natural immunology, Killer Cells, Natural metabolism, Lymphocyte Activation immunology, Lymphocyte Activation drug effects, Receptors, IgG metabolism, Receptors, IgG immunology, Recombinant Fusion Proteins

Abstract

Recombinant Factor VIII-Fc fusion protein (rFVIIIFc) is an enhanced half-life therapeutic protein product used for the management of hemophilia A. Recent studies have demonstrated that rFVIIIFc interacts with Fc gamma receptors (FcγR) resulting in the activation or inhibition of various FcγR-expressing immune cells. We previously demonstrated that rFVIIIFc, unlike recombinant Factor IX-Fc (rFIXFc), activates natural killer (NK) cells via Fc-mediated interactions with FcγRIIIA (CD16). Additionally, we showed that rFVIIIFc activated CD16 + NK cells to lyse a FVIII-specific B cell clone. Here, we used human NK cell lines and primary NK cells enriched from peripheral blood leukocytes to study the role of the FVIII moiety in rFVIIIFc-mediated NK cell activation. Following overnight incubation of NK cells with rFVIIIFc, cellular activation was assessed by measuring secretion of the inflammatory cytokine IFNγ by ELISA or by cellular degranulation. We show that anti-FVIII, anti-Fc, and anti-CD16 all inhibited indicating that these molecules were involved in rFVIIIFc-mediated NK cell activation. To define which domains of FVIII were involved, we used antibodies that are FVIII domain-specific and demonstrated that blocking FVIII C1 or C2 domain-mediated membrane binding potently inhibited rFVIIIFc-mediated CD16 + NK cell activation, while targeting the FVIII heavy chain domains did not. We also show that rFVIIIFc binds CD16 with about five-fold higher affinity than rFIXFc. Based on our results we propose that FVIII light chain-mediated membrane binding results in tethering of the fusion protein to the cell surface, and this, together with increased binding affinity for CD16, allows for Fc-CD16 interactions to proceed, resulting in NK cellular activation. Our working model may explain our previous results where we observed that rFVIIIFc activated NK cells via CD16, whereas rFIXFc did not despite having identical IgG1 Fc domains., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The author(s) declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision., (Copyright © 2024 Lagassé, Ou, Sauna and Golding.)

Published

2024

27. Emicizumab as a Promising Form of Therapy for Type A Hemophilia - A Review of Current Knowledge from Clinical Trials.

Author

Grabowska K, Grzelak M, Zhao LY, Płuciennik E, Pasieka Z, Kciuk M, Gielecińska A, Smakosz AK, Kałuzińska-Kołat Ż, and Kołat D

Subjects

Humans, Factor VIII therapeutic use, Factor VIII immunology, Hemorrhage drug therapy, Hemophilia A drug therapy, Hemophilia A immunology, Antibodies, Bispecific therapeutic use, Antibodies, Bispecific pharmacology, Antibodies, Monoclonal, Humanized therapeutic use, Clinical Trials as Topic

Abstract

Hemophilia is a plasma bleeding disorder characterized by a deficiency of certain blood clotting factors. The most common forms of this disease, i.e., type A and type B, affect approximately 400,000 people worldwide. Without appropriate treatment ensuring the proper coagulation cascade, this disease may lead to serious disability. Minimizing patient discomfort is possible via replacement therapy, consisting of the substitution of a missing coagulation factor via intravenous administration. Frequent medication and the risk related to factor inhibitors are significant disadvantages, necessitating the improvement of current therapies or the development of novel ones. This review examines the humanized bispecific antibody Emicizumab which ensures hemostasis by mimicking the action of the coagulation factor VIII, a deficiency of which causes type A hemophilia. The paper outlines the topic and then summarizes available clinical trials on Emicizumab in type A hemophilia. Several interventional clinical trials have found Emicizumab to be effective in decreasing bleeding episodes and raising patient satisfaction among various hemophilia A populations. Current Emicizumab-related trials are forecast to be completed between 2024 and 2030, and in addition to congenital hemophilia A, the trials cover acquired hemophilia A and patients playing sports. Providing a more comprehensive understanding of Emicizumab may revolutionize the management of hemophilia type A and improve quality of life. Conclusively, Emicizumab is a gentler therapy owing to subcutaneous delivery and fewer injections, which reduces injection-site reactions and makes therapy less burdensome, ultimately decreasing hospital visits and indirect costs., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2024

28. Peripheral Blood Lymphocyte Subsets in Factor VIII Inhibitor-Positive Patients with Severe Hemophilia A: A Case-Control Study.

Author

Zhao L, Zhang Y, Guo X, Li Z, Lu W, Pan Z, Guo Y, Sun J, Zhang Y, Hao J, and Guo Z

Subjects

Humans, Case-Control Studies, Male, Adult, Adolescent, Young Adult, Female, Child, Hemophilia A blood, Hemophilia A immunology, Factor VIII immunology, Lymphocyte Subsets

Abstract

Introduction and Objectives: The present study aimed to investigate different peripheral lymphocyte subsets in patients with severe hemophilia A (HA) and factor VIII (FVIII) inhibitor production. For this, age-matched cases of 19 FVIII inhibitor-positive (IP), 21 FVIII inhibitor-negative (IN) and 45 healthy controls were selected for study., Methods: Flow cytometry was used to analyze the peripheral lymphocyte subsets, including T, B, natural killer (NK) and NKT cells. The T cell subsets included CD3 + CD4-CD8- [double negative T (DNT)], CD3 + CD4 + CD8+ [double-positive T (DPT)], CD3 + CD4 + CD8- and CD3 + CD4-CD8+ T cells. Pairwise comparisons of absolute lymphocyte subset values were conducted among the three groups. The cut-off value for absolute lymphocyte counts was determined using receiver operating characteristic curve analysis., Results: The results demonstrated that the absolute values of DPT cells in the IN and IP groups were significantly lower than those in the healthy control group ( P =  0.007). The DNT values were also lower in severe HA patients with or without inhibitor than those in healthy subjects, but these differences were not statistically significant ( P =  0.053). In addition, the absolute value of CD4+ Th cells in the IP group was lower than that in the healthy controls ( P  = 0.013). Although not statistically significant ( P  = 0.064), the absolute values of NKT cells were higher in the IN group compared with the IP group, and higher in the IP group compared with the healthy control group. There were no statistically significant differences in total T, B, CD8  +  and NK cells among the IN, IP and healthy control groups. The cut-off value for absolute CD4+ Th cells in the IN group was < 598/µl., Conclusion: The decrease in absolute values of CD4+ Th cells in severe HA patients may contribute to the establishment of infused FVIII immune tolerance. If the CD4+ Th value remains > 598/µl, clinicians should be vigilant for possible FVIII inhibitor production, especially on days prior to FVIII exposure., Competing Interests: Declaration of Conflicting InterestsThe authors declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

29. Factor VIII trafficking to CD4+ T cells shapes its immunogenicity and requires several types of antigen-presenting cells.

Author

Kaczmarek R, Piñeros AR, Patterson PE, Bertolini TB, Perrin GQ, Sherman A, Born J, Arisa S, Arvin MC, Kamocka MM, Martinez MM, Dunn KW, Quinn SM, Morris JJ, Wilhelm AR, Kaisho T, Munoz-Melero M, Biswas M, Kaplan MH, Linnemann AK, George LA, Camire RM, and Herzog RW

Subjects

Animals, Mice, Dendritic Cells metabolism, Ovalbumin immunology, CD4-Positive T-Lymphocytes, Factor VIII immunology, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemostatics immunology, Hemostatics therapeutic use

Abstract

Despite >80 years of clinical experience with coagulation factor VIII (FVIII) inhibitors, surprisingly little is known about the in vivo mechanism of this most serious complication of replacement therapy for hemophilia A. These neutralizing antidrug alloantibodies arise in ∼30% of patients. Inhibitor formation is T-cell dependent, but events leading up to helper T-cell activation have been elusive because of, in part, the complex anatomy and cellular makeup of the spleen. Here, we show that FVIII antigen presentation to CD4+ T cells critically depends on a select set of several anatomically distinct antigen-presenting cells, whereby marginal zone B cells and marginal zone and marginal metallophilic macrophages but not red pulp macrophages (RPMFs) participate in shuttling FVIII to the white pulp in which conventional dendritic cells (DCs) prime helper T cells, which then differentiate into follicular helper T (Tfh) cells. Toll-like receptor 9 stimulation accelerated Tfh cell responses and germinal center and inhibitor formation, whereas systemic administration of FVIII alone in hemophilia A mice increased frequencies of monocyte-derived and plasmacytoid DCs. Moreover, FVIII enhanced T-cell proliferation to another protein antigen (ovalbumin), and inflammatory signaling-deficient mice were less likely to develop inhibitors, indicating that FVIII may have intrinsic immunostimulatory properties. Ovalbumin, which, unlike FVIII, is absorbed into the RPMF compartment, fails to elicit T-cell proliferative and antibody responses when administered at the same dose as FVIII. Altogether, we propose that an antigen trafficking pattern that results in efficient in vivo delivery to DCs and inflammatory signaling, shape the immunogenicity of FVIII., (© 2023 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2023

30. Immune tolerance induction in development.

Author

Berntorp E

Subjects

Humans, Immune Tolerance immunology, Factor VIII immunology, Hemophilia A immunology

Published

2023

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

Author

Becker-Gotot J, Meissner M, Kotov V, Jurado-Mestre B, Maione A, Pannek A, Albert T, Flores C, Schildberg FA, Gleeson PA, Reipert BM, Oldenburg J, and Kurts C

Subjects

Animals, Humans, Mice, Programmed Cell Death 1 Receptor metabolism, Disease Models, Animal, B7-H1 Antigen metabolism, Factor VIII administration & dosage, Factor VIII immunology, Hemophilia A drug therapy, Immune Tolerance, T-Lymphocytes, Regulatory immunology, Isoantibodies immunology, B-Lymphocytes

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.

Published

2022

32. Plasma-derived FVIII/VWF complex shows higher protection against inhibitors than isolated FVIII after infusion in haemophilic patients: A translational study.

Author

Bravo MI, Pérez A, Raventós A, Grancha S, Jorquera JI, Butta NV, Álvarez-Román MT, Costa M, Willis T, and Jiménez-Yuste V

Subjects

Animals, Disease Models, Animal, Immunoglobulin G immunology, Mice, Recombinant Proteins administration & dosage, Factor VIII administration & dosage, Factor VIII immunology, Factor VIII isolation & purification, Hemophilia A therapy, von Willebrand Factor administration & dosage, von Willebrand Factor isolation & purification

Abstract

Introduction: Presence of von Willebrand factor (VWF) in FVIII concentrates offers protection against neutralizing inhibitors in haemophilia A (HA). Whether this protection is more evident in plasma-derived (pd) FVIII/VWF or recombinant (r) FVIII concentrates remains controversial., Aim: We investigated the protection exerted by VWF against FVIII inhibitors in an in vivo mouse model of HA exposed to pdFVIII/VWF or to various rFVIII concentrates., Methods: Haemophilia A mice received the different FVIII concentrates after administration of vehicle or an inhibitory IgG purified from a commercial pool of HA plasma with inhibitors and FVIII:C recoveries were measured. Furthermore, using a novel clinically oriented ex vivo approach, Bethesda inhibitory activities (BU) of a commercial pool of HA plasma with inhibitors were assessed using normal plasma, or plasma from severe HA patients, without inhibitors, after treatment with the same concentrates., Results: in vivo studies showed that pdFVIII/VWF offers markedly higher protection against inhibitors when compared with any of the FVIII products without VWF. More importantly, in the ex vivo studies, plasma from patients treated with pdFVIII/VWF showed higher protection against inhibitors (P values ranging .05-.001) in comparison with that observed in plasma from patients who received FVIII products without VWF, regardless of the type of product evaluated., Conclusion: Data indicate that FVIII+VWF complexes assembled in the circulation after rFVIII infusion are not equivalent to the naturally formed complex in pdFVIII/VWF. Therefore, rFVIII infused into HA patients with inhibitors would be less protected by VWF than the FVIII in pdFVIII/VWF concentrates., (© 2022 The Authors. Haemophilia published by John Wiley & Sons Ltd.)

Published

2022

33. Nonhuman glycans can regulate anti-factor VIII antibody formation in mice.

Author

Arthur CM, Zerra PE, Shin S, Wang J, Song X, Doering CB, Lollar P, Meeks S, and Stowell SR

Subjects

Animals, CHO Cells, Cricetinae, Cricetulus, Hemophilia A genetics, Hemophilia A immunology, Mice, Mice, Knockout, Recombinant Proteins immunology, Recombinant Proteins pharmacology, Antibodies genetics, Antibodies immunology, Antibody Formation, Blood Coagulation Factor Inhibitors genetics, Blood Coagulation Factor Inhibitors immunology, Factor VIII immunology, Factor VIII pharmacology, Polysaccharides genetics, Polysaccharides immunology, Protein Processing, Post-Translational immunology

Abstract

Recombinant factor VIII (FVIII) products represent a life-saving intervention for patients with hemophilia A. However, patients can develop antibodies against FVIII that prevent its function and directly increase morbidity and mortality. The development of anti-FVIII antibodies varies depending on the type of recombinant product used, with previous studies suggesting that second-generation baby hamster kidney (BHK)-derived FVIII products display greater immunogenicity than do third-generation Chinese hamster ovary (CHO)-derived FVIII products. However, the underlying mechanisms responsible for these differences remain incompletely understood. Our results demonstrate that BHK cells express higher levels of the nonhuman carbohydrate α1-3 galactose (αGal) than do CHO cells, suggesting that αGal incorporation onto FVIII may result in anti-αGal antibody recognition that could positively influence the development of anti-FVIII antibodies. Consistent with this, BHK-derived FVIII exhibits increased levels of αGal, which corresponds to increased reactivity with anti-αGal antibodies. Infusion of BHK-derived, but not CHO-derived, FVIII into αGal-knockout mice, which spontaneously generate anti-αGal antibodies, results in significantly higher anti-FVIII antibody formation, suggesting that the increased levels of αGal on BHK-derived FVIII can influence immunogenicity. These results suggest that posttranslational modifications of recombinant FVIII products with nonhuman carbohydrates may influence the development of anti-FVIII antibodies., (© 2022 by The American Society of Hematology.)

Published

2022

34. Measurement of coagulation factor antibody levels is useful for diagnosis and determining therapeutic efficacy in hemorrhagic patients with autoantibodies to coagulation factor VIII and factor V: results from a single center in Japan.

Author

Ieko M, Ohmura K, Naito S, Yoshida M, Saito M, Kiyohara K, Miyazima S, Maeta T, Ohtsu A, Shimosegawa K, Takahashi N, and Ichinose A

Subjects

Aged, Aged, 80 and over, Biomarkers blood, Enzyme-Linked Immunosorbent Assay, Female, Humans, Japan, Male, Middle Aged, Autoantibodies blood, Autoimmune Diseases diagnosis, Factor V immunology, Factor VIII immunology, Hemophilia A diagnosis, Immunoglobulin G blood

Abstract

Coagulation factor inhibitors (CFIs) sometimes cause fatal bleeding conditions. Determination of an inhibitor titer (INH-titer) using the Bethesda method is essential for diagnosing diseases associated with CFIs and examining the effects of immunosuppressive therapy. We reviewed 17 cases with CFIs (acquired hemophilia A, n = 11; FV inhibitor, n = 6) to examine the usefulness of determining quantities of an autoantibody to a coagulation factor (CF-IgG) by ELISA for diagnosis and therapeutic efficacy, as compared with INH-titer. One patient with an INH-titer and no evidence of CF-IgG was lupus anticoagulant (LA)-positive, and thus the positive INH-titer may have been a false positive caused by LA. Although INH-titer alone was insufficient to correctly identify patients with CFI, determination of CF-IgG appeared to be useful. In addition, even after INH-titer disappearance, hemorrhagic conditions recurred when CF-IgG was detected. These findings suggest that the presence of a clearance antibody against the coagulation factor might reduce the activity of that coagulation factor even after disappearance of the corresponding neutralizing antibody. Although the diagnosis and therapeutic efficacy can also be determined by INH-titer disappearance and improvement of corresponding coagulation factor activity, determination of CF-IgG by ELISA can improve the accuracy of these assessments., (© 2021. Japanese Society of Hematology.)

Published

2022

35. FVIII at the crossroad of coagulation, bone and immune biology: Emerging evidence of biological activities beyond hemostasis.

Author

Cadé M, Muñoz-Garcia J, Babuty A, Fouassier M, Heymann MF, Monahan PE, and Heymann D

Subjects

Drug Discovery methods, Hemophilia A drug therapy, Hemophilia A metabolism, Hemostasis drug effects, Hemostasis physiology, Humans, Antibodies, Monoclonal, Humanized pharmacology, Bone Remodeling drug effects, Factor VIII immunology, Factor VIII metabolism, Immunity drug effects

Abstract

Hemophilia A is an X-linked hereditary disorder that results from deficient coagulation factor VIII (FVIII) activity, leading to spontaneous bleeding episodes, particularly in joints and muscles. FVIII deficiency has been associated with altered bone remodeling, dysregulated macrophage polarization, and inflammatory processes that are associated with the neoformation of abnormal blood vessels. Treatment based on FVIII replacement can lead to the development of inhibitors that render FVIII concentrate infusion ineffective. In this context, hemophilia has entered a new therapeutic era with the development of new drugs, such as emicizumab, that seek to restore the hemostatic balance by bypassing pathologically acquired antibodies. We discuss the potential extrahemostatic functions of FVIII that may be crucial for defining future therapies in hemophilia., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

36. A low-dose rituximab regimen for first-line treatment of acquired haemophilia A.

Author

Hunt S, Robertson J, Conn J, Casey J, Royle J, Collins J, Hourigan M, Richmond J, Yang Wang T, Mills A, and Mason J

Subjects

Adult, Aged, Aged, 80 and over, Autoantibodies immunology, Autoimmunity, Disease Management, Disease Susceptibility immunology, Factor VIII immunology, Female, Hemophilia A diagnosis, Humans, Immunologic Factors therapeutic use, Immunosuppressive Agents administration & dosage, Immunosuppressive Agents therapeutic use, Male, Middle Aged, Prognosis, Rituximab therapeutic use, Treatment Outcome, Hemophilia A drug therapy, Hemophilia A etiology, Immunologic Factors administration & dosage, Rituximab administration & dosage

Abstract

A low-dose rituximab regimen for first-line treatment of acquired haemophilia A., Introduction: Acquired haemophilia A (AHA) is a rare disease caused by the development of autoantibodies against FVIII. Diagnosis involves confirmation of FVIII deficiency and the presence of an inhibitor via the Bethesda assay. Severe bleeding is often managed with bypassing agents such as recombinant factor VII. This is then followed by eradication of the inhibitor with immunosuppression which typically includes a corticosteroid backbone., Aim: Review the current management and outcomes of AHA in Queensland, Australia. Determine the incidence, demographics and clinical characteristics of AHA patients., Methods: Retrospective case series of AHA diagnosed between May 2014 and August 2018. Data were derived from the Australian Bleeding Disorders Registry and state-wide pathology database. Data collection proforma was completed by the treating haematologist and reviewed/compiled centrally., Results: 24 patients were identified (incidence 1 in 1.27 million). The median age was 76.5 years. Median follow-up was 20 months. Index bleed was atraumatic and skin/soft tissue in the majority of patients. Recombinant FVIIa was the most commonly used haemostatic therapy and effective in 85% of patients. Immunosuppression and steroid usage were uniform. Upfront second agent was used in 75% of patients and was most commonly rituximab. 87.5% of patients achieved a complete remission in a median time of 48 days. Low-dose rituximab was frequently used and equally as efficacious as standard dose., Conclusion: Immunosuppression with combination therapy, notably rituximab, appears to be non-inferior and has a favourable side effect profile., (© 2021 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2022

37. Serum TNF- α Level as a Possible Predictor of Inhibitor Levels in Severe Hemophilia A.

Author

Susanah S, Raspati H, Sari NM, Rakhmilla LE, Sribudiani Y, Moestopo O, Sinaga P, Idjradinata P, and Maskoen AM

Subjects

Adolescent, Biomarkers, Pharmacological blood, Child, Child, Preschool, Cross-Sectional Studies, Factor VIII genetics, Factor VIII metabolism, Hemophilia A drug therapy, Humans, Indonesia, Infant, Isoantibodies immunology, Male, Polymorphism, Single Nucleotide genetics, Prognosis, Risk Factors, Tumor Necrosis Factor-alpha blood, Young Adult, Factor VIII immunology, Hemophilia A metabolism, Tumor Necrosis Factor-alpha genetics

Abstract

Background: The development of factor VIII (FVIII) inhibitor in patients with hemophilia A (PWHA) is a great challenge for hemophilia care. Both genetic and environmental factors led to complications in PWHA. The development of inhibitory antibodies is usually induced by the immune response. Tumor necrosis factor α (TNF- α ), one of the cytokines, might contribute to its polymorphism. In this study, we investigated the clinical factors, level of serum TNF- α , and polymorphism of c.-308G > A TNF - α gene in inhibitor development in severe PWHA., Methods: A cross-sectional study was conducted among all PWHA in West Java province. The clinical parameters, FVIII, FVIII inhibitor, and serum TNF- α level were assessed. The genotyping of -380G > A TNF- α gene polymorphism was performed using polymerase chain reaction and Sanger sequencing., Results: Among the 258 PWHA, 216 (83.7%) were identified as severe PWHA. The FVIII inhibitor was identified in 90/216 (41.6%) of severe PWHA, consisting of 45 high-titer inhibitors (HTI) and 45 low-titer inhibitors (LTI). There was a significant correlation between serum TNF- α level and the development of HTI ( p = 0.043). The cutoff point of serum TNF- α level, which can be used to differentiate between HTI and LTI, was 11.45 pg/mL. The frequency of FVIII replacement therapy was significant only in HTI of severe PWHA regarding serum TNF- α level ( p = 0.028). There is no correlation between polymorphisms of -380G > A TNF- α gene and inhibitor development ( p = 0.645)., Conclusions: The prevalence of FVIII inhibitor in severe PWHA in West Java, Indonesia, was 41.6%. The frequency of replacement therapy is a risk factor for inhibitor development. Serum TNF- α level might be used to differentiate between high and low inhibitor levels in severe hemophilia A, and this might support decision making regarding treatment options for inhibitor in severe hemophilia A., Competing Interests: The authors declare no conflict of interest regarding the publication of this article., (Copyright © 2021 Susi Susanah et al.)

Published

2021

38. Simoctocog Alfa (Nuwiq) in Previously Untreated Patients with Severe Haemophilia A: Final Results of the NuProtect Study.

Author

Liesner RJ, Abraham A, Altisent C, Belletrutti MJ, Carcao M, Carvalho M, Chambost H, Chan AKC, Dubey L, Ducore J, Gattens M, Gresele P, Gruel Y, Guillet B, Jimenez-Yuste V, Kitanovski L, Klukowska A, Lohade S, Mancuso ME, Oldenburg J, Pavlova A, Pollio B, Sigaud M, Vdovin V, Vilchevska K, Wu JKM, Jansen M, Belyanskaya L, Walter O, Knaub S, and Neufeld EJ

Subjects

Coagulants immunology, Factor VIII genetics, Factor VIII immunology, Genetic Predisposition to Disease, Hemophilia A blood, Hemophilia A genetics, Hemorrhage blood, Hemorrhage diagnosis, Hemorrhage genetics, Humans, Infant, Male, Mutation, Prospective Studies, Recombinant Proteins immunology, Recombinant Proteins therapeutic use, Severity of Illness Index, Time Factors, Treatment Outcome, Antibodies blood, Coagulants therapeutic use, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemorrhage prevention & control

Abstract

Introduction:  FVIII inhibitor development is the most serious contemporary treatment complication in haemophilia A, particularly in previously untreated patients (PUPs). No inhibitors developed in clinical trials in previously treated patients treated with simoctocog alfa (Nuwiq), a fourth-generation recombinant FVIII produced in a human cell line., Methods:  The NuProtect study investigated the immunogenicity of simoctocog alfa in PUPs. NuProtect was a prospective, multinational, open-label, non-controlled, phase III study. PUPs with severe haemophilia A (FVIII:C <1%) of any age and ethnicity were treated with simoctocog alfa for 100 exposure days or a maximum of 5 years. Patients were true PUPs without prior exposure to FVIII concentrates or blood components. Inhibitor titres were measured with the Nijmegen-modified Bethesda assay; cut-off for positivity was 0.6 BU mL -1 (≥0.6 to <5 low-titre, ≥5 high titre)., Results:  A total of 108 PUPs with a median age at first treatment of 12.0 months (interquartile range: 8.0-23.5) were treated with simoctocog alfa. F8 mutation type was known for 102 patients (94.4%) of whom 90 (88.2%) had null F8 mutations and 12 (11.8%) had non-null mutations. Of 105 PUPs evaluable for inhibitor development, 28 (26.7%) developed inhibitors; 17 high titre (16.2%) and 11 low titre (10.5%). No PUPs with non-null F8 mutations developed inhibitors., Conclusion:  In the NuProtect study, the rate of inhibitor development in PUPs with severe haemophilia A treated with simoctocog alfa was lower than the rate reported for hamster-cell-derived recombinant factor VIII products in other recent clinical trials. No inhibitors were reported in PUPs with non-null F8 mutations., Competing Interests: R. J. Liesner, A. Abraham, C. Altisent, M. J. Belletrutti, M. Carcao, M. Carvalho, H. Chambost, A. K. C. Chan, L. Dubey, J. Ducore, M. Gattens, P. Gresele, Y. Gruel, B. Guillet, V. J. Yuste, L. Kitanovski, A. Klukowska, S. Lohade, J. Oldenburg, A. Pavlova, B. Pollio, M. Sigaud, V. Vdovin, K. Vilchevska, J. K. M. Wu and E. J. Neufeld were clinical study investigators for the NuProtect Study (Octapharma-sponsored). R. J. Liesner has received grants/research support from Octapharma, Bayer, Baxalta, Novo Nordisk and Roche, has acted as a consultant for Bayer and Baxalta, and has participated in speaker bureaus for Novo Nordisk, Octapharma and SOBI. A. Abraham has received grants/research support from Novo Nordisk and Roche, and has received support for attending scientific meetings from Novo Nordisk. C. Altisent has been a member of advisory boards and/or speaker bureaus for Baxalta (Shire), Bayer, CSL Behring, Grifols, Octapharma, Novo Nordisk, Pfizer, Roche and SOBI. M. J. Belletrutti has received research support from Octapharma, has acted as a consultant for Roche Canada, Sanofi and Takeda Canada, and has participated in speaker bureaus for Octapharma Canada and Takeda Canada. M. Carcao received research support/grants from Bayer, Novo Nordisk, Pfizer, Sanofi and Takeda, and has participated in speaker bureaus for Bayer, CSL Behring, Grifols, LFB, Novo Nordisk, Octapharma, Pfizer, Roche, Sanofi and Takeda. M. Carvalho has been an investigator on clinical trials sponsored by CSL Behring, Novo Nordisk, Octapharma and Roche, and has received support for attending scientific meetings and honoraria (speaker fees/consultant in advisory boards) for Bayer, Baxalta (Shire), CSL Behring, Novo Nordisk, Octapharma, Pfizer, Siemens, SOBI and Stago. H. Chambost has received research support from CSL Behring, LFB, Novo Nordisk, Octapharma, Roche/Chugaï, Shire/Takeda, SOBI; honoraria from Bayer, LFB, Octapharma, Pfizer, Roche and SOBI. A. K. C. Chan has been an investigator on clinical trials sponsored by Bayer, Biogen, CSL, Novo Nordisk, Octapharma and Shire and has received grants/research support from Bayer and Pfizer, and has participated in advisory boards for Bayer, Biogen, BioMarin, Novo Nordisk and Octapharma. J. Ducore has been an investigator on clinical trials sponsored by Octapharma, CSL Behring, OPKO Biologics, Bayer, Baxalta (Shire), Sparks Therapeutics, Biogen, Pfizer, Genentech (Roche), LFB and RevBio, has provided consultancy services to Octapharma, Bayer, Baxalta (Shire), Biogen and LFB, and is a speaker for Bayer. Y. Gruel has received support for attending scientific meetings and honoraria (speaker fees/consultant in advisory boards) from Baxalta (Shire), Bayer Healthcare, CSL Behring, LFB, Novo Nordisk, Octapharma, Pfizer, Roche and SOBI, has been an investigator in studies sponsored by Biogen, LFB and SOBI, and has received research support from CSL Behring, LFB and Octapharma. B. Guillet has been an investigator on clinical trials, or has received honoraria for speaking/consulting or funds for research from Bayer, CSL Behring, LFB, Novo Nordisk, Octapharma, Roche, SOBI and Takeda/Shire. V. J. Yuste has received reimbursement for attending symposia/congresses and/or honoraria for speaking and/or honoraria for consulting, and/or funds for research from Shire, Bayer, CSL Behring, Grifols, Novo Nordisk, SOBI, Octapharma and Pfizer. A. Klukowska has received personal fees from CSL Behring, Novo Nordisk, Octapharma, Pfizer, Roche, Shire and SOBI. M. E. Mancuso has received speaker and/or consultancy fees from Bayer Healthcare, CSL Behring, Takeda, Octapharma, Roche, Pfizer, Kedrion, Grifols, Novo Nordisk and SOBI. J. Oldenburg has received reimbursement for attending symposia/congresses or honoraria for speaking or honoraria for consulting, or funds for research from Bayer, Biogen Idec, Biotest, Chugai, CSL Behring, Grifols, Novo Nordisk, Octapharma, Pfizer, Roche, Shire and SOBI. A. Pavlova has participated in studies sponsored by Octapharma AG. B. Pollio has received support for attending scientific meetings and honoraria (speaker fees/consultant in advisory boards) from Baxalta (Shire), Bayer Healthcare, CSL Behring, Kedrion, Novo Nordisk, Octapharma, Pfizer and SOBI. M. Sigaud has received reimbursement for attending symposia/congresses, honoraria for speaking or for consulting from Biomarin, CSL Behring, Novo Nordisk, Octapharma, Roche and Shire/Takeda. J. K. M. Wu received funding to attend meetings and has participated in Octapharma-funded clinical research. M. Jansen is a full-time employee of Octapharma GmbH, Vienna, Austria. L. Belyanskaya, O. Walter and S. Knaub are employees of Octapharma AG, Lachen, Switzerland. E. J. Neufeld has received honoraria and participated in advisory boards for Octapharma. He has been a consultant for Genentech and Pfizer, and has participated in advisory boards for Novo Nordisk, Kedrion, Genentech, Baxalta/Shire (now Takeda), Novartis and CSL-Behring during the course of the NuProtect study. He has served on data monitoring committees for Bayer, Acceleron Pharma and ApoPharma (now Chiesi), and received research funding from the American Thrombosis and Hemostasis Network (ATHN). L. Dubey, M. Gattens, P. Gresele, L. Kitanovski, S. Lohade, V. Vdovin and K. Vilchevska declare no competing financial interests., (The Author(s). This is an open access article published by Thieme under the terms of the Creative Commons Attribution License, permitting unrestricted use, distribution, and reproduction so long as the original work is properly cited. (https://creativecommons.org/licenses/by/4.0/).)

Published

2021

39. Ex Vivo Prediction of Comprehensive Coagulation Potential Using Simulated Blood Concentrations of Emicizumab in Patients with Acquired Hemophilia A.

Author

Takeyama M, Furukawa S, Yada K, Ogiwara K, Shimonishi N, Nakajima Y, Mizumachi K, Noguchi-Sasaki M, Shima M, and Nogami K

Subjects

Adult, Aged, Aged, 80 and over, Antibodies, Bispecific blood, Antibodies, Bispecific pharmacokinetics, Antibodies, Monoclonal, Humanized blood, Antibodies, Monoclonal, Humanized pharmacokinetics, Autoantibodies blood, Child, Coagulants blood, Coagulants pharmacokinetics, Drug Monitoring, Factor VIII immunology, Female, Hemophilia A blood, Hemophilia A immunology, Hemorrhage blood, Hemorrhage immunology, Humans, Male, Middle Aged, Thrombelastography, Young Adult, Antibodies, Bispecific administration & dosage, Antibodies, Monoclonal, Humanized administration & dosage, Blood Coagulation drug effects, Coagulants administration & dosage, Hemophilia A drug therapy, Hemorrhage prevention & control

Abstract

Introduction:  Emicizumab prophylaxis improves coagulation function in congenital hemophilia A, regardless of inhibitor presence. We recently reported that emicizumab enhanced the coagulant potentials, ex vivo, in plasmas from patients with acquired hemophilia A (PwAHAs) at diagnosis. However, coagulant effects of emicizumab in PwAHAs during the clinical course remain unclear., Aim:  To assess ex vivo coagulant effects of emicizumab in PwAHAs during the clinical course., Methods/results:  Blood samples were obtained from 14 PwAHAs on (median) days 0 and 6 during a severe-bleeding phase, and days 27 and 59 during a reduced-bleeding phase with elevated endogenous factor VIII (FVIII) and decreased inhibitor titers. If administered a single dose of 3 or 6 mg/kg, or two doses at 6 mg/kg followed by 3 mg/kg, estimated plasma emicizumab concentrations (10/5/2.5, 20/10/5, and 30/15/7.5 µg/mL on days 0-7/30/60, respectively) could be used to represent potential changes, based on the half-life ( T 1/2 : ∼30 days). Emicizumab concentrations that covered maximum plasma concentrations of each dosage were used for spiking on day 0. Ex vivo addition of estimated emicizumab to PwAHA's plasma containing endogenous FVIII and/or inhibitor, without and with recombinant (r)FVIIa administration during immunosuppressive therapy, increased the calculated Ad|min1| values, assessed by clot waveform analysis, and their coagulant potentials were below normal levels. Rotational thromboelastometry revealed that ex vivo emicizumab addition resulted in the further improvement of coagulant potentials in whole bloods when combined with rFVIIa administration., Conclusion:  Based on ex vivo and in vitro data, emicizumab has the potential to be effective in clinical situations for PwAHAs., Competing Interests: M.T., S.F., K.Y., K.O., N.S., Y.N., K.M., M.S., and K.N. have received research grants from Chugai Pharmaceutical Co., Ltd. (Chugai), and are engaged in clinical studies sponsored by Chugai. M.S. and K.N.-S. have received (consulting) honoraria from Chugai. M.N.-S. is an employee of Chugai. M.S. and K.N. are inventors of the patents relating to emicizumab., (Thieme. All rights reserved.)

Published

2021

40. Risk factors for antibody formation in children with hemophilia: methodological aspects and clinical characteristics of the HEMFIL cohort study.

Author

Jardim LL, Santana MP, Chaves DG, van der Bom J, and Rezende SM

Subjects

Brazil epidemiology, Factor VIII therapeutic use, Female, Hemophilia A epidemiology, Hemophilia A therapy, Hemophilia B epidemiology, Hemophilia B immunology, Hemophilia B therapy, Humans, Immune Tolerance, Infant, Male, Prospective Studies, Risk Factors, Antibodies, Neutralizing immunology, Antibody Formation, Factor VIII immunology, Hemophilia A immunology

Abstract

Up to 35% of patients with hemophilia A and 5% with hemophilia B develop neutralizing antibodies which can inhibit the therapeutic activity of factor replacement (inhibitors). Despite the clinical relevance of antifactor VIII and IX neutralizing antibodies, there is still a major gap on the knowledge of risk factors for their development. Furthermore, most of the studies on risk factors for inhibitor development come from Caucasian and Afro-American populations. The HEMFIL is a Brazilian prospective cohort study of previously untreated children with hemophilia, which primary aim is to identify new risk factors related to inhibitor development. This manuscript aims at describing the study design and its methodology. After the diagnosis, children are followed up to 75 exposure days or to inhibitor development. Standardized forms and blood samples are collected to describe clinical characteristics and to perform the measurement of immunological and genetic biomarkers at three time points; Inclusion time (T0), at inhibitor development or at 75 exposure days without inhibitors (T1) and after immune tolerance induction for patients in whom it is indicated and performed (T2). Currently, 120 children have been included, of whom, 95 have completed the follow-up. For severe/moderately severe hemophilia A, the cumulative incidence of inhibitors at 75 exposure days was 35% (95% confidence interval, 26-46%). The inclusion of additional patients and a longer follow-up will allow the analysis of risk factors for inhibitor development., (Copyright © 2021 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2021

41. Calibration-free concentration analysis for quantification of anti-drug specific antibodies in polyclonal positive control antibodies and in clinical samples.

Author

Aniol-Nielsen C, Toft-Hansen H, Dahlbäck M, Nielsen CH, and Solberg H

Subjects

Autoantibodies blood, Biomarkers blood, Diabetes Mellitus blood, Diabetes Mellitus drug therapy, Humans, Hypoglycemic Agents therapeutic use, Insulin, Long-Acting therapeutic use, Predictive Value of Tests, Reproducibility of Results, Antibodies, Neutralizing blood, Coagulants immunology, Diabetes Mellitus immunology, Factor VIII immunology, Hypoglycemic Agents immunology, Immunoglobulin G blood, Immunologic Techniques, Insulin, Long-Acting immunology, Surface Plasmon Resonance

Abstract

Highly sensitive assays for anti-drug antibodies (ADAs) are both a regulatory requirement and requisite for proper evaluation of the effects of immunogenicity on clinical efficacy and safety. Determination of ADA assay sensitivity depends on positive control antibodies to represent naturally occurring or treatment-induced ADA responses. An accurate determination of the proportion of drug-specific antibodies in these polyclonal positive control batches is critical for correct evaluation of assay sensitivity. Target purification of positive control antibodies is commonly applied but infers the risk to lose a proportion of the antibodies. This may lead to an incorrect estimate of the ADA assay sensitivity, especially if high-affinity antibodies are lost that may be representative of natural ADAs with clinical implication. The Surface Plasmon Resonance platform on the Biacore™ systems offers methods for real-time analysis of biomolecular interactions without introducing any modifications to the analysed material. Calibration-free concentration analysis (CFCA) is such an application for determination of the proportion of drug-specific antibodies, which allows direct determination of active antibody concentrations, as defined by the ligand, in a flow-based system. Here, we present a novel CFCA method for ADA quantification developed and validated using polyclonal positive control antibodies against endogenous human insulin, insulin degludec (Tresiba®) and turoctocog alfa (NovoEight®). We find that CFCA precisely and accurately measures concentrations of drug-specific IgG antibodies with a precision of ±10% and 90%-112% recovery of expected values of monoclonal positive control antibodies. Additionally, we have achieved a more accurate measure of the sensitivity of a cell-based bioassay for in vitro neutralising ADAs using the specific concentration determined with CFCA. Moreover, we effectively quantified serum anti-insulin antibodies in high-titre clinical samples from individuals with diabetes mellitus. This application extends the relevance of the CFCA technology to analysis of immunogenicity for accurate quantification of ADAs in both the polyclonal positive control and in clinical samples., (Copyright © 2021. Published by Elsevier B.V.)

Published

2021

42. CAR- and TRuC-redirected regulatory T cells differ in capacity to control adaptive immunity to FVIII.

Author

Rana J, Perry DJ, Kumar SRP, Muñoz-Melero M, Saboungi R, Brusko TM, and Biswas M

Subjects

Adaptive Immunity, Animals, CD28 Antigens genetics, CD3 Complex genetics, Disease Models, Animal, Hemophilia A genetics, Hemophilia A immunology, Humans, Interleukin-10 genetics, Male, Mice, Factor VIII immunology, Hemophilia A therapy, Mutation, Receptors, Chimeric Antigen metabolism, T-Lymphocytes, Regulatory immunology

Abstract

Regulatory T cells (Tregs) control immune responses in autoimmune disease, transplantation, and enable antigen-specific tolerance induction in protein-replacement therapies. Tregs can exert a broad array of suppressive functions through their T cell receptor (TCR) in a tissue-directed and antigen-specific manner. This capacity can now be harnessed for tolerance induction by "redirecting" polyclonal Tregs to overcome low inherent precursor frequencies and simultaneously augment suppressive functions. With the use of hemophilia A as a model, we sought to engineer antigen-specific Tregs to suppress antibody formation against the soluble therapeutic protein factor (F)VIII in a major histocompatibility complex (MHC)-independent fashion. Surprisingly, high-affinity chimeric antigen receptor (CAR)-Treg engagement induced a robust effector phenotype that was distinct from the activation signature observed for endogenous thymic Tregs, which resulted in the loss of suppressive activity. Targeted mutations in the CD3ζ or CD28 signaling motifs or interleukin (IL)-10 overexpression were not sufficient to restore tolerance. In contrast, complexing TCR-based signaling with single-chain variable fragment (scFv) recognition to generate TCR fusion construct (TRuC)-Tregs delivered controlled antigen-specific signaling via engagement of the entire TCR complex, thereby directing functional suppression of the FVIII-specific antibody response. These data suggest that cellular therapies employing engineered receptor Tregs will require regulation of activation thresholds to maintain optimal suppressive function., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

43. Predictors of the outcome of immune tolerance induction in patients with haemophilia A and inhibitors: The Brazilian Immune Tolerance (BrazIT) Study protocol.

Author

Camelo RM, Chaves DG, Zuccherato LW, and Rezende SM

Subjects

Biomarkers blood, Brazil epidemiology, Factor VIII immunology, Female, Hemophilia A blood, Hemophilia A genetics, Hemophilia A immunology, Humans, Immune Tolerance immunology, Male, Risk Factors, Antibodies, Bispecific administration & dosage, Antibodies, Monoclonal, Humanized administration & dosage, Factor VIII genetics, Hemophilia A drug therapy, Immune Tolerance drug effects

Abstract

The development of inhibitors is the main complication of haemophilia A (HA) treatment. Immune tolerance induction (ITI) is the treatment of choice for inhibitor eradication. We describe the methodology of the Brazilian Immune Tolerance Induction (BrazIT) Study, aimed to identify clinical, genetic, and immune biomarkers associated with response to ITI and inhibitor recurrence. This cohort study includes people with HA (PwHA) and inhibitors (a) who require bypassing agents to treat and/or prevent bleeding, and (b) who are at any stage of ITI treatment. Patients are included in each haemophilia treatment centre (HTC). Factor VIII (FVIII) and inhibitor assessments are performed at local laboratories of each HTC. The ITI regimen followed the national protocol of the Brazilian Ministry of Health. All PwHA starts with low-dose ITI (50 IU/kg three times weekly); high-dose regimen (100 IU/kg daily) is used if there is lack of response to the low-dose ITI. Outcomes are classified as total or partial success, and failure. Standardized case report forms with clinical, laboratory, and treatment data are collected from medical files and interviews. Blood samples are collected for genetic and immune biomarkers at the time of inclusion in the study and at the end of ITI. The study is ongoing and, currently, 202/250 (80.8%) PwHA from 15 HTCs have been included. BrazIT Study is the largest cohort of PwHA and inhibitor under treatment with the same ITI regimen reported to date. This study is likely to contribute with novel predictors of ITI response., Competing Interests: RMC has received speaker/consultant fees and scientific event grants from Hoffman-La Roche and Takeda. DGC and LWZ have no conflicts of interest to declare. SMR works as an advisor to the Brazilian Program of Inherited Bleeding Disorders (Brazilian Ministry of Health) and received consultancy fees from the Brazilian Ministry of Health. This does not alter our adherence to all PLOS ONE policies on sharing data and materials. After the publication of the final analysis, the data can be shared upon request and guarantee of the confidentiality of each participant. Furthermore, this must adhere to the rules of the Brazilian ethical resolutions for the development of research with human beings.

Published

2021

44. Measurement of antifactor VIII antibody titre in the presence of emicizumab; Use of chromogenic Bethesda assays.

Author

Bowyer A, Kitchen S, and Maclean R

Subjects

Antibodies, Bispecific pharmacokinetics, Antibodies, Bispecific therapeutic use, Antibodies, Monoclonal, Humanized pharmacokinetics, Antibodies, Monoclonal, Humanized therapeutic use, Hemophilia A diagnosis, Hemophilia A drug therapy, Humans, Antibodies immunology, Blood Coagulation Tests methods, Factor VIII antagonists & inhibitors, Factor VIII immunology, Hemophilia A blood, Hemophilia A immunology

Published

2021

45. Structure of Blood Coagulation Factor VIII in Complex With an Anti-C2 Domain Non-Classical, Pathogenic Antibody Inhibitor.

Author

Ronayne EK, Peters SC, Gish JS, Wilson C, Spencer HT, Doering CB, Lollar P, Spiegel PC Jr, and Childers KC

Subjects

Animals, Antibodies, Monoclonal, Murine-Derived immunology, Crystallography, X-Ray, Factor VIII immunology, Hemophilia A blood, Hemophilia A immunology, Humans, Mice, Molecular Dynamics Simulation, Protein Conformation, Protein Engineering, Protein Interaction Domains and Motifs, Protein Structure, Quaternary, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins immunology, Swine, Antibodies, Monoclonal, Murine-Derived chemistry, Factor VIII antagonists & inhibitors, Factor VIII chemistry

Abstract

Factor VIII (fVIII) is a procoagulant protein that binds to activated factor IX (fIXa) on platelet surfaces to form the intrinsic tenase complex. Due to the high immunogenicity of fVIII, generation of antibody inhibitors is a common occurrence in patients during hemophilia A treatment and spontaneously occurs in acquired hemophilia A patients. Non-classical antibody inhibitors, which block fVIII activation by thrombin and formation of the tenase complex, are the most common anti-C2 domain pathogenic inhibitors in hemophilia A murine models and have been identified in patient plasmas. In this study, we report on the X-ray crystal structure of a B domain-deleted bioengineered fVIII bound to the non-classical antibody inhibitor, G99. While binding to G99 does not disrupt the overall domain architecture of fVIII, the C2 domain undergoes an ~8 Å translocation that is concomitant with breaking multiple domain-domain interactions. Analysis of normalized B-factor values revealed several solvent-exposed loops in the C1 and C2 domains which experience a decrease in thermal motion in the presence of inhibitory antibodies. These results enhance our understanding on the structural nature of binding non-classical inhibitors and provide a structural dynamics-based rationale for cooperativity between anti-C1 and anti-C2 domain inhibitors., Competing Interests: PL is inventor on a patent application describing ET3i and is an inventor on patents owned by Emory University claiming compositions of matter that include modified fVIII proteins with reduced reactivity with anti-fVIII antibodies. CD, PL and HS are cofounders of Expression Therapeutics and own equity in the company. Expression Therapeutics owns the intellectual property associated with ET3i. The terms of this arrangement have been reviewed and approved by Emory University in accordance with its conflict of interest policies. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Ronayne, Peters, Gish, Wilson, Spencer, Doering, Lollar, Spiegel and Childers.)

Published

2021

46. Structure of blood coagulation factor VIII in complex with an anti-C1 domain pathogenic antibody inhibitor.

Author

Gish JS, Jarvis L, Childers KC, Peters SC, Garrels CS, Smith IW, Spencer HT, Doering CB, Lollar P, and Spiegel PC

Subjects

Animals, Antibodies, Monoclonal immunology, Antibodies, Monoclonal metabolism, Crystallography, X-Ray, Epitopes chemistry, Epitopes immunology, Factor VIII genetics, Factor VIII immunology, Factor VIII metabolism, Hemophilia A genetics, Humans, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments metabolism, Mice, Models, Molecular, Protein Conformation, Protein Domains immunology, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins immunology, Recombinant Fusion Proteins metabolism, Swine, Antibodies, Monoclonal chemistry, Antigen-Antibody Complex chemistry, Factor VIII chemistry, Recombinant Fusion Proteins chemistry

Abstract

Antibody inhibitor development in hemophilia A represents the most significant complication resulting from factor VIII (fVIII) replacement therapy. Recent studies have demonstrated that epitopes present in the C1 domain contribute to a pathogenic inhibitor response. In this study, we report the structure of a group A anti-C1 domain inhibitor, termed 2A9, in complex with a B domain-deleted, bioengineered fVIII construct (ET3i). The 2A9 epitope forms direct contacts to the C1 domain at 3 different surface loops consisting of Lys2065-Trp2070, Arg2150-Tyr2156, and Lys2110-Trp2112. Additional contacts are observed between 2A9 and the A3 domain, including the Phe1743-Tyr1748 loop and the N-linked glycosylation at Asn1810. Most of the C1 domain loops in the 2A9 epitope also represent a putative interface between fVIII and von Willebrand factor. Lastly, the C2 domain in the ET3i:2A9 complex adopts a large, novel conformational change, translocating outward from the structure of fVIII by 20 Å. This study reports the first structure of an anti-C1 domain antibody inhibitor and the first fVIII:inhibitor complex with a therapeutically active fVIII construct. Further structural understanding of fVIII immunogenicity may result in the development of more effective and safe fVIII replacement therapies., (© 2021 by The American Society of Hematology.)

Published

2021

47. Spectrum of F8 Genotype and Genetic Impact on Inhibitor Development in Patients with Hemophilia A from Multicenter Cohort Studies (J-HIS) in Japan.

Author

Shinozawa K, Yada K, Kojima T, Nogami K, Taki M, Fukutake K, Yoshioka A, Shirahata A, and Shima M

Subjects

Adolescent, Adult, Antibody Formation genetics, Child, Child, Preschool, Cohort Studies, Factor VIII immunology, Factor VIII therapeutic use, Female, Genetic Association Studies, Genetic Variation, Hemophilia A therapy, Humans, Isoantibodies metabolism, Japan, Male, Retrospective Studies, Risk, Young Adult, Factor VIII genetics, Genotype, Hemophilia A genetics, Isoantibodies genetics, Mutation genetics

Abstract

Some genetic and treatment-related factors are risk factors for inhibitor development in patients with hemophilia A (PwHA). However, the genotype distribution of the factor VIII gene ( F8 ) and genetic impact on inhibitor development in Japanese PwHA remain unknown. In 2007, the Japan Hemophilia Inhibitor Study 2 (J-HIS2) was organized to establish a nationwide registry system for hemophiliacs and to elucidate risk factors for inhibitor development, designed for prospective investigation following a retrospective study (J-HIS1) which had already finished. Patients, newly diagnosed after January 2007, were enrolled in J-HIS2 and followed up for inhibitor development and clinical environments since 2008 onward. In the present study, F8 genotypes of PwHA were investigated in the patients recruited from the J-HIS2 cohort as well as those with inhibitor from the J-HIS1 cohort. F8 variants identified in 59 PwHA with inhibitor in J-HIS1 were: 20 intron-22 inversions, 5 intron-1 inversions, 9 large deletions, 4 nonsense, 8 missense, 11 small in/del, and 2 splice-site variants. F8 variants identified in 267 (67 with inhibitor) PwHA in J-HIS2 were: 76(28) intron-22 inversions, 3(2) intron-1 inversion, 1(0) duplication, 8(5) large deletions, 21(7) nonsense, 109(7) missense, 40(11) small in/del, and 9(7) splice-site variants. Forty variants were novel. The cumulative inhibitor incidence rate in the severe group with null changes was 42.4% (95% confidence interval [CI]: 33.7-50.8), higher than that with nonnull changes (15.6% [95%CI: 6.8-27.8]), in J-HIS2. Relative risk for inhibitor development of null changes was 2.89. The spectrum of F8 genotype and genetic impact on inhibitor development in Japanese PwHA were consistent with the previous reports., Competing Interests: K.S. was an endowed assistant professor funded by CSL Behring. K.Y. teaches a course endowed by Takeda Co. Ltd. T.K. received research funding from Chugai Pharmaceutical Co., Ltd. and Bayer AG, and a lecture reward from Chugai Pharmaceutical Co., Ltd., Takeda Co. Ltd., Novo Nordisk A/S, Sanofi S.A., Bayer A/G, and Sysmex Corporation. K.N. has received grants from Takeda Co. Ltd. and Sanofi S.A., and research funding from Chugai Pharmaceutical Co., Ltd., F. Hoffmann-La Roche Ltd., Bayer A/G, Novo Nordisk A/S, KM Biologics, and also honoraria from Takeda Co. Ltd., Bayer A/G, Novo Nordisk A/S, Sanofi S.A., CSL Behring, Chugai Pharmaceutical Co., Ltd., F. Hoffmann-La Roche Ltd. outside the submitted work. M.T. has received research funding from Chugai Pharmaceutical Co., Ltd., F. Hoffmann-La Roche Ltd., Sanofi S.A., CSL Behring, and Novo Nordisk A/S and also honoraria from Chugai Pharmaceutical Co., Ltd., CSL Behring, Bayer AG, Takeda Co. Ltd., Sanofi S.A., and Novo Nordisk A/S outside the submitted work and listed as an entity's board of directors or advisory committee member for Chugai Pharmaceutical Co., Ltd., Novo Nordisk A/S, Sanofi S.A., and Bayer AG. K.F. has received grants and personal fees from Takeda Co. Ltd. (Baxalta/Shire), Bayer, Pfizer, CSL Behring, Novo Nordisk, Sanofi S.A. (Biogen/Bioverativ), KM Biologics (Kaketsuken) and Chugai Pharmaceutical Co. LTD, and grants from Japan Blood Products Organization, personal fees from SRL Inc., LSI Medience, Roche Diagnostics, Siemens, Sekisui Medical, Fujirebio Inc., Torii Pharmaceuticals, Octapharma, Sysmex, MSD, and other from CIMIC, outside the submitted work. A.Y. has received payment for a manuscript and consulting fee from Japan Blood Products Organization, and honoraria for lectures from Takeda Co., Ltd., Bayer A/G, and Chugai Pharmaceutical Co., Ltd. A.S. has no conflict of interest. M.S. received research funding from Chugai Pharmaceutical Co., Ltd., F. Hoffmann-La Roche Ltd., Sanofi S.A., Takeda Co. Ltd., CSL Behring, KM Biologics Co., Ltd., and Novo Nordisk A/S; and consulting fee from Chugai Pharmaceutical Co., Ltd.; and payment for lectures on speaker's bureau from Chugai Pharmaceutical Co., Ltd., Sanofi S.A., Bayer AG, and Sysmex corporation; and is listed as an entity's board of directors or advisory committee member for Chugai Pharmaceutical Co., Ltd., F. Hoffmann-La Roche Ltd., BioMarin Pharmaceutical Inc., Bayer AG, and Sanofi S.A.; and is an inventor of patents related to anti-FIXa/FX bispecific antibodies., (Thieme. All rights reserved.)

Published

2021

48. IVIg increases interleukin-11 levels, which in turn contribute to increased platelets, VWF and FVIII in mice and humans.

Author

Nguyen A, Repesse Y, Ebbo M, Allenbach Y, Benveniste O, Vallat JM, Magy L, Deshayes S, Maigné G, de Boysson H, Karnam A, Delignat S, Lacroix-Desmazes S, Bayry J, and Aouba A

Subjects

Animals, Female, Humans, Male, Mice, Mice, Inbred C57BL, Middle Aged, Retrospective Studies, Blood Platelets immunology, Factor VIII immunology, Immunoglobulins, Intravenous immunology, Interleukin-11 immunology, von Willebrand Factor immunology

Abstract

The mechanisms of action of intravenous immunoglobulins (IVIg) in autoimmune diseases are not fully understood. The fixed duration of efficacy and noncumulative effects of IVIg in immune thrombocytopenia (ITP) and acquired von Willebrand disease (AVWD) suggest other mechanisms besides immunological ones. Additionally to the peripheral destruction of platelets in ITP, their medullary hypoproduction emerged as a new paradigm with rescue of thrombopoietin receptor agonists (TPO-RA). In an ITP mouse model, interleukin (IL)-11 blood levels increase following IVIg. IL-11 stimulates the production of platelets and other haemostasis factors; recombinant IL-11 (rIL-11) is thus used as a growth factor in post-chemotherapy thrombocytopenia. We therefore hypothesized that IVIg induces IL-11 over-production, which increases platelets, VWF and factor VIII (FVIII) levels in humans and mice. First, in an ITP mouse model, we show that IVIg or rIL-11 induces a rapid increase (72 h) in platelets, FVIII and VWF levels, whereas anti-IL-11 antibody greatly decreased this effect. Secondly, we quantify for the first time in patients with ITP, AVWD, inflammatory myopathies or Guillain-Barré syndrome the dramatic IL-11 increase following IVIg, regardless of the disease. As observed in mice, platelets, VWF and FVIII levels increased following IVIg. The late evolution (4 weeks) of post-IVIg IL-11 levels overlapped with those of VWF and platelets. These data may explain thrombotic events following IVIg and open perspectives to monitor post-IVIg IL-11/thrombopoietin ratios, and to assess rIL-11 use with or without TPO-RA as megakaryopoiesis co-stimulating factors to overcome the relative hypoproduction of platelets or VWF in corresponding autoimmune diseases, besides immunosuppressant., (© 2021 British Society for Immunology.)

Published

2021

49. Acquired hemophilia A associated with Epstein-Barr-virus-associated T/natural killer-cell lymphoproliferative disease: A case report.

Author

Yamamoto M, Shindo M, Sumi C, Igarashi S, Saito T, Tsukada N, Toki Y, Hatayama M, Inamura J, Sato K, Mizukami Y, Torimoto Y, and Okumura T

Subjects

Aged, Autoantibodies immunology, DNA, Viral isolation & purification, Epstein-Barr Virus Infections complications, Epstein-Barr Virus Infections immunology, Epstein-Barr Virus Infections virology, Factor VIII immunology, Hemophilia A blood, Hemophilia A immunology, Hemophilia A virology, Herpesvirus 4, Human genetics, Herpesvirus 4, Human isolation & purification, Humans, Lymph Nodes, Lymphoproliferative Disorders complications, Lymphoproliferative Disorders immunology, Lymphoproliferative Disorders virology, Male, Partial Thromboplastin Time, Prednisolone therapeutic use, Treatment Outcome, Epstein-Barr Virus Infections diagnosis, Hemophilia A diagnosis, Killer Cells, Natural immunology, Lymphoproliferative Disorders diagnosis, T-Lymphocytes immunology

Abstract

Introduction: Acquired hemophilia A (AHA) is a rare bleeding disorder caused by autoantibodies against factor VIII (FVIII). Hematological malignancies, especially lymphoid malignancies, are known to be underlying causes of AHA; however, thus far, there is no report of AHA associated with Epstein-Barr-virus-associated T/natural killer-cell lymphoproliferative disease (EBV-T/NK-LPD). Here, we present a case of AHA that developed during treatment for EBV-T/NK-LPD., History: A 69-year-old man visited our hospital because of general fatigue. Blood examination showed pancytopenia, and computed tomography revealed whole-body lymphadenopathy, but there were no findings indicating hematological malignancy from bone marrow aspiration and cervical lymph node biopsy. The level of EBV DNA in peripheral blood was extremely high, and he was diagnosed with EBV-T/NK-LPD. EBV-T/NK-LPD improved with prednisolone (PSL) administration. Seventeen months after starting treatment, the patient complained of back and right leg pain. At that time, he had been treated with low-dose PSL, and EBV-T/NK-LPD was well controlled. Imaging revealed hematoma of the right iliopsoas muscle. Prolonged activated partial thromboplastin time (APTT) was the only abnormal finding in a screening coagulation test. FVIII coagulant activity was below detection limit, and FVIII inhibitor level was increased. From these results, he was diagnosed with AHA.A higher dose of PSL was administered, and, after 1 month of treatment, FVIII activity gradually increased, and FVIII inhibitor level became undetectable. APTT also normalized, and complete remission was achieved and maintained for 13 months with low-dose PSL. During treatment, EBV-T/NK-LPD was well controlled., Conclusion: It is speculated that proliferating lymphocytes interfere with normal immune functions and that abnormal autoantibodies are produced from those lymphocytes in patients with LPD. Therefore, we speculate that EBV-infected and proliferating monoclonal NK cells might have modulated the immune system and produced autoantibodies against FVIII, thus causing AHA in this patient with EBV-T/NK-LPD., Competing Interests: The authors have no funding and conflicts of interests to disclose., (Copyright © 2021 the Author(s). Published by Wolters Kluwer Health, Inc.)

Published

2021

50. B cell-activating factor modulates the factor VIII immune response in hemophilia A.

Author

Doshi BS, Rana J, Castaman G, Shaheen MA, Kaczmarek R, Butterfield JS, Meeks SL, Leissinger C, Biswas M, and Arruda VR

Subjects

Adolescent, Adult, Animals, Antibodies immunology, Antibodies pharmacology, B-Cell Activating Factor genetics, Blood Coagulation Factor Inhibitors genetics, Child, Child, Preschool, Factor VIII antagonists & inhibitors, Factor VIII genetics, Factor VIII therapeutic use, Female, HEK293 Cells, Hemophilia A drug therapy, Hemophilia A genetics, Humans, Immune Tolerance drug effects, Infant, Male, Mice, Mice, Inbred BALB C, Mice, Knockout, Middle Aged, B-Cell Activating Factor immunology, Blood Coagulation Factor Inhibitors immunology, Factor VIII immunology, Hemophilia A immunology

Abstract

Inhibitors of factor VIII (FVIII) remain the most challenging complication of FVIII protein replacement therapy in hemophilia A (HA). Understanding the mechanisms that guide FVIII-specific B cell development could help identify therapeutic targets. The B cell-activating factor (BAFF) cytokine family is a key regulator of B cell differentiation in normal homeostasis and immune disorders. Thus, we used patient samples and mouse models to investigate the potential role of BAFF in modulating FVIII inhibitors. BAFF levels were elevated in pediatric and adult HA inhibitor patients and decreased to levels similar to those of noninhibitor controls after successful immune tolerance induction (ITI). Moreover, elevations in BAFF levels were seen in patients who failed to achieve FVIII tolerance with anti-CD20 antibody-mediated B cell depletion. In naive HA mice, prophylactic anti-BAFF antibody therapy prior to FVIII immunization prevented inhibitor formation and this tolerance was maintained despite FVIII exposure after immune reconstitution. In preimmunized HA mice, combination therapy with anti-CD20 and anti-BAFF antibodies dramatically reduced FVIII inhibitors via inhibition of FVIII-specific plasma cells. Our data suggest that BAFF may regulate the generation and maintenance of FVIII inhibitors and/or anti-FVIII B cells. Finally, anti-CD20/anti-BAFF combination therapy may be clinically useful for ITI.

Published

2021