Your search keyword '"Hemophilia A metabolism"' showing total 385 results

1. Biomarkers Involved in the Pathogenesis of Hemophilic Arthropathy.

Author

Badulescu OV, Scripcariu DV, Badescu MC, Ciocoiu M, Vladeanu MC, Plesoianu CE, Bojan A, Iliescu-Halitchi D, Tudor R, Huzum B, Frasinariu OE, and Bararu-Bojan I

Subjects

Humans, Hemarthrosis metabolism, Hemarthrosis etiology, Hemarthrosis pathology, Joint Diseases metabolism, Joint Diseases pathology, Joint Diseases etiology, Cartilage, Articular metabolism, Cartilage, Articular pathology, Synovial Membrane metabolism, Synovial Membrane pathology, Biomarkers, Hemophilia A complications, Hemophilia A metabolism, Hemophilia A pathology

Abstract

Hemophilia, which is a rare disease, results from congenital deficiencies of coagulation factors VIII and IX, respectively, leading to spontaneous bleeding into joints, resulting in hemophilic arthropathy (HA). HA involves complex processes, including synovial proliferation, angiogenesis, and tissue remodeling. Despite ongoing research, factors contributing to HA progression, especially in adults with severe HA experiencing joint pain, remain unclear. Blood markers, particularly collagen-related ones, have been explored to assess joint health in hemophilia. For example, markers like CTX-I and CTX-II reflect bone and cartilage turnover, respectively. Studies indicate elevated levels of certain markers post-bleeding episodes, suggesting joint health changes. However, longitudinal studies on collagen turnover and basement membrane or endothelial cell markers in relation to joint outcomes, particularly during painful episodes, are scarce. Given the role of the CX3CL1/CX3XR1 axis in arthritis, other studies investigate its involvement in HA. The importance of different inflammatory and bone damage biomarkers should be assessed, alongside articular cartilage and synovial membrane morphology, aiming to enhance understanding of hemophilic arthropathy progression.

Published

2024

2. Aberrant methylation and expression of TNXB promote chondrocyte apoptosis and extracullar matrix degradation in hemophilic arthropathy via AKT signaling.

Author

Chen J, Zeng Q, Wang X, Xu R, Wang W, Huang Y, Sun Q, Yuan W, Wang P, Chen D, Tong P, and Jin H

Subjects

Animals, Humans, Mice, Cartilage, Articular metabolism, Cartilage, Articular pathology, Extracellular Matrix metabolism, Osteoarthritis metabolism, Osteoarthritis genetics, Osteoarthritis pathology, Apoptosis, Chondrocytes metabolism, Chondrocytes pathology, DNA Methylation, Hemophilia A metabolism, Hemophilia A genetics, Hemophilia A complications, Proto-Oncogene Proteins c-akt metabolism, Proto-Oncogene Proteins c-akt genetics, Signal Transduction, Tenascin metabolism, Tenascin genetics

Abstract

Recurrent joint bleeding in hemophilia patients frequently causes hemophilic arthropathy (HA). Drastic degradation of cartilage is a major characteristic of HA, but its pathological mechanisms has not yet been clarified. In HA cartilages, we found server matrix degradation and increased expression of DNA methyltransferase proteins. We thus performed genome-wide DNA methylation analysis on human HA (N=5) and osteoarthritis (OA) (N=5) articular cartilages, and identified 1228 differentially methylated regions (DMRs) associated with HA. Functional enrichment analyses revealed the association between DMR genes (DMGs) and extracellular matrix (ECM) organization. Among these DMGs, Tenascin XB (TNXB) expression was down-regulated in human and mouse HA cartilages. The loss of Tnxb in F8 -/- mouse cartilage provided a disease-promoting role in HA by augmenting cartilage degeneration and subchondral bone loss. Tnxb knockdown also promoted chondrocyte apoptosis and inhibited phosphorylation of AKT. Importantly, AKT agonist showed chondroprotective effects following Tnxb knockdown. Together, our findings indicate that exposure of cartilage to blood leads to alterations in DNA methylation, which is functionally related to ECM homeostasis, and further demonstrate a critical role of TNXB in HA cartilage degeneration by activating AKT signaling. These mechanistic insights allow development of potentially new strategies for HA cartilage protection., Competing Interests: JC, QZ, XW, RX, WW, YH, QS, WY, PW, PT, HJ No competing interests declared, DC Reviewing editor, eLife, (© 2024, Chen, Zeng et al.)

Published

2024

3. Frequency of natural regulatory T cells specific for factor VIII in the peripheral blood of healthy donors.

Author

Menier C, Meunier S, Porcheddu V, Romano L, Correia E, Busato F, Tost J, and Maillère B

Subjects

Humans, T-Lymphocytes, Regulatory, Autoantibodies, Forkhead Transcription Factors metabolism, Factor VIII metabolism, Hemophilia A metabolism

Abstract

Tolerance to self-proteins involves multiple mechanisms, including conventional CD4 + T-cell (Tconv) deletion in the thymus and the recruitment of natural regulatory T cells (nTregs). The significant incidence of autoantibodies specific for the blood coagulation factor VIII (FVIII) in healthy donors illustrates that tolerance to self-proteins is not always complete. In contrast to FVIII-specific Tconvs, FVIII-specific nTregs have never been revealed and characterized. To determine the frequency of FVIII-specific Tregs in human peripheral blood, we assessed the specificity of in vitro expanded Tregs by the membrane expression of the CD137 activation marker. Amplified Tregs maintain high levels of FOXP3 expression and exhibit almost complete demethylation of the FOXP3 Treg-specific demethylated region. The cells retained FOXP3 expression after long-term culture in vitro, strongly suggesting that FVIII-specific Tregs are derived from the thymus. From eleven healthy donors, we estimated the frequencies of FVIII-specific Tregs at 0.17 cells per million, which is about 10-fold lower than the frequency of FVIII-specific CD4 + T cells we previously published. Our results shed light on the mechanisms of FVIII tolerance by a renewed approach that could be extended to other self- or non-self-antigens., (© 2024 The Authors. European Journal of Immunology published by Wiley‐VCH GmbH.)

Published

2024

4. Cellular stress and coagulation factor production: when more is not necessarily better.

Author

Chen Z, Herzog RW, and Kaufman RJ

Subjects

Animals, Humans, Factor VIII metabolism, Blood Coagulation Factors genetics, Genetic Therapy, Mammals genetics, Mammals metabolism, Hemophilia A genetics, Hemophilia A therapy, Hemophilia A metabolism, Hemophilia B therapy, Hemophilia B drug therapy

Abstract

Remarkably, it has been 40 years since the isolation of the 2 genes involved in hemophilia A (HA) and hemophilia B (HB), encoding clotting factor (F) VIII (FVIII) and FIX, respectively. Over the years, these advances led to the development of purified recombinant protein factors that are free of contaminating viruses from human pooled plasma for hemophilia treatments, reducing the morbidity and mortality previously associated with human plasma-derived clotting factors. These discoveries also paved the way for modified factors that have increased plasma half-lives. Importantly, more recent advances have led to the development and Food and Drug Administration approval of a hepatocyte-targeted, adeno-associated viral vector-mediated gene transfer approach for HA and HB. However, major concerns regarding the durability and safety of HA gene therapy remain to be resolved. Compared with FIX, FVIII is a much larger protein that is prone to misfolding and aggregation in the endoplasmic reticulum and is poorly secreted by the mammalian cells. Due to the constraint of the packaging capacity of adeno-associated viral vector, B-domain deleted FVIII rather than the full-length protein is used for HA gene therapy. Like full-length FVIII, B-domain deleted FVIII misfolds and is inefficiently secreted. Its expression in hepatocytes activates the cellular unfolded protein response, which is deleterious for hepatocyte function and survival and has the potential to drive hepatocellular carcinoma. This review is focused on our current understanding of factors limiting FVIII secretion and the potential pathophysiological consequences upon expression in hepatocytes., Competing Interests: Declaration of competing interests R.J.K. is a consultant for Miltenil Biotech. R.W.H. is serving on the scientific advisory boards and committees of Regeneron Pharmaceuticals, Pfizer, BioMarin, Spark Therapeutics, and Prevail Therapeutics and has received grant support from Hoffman-La Roche. Z.C. has no conflict of interest to disclose., (Copyright © 2023 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2023

5. Targeted delivery of miR125a-5p and human Factor VIII attenuates molecular mediators of hemophilic arthropathy.

Author

Senthilkumar MB, Sarangi P, Amit S, Senguttuvan S, Kumar N, and Jayandharan GR

Subjects

Humans, Mice, Animals, Factor VIII genetics, Factor VIII therapeutic use, Factor VIII metabolism, TNF Receptor-Associated Factor 6 metabolism, Disease Models, Animal, Joint Diseases genetics, Hemophilia A complications, Hemophilia A genetics, Hemophilia A metabolism

Abstract

Hemophilic arthropathy (HA) due to repeated bleeding into the joint cavity is a major cause of morbidity in patients with hemophilia. The molecular mechanisms contributing to this condition are not well characterized. MicroRNAs (miRs) are known to modulate the phenotype of multiple joint diseases such as osteoarthritis (OA) and rheumatoid arthritis (RA). Since miR125a is known to modulate disease progression in OA and RA, we performed a targeted screen of miR125a-5p and its target genes in a murine model of chronic HA. A digital PCR analysis demonstrated significant downregulation of miR125a-5p (2-fold vs control joint). Further molecular evaluation revealed elevated expression of the immunological markers STAT1 (7.6-fold vs control joint) and TRAF6 (10.6 fold vs control joint), which are direct targets of miR125a-5p. We then studied the impact of targeted overexpression of miR125a-5p using an Adeno-associated virus (AAV) vector in modulating the molecular mediators of HA. AAV5-miR125a vectors were administered intra-articularly either alone or in combination with a low dose of AAV8-based human factor 8 (F8) gene in a murine model of HA. We observed significantly increased expression of miR125a-5p in AAV5-miR125a administered mice (~12 fold vs injured joint) or in combination with AAV8-F8 vectors (~44 fold vs injured joint). The activity assay revealed ~17 %-20 % FVIII levels in mice that received low dose liver-directed F8 gene therapy. Further immunohistochemical analysis, demonstrated a decrease in inflammatory markers (STAT1 and TRAF6) and cartilage-degrading matrix metalloproteinases (MMPs) 3, 9, 13 in the joints of treated animals. These data highlight the crucial role of miR125a-5p in the development of HA., Competing Interests: Declaration of competing interest MK, PS, NK, GRJ have applied for patents on AAV technology for gene therapy and few technologies have been licensed., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

6. Augmented Degradation of Factors VIII and IX in the Intermittent Movement State.

Author

Cohen H, Keren-Politansky A, Crispel Y, Yanovich C, Asayag K, and Nadir Y

Subjects

Animals, Mice, Factor VIII metabolism, Factor IX metabolism, Thrombin, Hemorrhage, Hemostatics, Hemophilia A metabolism

Abstract

The most common clinical presentation of hemophilia A and hemophilia B is bleeding in large joints and striated muscles. It is unclear why bleeding has a predilection to affect joints and muscles. As muscles and joints are involved in intermittent movement, we explored whether this phenomenon could be associated with an impact on factor VIII and IX levels. Purified proteins and a mouse model were assessed using coagulation assays, Western blot analysis and immuno-staining. Movement caused an increase in thrombin activity and a decrease in factor VIII and factor IX activity. The decrease in factor VIII activity was more significant in the presence of thrombin and during movement. Under movement condition, sodium ions appeared to enhance the activity of thrombin that resulted in decreased factor VIII activity. Unlike factor VIII, the reduction in factor IX levels in the movement condition was thrombin-independent. High factor VIII levels were found to protect factor IX from degradation and vice versa. In mice that were in movement, factor VIII and IX levels decreased in the microcirculation of the muscle tissue compared with other tissues and to the muscle tissue at rest. Movement had no effect on von Willebrand factor levels. Movement induces reduction in factor VIII and IX levels. It enables an increase in the binding of sodium ions to thrombin leading to enhanced thrombin activity and augmented degradation of factor VIII. These data suggest a potential mechanism underlying the tendency of hemophilia patients to bleed in muscles and joints.

Published

2023

7. Delivery of Cas9-guided ABE8e into stem cells using poly(l-lysine) polypeptides for correction of the hemophilia-associated FIX missense mutation.

Author

Rong L, Chen D, Huang X, and Sun L

Subjects

Aminohydrolases genetics, Blood Coagulation Factors genetics, Blood Coagulation Factors metabolism, CRISPR-Cas Systems genetics, Deoxyribonuclease I metabolism, HEK293 Cells, Humans, Mutation, Mutation, Missense, Polylysine chemistry, Stem Cells metabolism, Gene Editing methods, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia B genetics, Hemophilia B therapy

Abstract

The coagulation factor 9 gene (FIX) point mutation contributes to most hemophilia B cases, providing ideal gene correction models. Here we identified the frequent mutation G20519A (R226Q) in FIX, which resulted in many severe and moderate hemophilia B patients. This study aimed to investigate the effect of HDR and base editing in correcting FIX mutant. We first constructed HEK293 and liver-derived cell lines Huh7 cells stabling carrying mutated FIX containing G20519A (HEK293-FIXmut and Huh7-FIXmut). Then, CRISPR/Cas9-based homology-directed repair (HDR) and base editing were used for the correction of this mutated point. We used Cas9 nickase (nCas9) mediated HDR and the advanced base editor ABE8e to correct G20519A and then measured the concentration and activity of FIX. Furthermore, we used the star-shaped poly(lysine) gene nanocarriers to deliver the ABE8e correction systems into HEK293-FIXmut and Huh7-FIXmut stem cells to correct mutated FIX. As a result, we found that gRNAs directed inefficient HDR in correcting G20519A. The ABE8e corrected the mutation efficiently in both HEK293-FIXmut and Huh7-FIXmut stem cells. In addition, the star-shaped poly(lysine) carriers delivered non-viral vectors into stem cells efficiently. The nanocarriers-delivered ABE8e system corrected mutated FIX in stem cells, and the stem cells secreted active FIX in high concentration. In conclusion, our study provides a potential alternative for correcting mutated FIX in hemophilia B patients., Competing Interests: Declaration of competing interest The authors have no conflicts of interest to declare., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

8. Intraosseous delivery of platelet-targeted factor VIII lentiviral vector in humanized NBSGW mice.

Author

Joo JH, Wang X, Singh S, Chen CY, Li C, Adair JE, Kiem HP, Rawlings DJ, and Miao CH

Subjects

Animals, Humans, Mice, Blood Platelets metabolism, Factor VIII metabolism, Genetic Therapy methods, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy, Hemostatics

Abstract

We previously showed that intraosseous (IO) delivery of factor VIII (FVIII, gene F8) lentiviral vector (LV) driven by the megakaryocyte-specific promoter Gp1bα (G-F8-LV) partially corrected the bleeding phenotype in hemophilia A (HemA) mice for up to 5 months. In this study, we further characterized and confirmed the successful transduction of self-regenerating hematopoietic stem and progenitor cells (HSPCs) in treated mice. In addition, secondary transplant of HSPCs isolated from G-F8-LV-treated mice corrected the bleeding phenotype of the recipient HemA mice, indicating the potential of long-term transgene expression following IO-LV therapy. To facilitate the translation of this technology to human applications, we evaluated the safety and efficacy of this gene transfer therapy into human HSPCs. In vitro transduction of human HSPCs by the platelet-targeted G-F8-LV confirmed megakaryocyte-specific gene expression after preferential differentiation of HSPCs to megakaryocyte lineages. Lentiviral integration analysis detected a polyclonal integration pattern in G-F8-LV-transduced human cells, profiling the clinical safety of hemophilia treatment. Most importantly, IO delivery of G-F8-LV to humanized NBSGW mice produced persistent FVIII expression in human platelets after gene therapy, and the megakaryocytes differentiated from human CD34+ HSPCs isolated from LV-treated humanized mice showed up to 10.2% FVIII expression, indicating efficient transduction of self-regenerating human HSPCs. Collectively, these results indicate the long-term safety and efficacy of the IO-LV gene therapy strategy for HemA in a humanized model, adding further evidence to the feasibility of translating this method for clinical applications., (© 2022 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

2022

9. In Vitro Conditioning of Adipose-Derived Mesenchymal Stem Cells by the Endothelial Microenvironment: Modeling Cell Responsiveness towards Non-Genetic Correction of Haemophilia A.

Author

Barbon S, Stocco E, Rajendran S, Zardo L, Macchi V, Grandi C, Tagariello G, Porzionato A, Radossi P, De Caro R, and Parnigotto PP

Subjects

Adult, Blood Coagulation Tests, Cell Differentiation, Cells, Cultured, Culture Media metabolism, Humans, Partial Thromboplastin Time, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy, Mesenchymal Stem Cells metabolism

Abstract

In recent decades, the use of adult multipotent stem cells has paved the way for the identification of new therapeutic approaches for the treatment of monogenic diseases such as Haemophilia A. Being already studied for regenerative purposes, adipose-derived mesenchymal stem cells (Ad-MSCs) are still poorly considered for Haemophilia A cell therapy and their capacity to produce coagulation factor VIII (FVIII) after proper stimulation and without resorting to gene transfection. In this work, Ad-MSCs were in vitro conditioned towards the endothelial lineage, considered to be responsible for coagulation factor production. The cells were cultured in an inductive medium enriched with endothelial growth factors for up to 21 days. In addition to significantly responding to the chemotactic endothelial stimuli, the cell populations started to form capillary-like structures and up-regulated the expression of specific endothelial markers (CD34, PDGFRα, VEGFR2, VE-cadherin, CD31, and vWF). A dot blot protein study detected the presence of FVIII in culture media collected from both unstimulated and stimulated Ad-MSCs. Remarkably, the activated partial thromboplastin time test demonstrated that the clot formation was accelerated, and FVIII activity was enhanced when FVIII deficient plasma was mixed with culture media from the untreated/stimulated Ad-MSCs. Overall, the collected evidence supported a possible Ad-MSC contribution to HA correction via specific stimulation by the endothelial microenvironment and without any need for gene transfection.

Published

2022

10. Defenestrated endothelium delays liver-directed gene transfer in hemophilia A mice.

Author

Kaminski TW, Ju EM, Gudapati S, Vats R, Arshad S, Dubey RK, Katoch O, Tutuncuoglu E, Frank J, Brzoska T, Stolz DB, Watkins SC, Chan SY, Ragni MV, Novelli EM, Sundd P, and Pradhan-Sundd T

Subjects

Animals, Endothelium, Genetic Therapy, Genetic Vectors genetics, Humans, Liver metabolism, Mice, Mice, Knockout, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy

Abstract

Hemophilia A is an inherited bleeding disorder caused by defective or deficient coagulation factor VIII (FVIII) activity. Until recently, the only treatment for prevention of bleeding involved IV administration of FVIII. Gene therapy with adeno-associated vectors (AAVs) has shown some efficacy in patients with hemophilia A. However, limitations persist due to AAV-induced cellular stress, immunogenicity, and reduced durability of gene expression. Herein, we examined the efficacy of liver-directed gene transfer in FVIII knock-out mice by AAV8-GFP. Surprisingly, compared with control mice, FVIII knockout (F8TKO) mice showed significant delay in AAV8-GFP transfer in the liver. We found that the delay in liver-directed gene transfer in F8TKO mice was associated with absence of liver sinusoidal endothelial cell (LSEC) fenestration, which led to aberrant expression of several sinusoidal endothelial proteins, causing increased capillarization and decreased permeability of LSECs. This is the first study to link impaired liver-directed gene transfer to liver-endothelium maladaptive structural changes associated with FVIII deficiency in mice., (© 2022 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

2022

11. Therapeutic correction of hemophilia A using 2D endothelial cells and multicellular 3D organoids derived from CRISPR/Cas9-engineered patient iPSCs.

Author

Son JS, Park CY, Lee G, Park JY, Kim HJ, Kim G, Chi KY, Woo DH, Han C, Kim SK, Park HJ, Kim DW, and Kim JH

Subjects

Animals, CRISPR-Cas Systems genetics, Endothelial Cells metabolism, Humans, Mice, Organoids metabolism, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy, Induced Pluripotent Stem Cells metabolism

Abstract

The bleeding disorder hemophilia A (HA) is caused by a single-gene (F8) defect and its clinical symptom can be substantially improved by a small increase in the plasma coagulation factor VIII (FVIII) level. In this study, we used F8-defective human induced pluripotent stem cells from an HA patient (F8d-HA hiPSCs) and F8-corrected (F8c) HA hiPSCs produced by CRISPR/Cas9 genome engineering of F8d-HA hiPSCs. We obtained a highly enriched population of CD157 + cells from CRISPR/Cas9-edited F8c-HA hiPSCs. These cells exhibited multiple cellular and functional phenotypes of endothelial cells (ECs) with significant levels of FVIII activity, which was not observed in F8d-HA hiPSC-ECs. After transplantation, the engineered F8c-HA hiPSC-ECs dramatically changed bleeding episodes in HA animals and restored plasma FVIII activity. Notably, grafting a high dose of ECs substantially reduced the bleeding time during multiple consecutive bleeding challenges in HA mice, demonstrating a robust hemostatic effect (90% survival). Furthermore, the engrafted ECs survived more than 3 months in HA mice and reversed bleeding phenotypes against lethal wounding challenges. We also produced F8c-HA hiPSC-derived 3D liver organoids by assembling three different cell types in microwell devices and confirmed its therapeutic effect in HA animals. Our data demonstrate that the combination of genome-engineering and iPSC technologies represents a novel modality that allows autologous cell-mediated gene therapy for treating HA., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

12. 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

13. Transduction of modified factor VIII gene improves lentiviral gene therapy efficacy for hemophilia A.

Author

Gong J, Chung TH, Zheng J, Zheng H, and Chang LJ

Subjects

Humans, K562 Cells, Factor VIII biosynthesis, Factor VIII genetics, Genetic Therapy, Genetic Vectors, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy, Lentivirus, Transduction, Genetic

Abstract

Hemophilia A (HA) is a bleeding disorder caused by deficiency of the coagulation factor VIII (F8). F8 replacement is standard of care, whereas gene therapy (F8 gene) for HA is an attractive investigational approach. However, the large size of the F8 gene and the immunogenicity of the product present challenges in development of the F8 gene therapy. To resolve these problems, we synthesized a shortened F8 gene (F8-BDD) and cloned it into a lentiviral vector (LV). The F8-BDD produced mainly short cleaved inactive products in LV-transduced cells. To improve F8 functionality, we designed two novel F8-BDD genes, one with an insertion of eight specific N-glycosylation sites (F8-N8) and another which restored all N-glycosylation sites (F8-299) in the B domain. Although the overall protein expression was reduced, high coagulation activity (>100-fold) was detected in the supernatants of LV-F8-N8- and LV-F8-299-transduced cells. Protein analysis of F8 and the procoagulation cofactor, von Willebrand Factor, showed enhanced interaction after restoration of B domain glycosylation using F8-299. HA mouse hematopoietic stem cell transplantation studies illustrated that the bleeding phenotype was corrected after LV-F8-N8 or -299 gene transfer into the hematopoietic stem cells. Importantly, the F8-299 modification markedly reduced immunogenicity of the F8 protein in these HA mice. In conclusion, the modified F8-299 gene could be efficiently packaged into LV and, although with reduced expression, produced highly stable and functional F8 protein that corrected the bleeding phenotype without inhibitory immunogenicity. We anticipate that these results will be beneficial in the development of gene therapies against HA., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

14. 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

15. An epileptic seizure and haemorrhage into the ventricular system of the brain as the first manifestations of acquired haemophilia A - Case report.

Author

Sokołowska B, Kozińska J, Szczepanek D, Wąsik-Szczepanek E, Kozioł M, Majowicz D, Juda A, and Hus M

Subjects

Autoantibodies blood, Cerebral Ventricles diagnostic imaging, Factor VIII metabolism, Hemophilia A diagnostic imaging, Hemophilia A metabolism, Hemophilia A pathology, Hemorrhage diagnostic imaging, Hemorrhage etiology, Hemorrhage pathology, Humans, Male, Middle Aged, Seizures blood, Seizures pathology, Cerebral Ventricles blood supply, Hemophilia A complications, Seizures etiology

Abstract

Acquired haemophilia (AH) is a suddenly occurring severe blood diathesis that affects both males and females and is caused by autoantibodies which inhibit coagulation factor VIII. The report describes an unusual case of acquired haemophilia in which an epileptic seizure and haemorrhage into the ventricular system of the brain were the first manifestations of the disease. In addition, APTT was prolonged to 94.6 seconds and the factor VIII level was as low as 1.5%. The level of anti-FVIII antibody was extremely high - 272BU/ml. The patient did not undergo invasive diagnostic procedure or an operation. Recombinant factor VIIa was used to control the bleeding. In order to eradicate the inhibitor, the patient received prednisone and cyclophosphamide. Complete remission was achieved after 5.5 weeks of treatment.

Published

2021

16. Dissection of pleiotropic effects of variants in and adjacent to F8 exon 19 and rescue of mRNA splicing and protein function.

Author

Lombardi S, Leo G, Merlin S, Follenzi A, McVey JH, Maestri I, Bernardi F, Pinotti M, and Balestra D

Subjects

Computational Biology, Hemophilia A genetics, Hemophilia A metabolism, Humans, Phenotype, Protein Biosynthesis, RNA, Messenger metabolism, Exons, Factor VIII genetics, Factor VIII metabolism, Hemophilia A pathology, Mutation, RNA Splicing, RNA, Messenger genetics

Abstract

The pathogenic significance of nucleotide variants commonly relies on nucleotide position within the gene, with exonic changes generally attributed to quantitative or qualitative alteration of protein biosynthesis, secretion, activity, or clearance. However, these changes may exert pleiotropic effects on both protein biology and mRNA splicing due to the overlapping of the amino acid and splicing codes, thus shaping the disease phenotypes. Here, we focused on hemophilia A, in which the definition of F8 variants' causative role and association to bleeding phenotypes is crucial for proper classification, genetic counseling, and management of affected individuals. We extensively characterized a large panel of hemophilia A-causing variants (n = 30) within F8 exon 19 by combining and comparing in silico and recombinant expression analyses. We identified exonic variants with pleiotropic effects and dissected the altered protein features of all missense changes. Importantly, results from multiple prediction algorithms provided qualitative results, while recombinant assays allowed us to correctly infer the likely phenotype severity for 90% of variants. Molecular characterization of pathogenic variants was also instrumental for the development of tailored correction approaches to rescue splicing affecting variants or missense changes impairing protein folding. A single engineered U1snRNA rescued mRNA splicing of nine different variants and the use of a chaperone-like drug resulted in improved factor VIII protein secretion for four missense variants. Overall, dissection of the molecular mechanisms of a large panel of HA variants allowed precise classification of HA-affected individuals and favored the development of personalized therapeutic approaches., Competing Interests: Declaration of interests M.P. is the inventor of a patent (PCT/IB2011/054573) on modified U1snRNAs. All other authors declare no competing interests., (Copyright © 2021 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2021

17. Tailoring the effect of antithrombin-targeting therapy in haemophilia A using in silico thrombin generation.

Author

de Laat-Kremers RMW, Ninivaggi M, van Moort I, de Maat M, and de Laat B

Subjects

Adult, Blood Coagulation drug effects, Hemophilia A metabolism, Hemophilia B drug therapy, Hemophilia B metabolism, Humans, Male, Middle Aged, Prothrombin metabolism, Thrombin metabolism, Antithrombins pharmacology, Hemophilia A drug therapy

Abstract

Factor (F) VIII deficiency causes bleeding in haemophilia A patients because of the reduced formation of procoagulant enzyme thrombin, which is needed to make the blood clot. We measured the dynamics of coagulation in haemophilia A patients by measuring thrombin generation (TG). Additionally, we quantified the procoagulant process of prothrombin conversion and anticoagulant process of thrombin inhibitor complex formation. In haemophilia A, prothrombin conversion is severely reduced, causing TG to be low. Nevertheless, the thrombin inactivation capacity of these patients is comparable to that in healthy subjects, leading to a severe imbalance between procoagulant and anticoagulant processes and a subsequent increased bleeding risk. A novel therapy in haemophilia A is the targeting of anticoagulant pathway, e.g. thrombin inhibitor antithrombin (AT), to restore the haemostatic balance. We simulated the effect of AT reduction on TG in silico. Lowering AT levels restored TG dose-dependently and an AT reduction of 90-95% led to almost normal TG in most patients . However, the variation in response to AT reduction was large between patients, indicating that this approach should be tailored to each individual patients. Ideally, TG and thrombin dynamics simulation could in the future contribute to the management of patients undergoing AT targeting therapy., (© 2021. The Author(s).)

Published

2021

18. Gene Therapy in Hemophilia: Recent Advances.

Author

Rodríguez-Merchán EC, De Pablo-Moreno JA, and Liras A

Subjects

Animals, Factor IX genetics, Factor IX metabolism, Factor VIII genetics, Factor VIII metabolism, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A pathology, Hemophilia B genetics, Hemophilia B metabolism, Hemophilia B pathology, Humans, Genetic Therapy methods, Hemophilia A therapy, Hemophilia B therapy

Abstract

Hemophilia is a monogenic mutational disease affecting coagulation factor VIII or factor IX genes. The palliative treatment of choice is based on the use of safe and effective recombinant clotting factors. Advanced therapies will be curative, ensuring stable and durable concentrations of the defective circulating factor. Results have so far been encouraging in terms of levels and times of expression using mainly adeno-associated vectors. However, these therapies are associated with immunogenicity and hepatotoxicity. Optimizing the vector serotypes and the transgene (variants) will boost clotting efficacy, thus increasing the viability of these protocols. It is essential that both physicians and patients be informed about the potential benefits and risks of the new therapies, and a register of gene therapy patients be kept with information of the efficacy and long-term adverse events associated with the treatments administered. In the context of hemophilia, gene therapy may result in (particularly indirect) cost savings and in a more equitable allocation of treatments. In the case of hemophilia A, further research is needed into how to effectively package the large factor VIII gene into the vector; and in the case of hemophilia B, the priority should be to optimize both the vector serotype, reducing its immunogenicity and hepatotoxicity, and the transgene, boosting its clotting efficacy so as to minimize the amount of vector administered and decrease the incidence of adverse events without compromising the efficacy of the protein expressed.

Published

2021

19. Protein residue network analysis reveals fundamental properties of the human coagulation factor VIII.

Author

Lopes TJS, Rios R, Nogueira T, and Mello RF

Subjects

Amino Acid Motifs, Binding Sites, Factor VIII metabolism, Hemophilia A genetics, Humans, Machine Learning, Models, Molecular, Protein Conformation, Protein Stability, Factor VIII chemistry, Factor VIII genetics, Hemophilia A metabolism, Mutation

Abstract

Hemophilia A is an X-linked inherited blood coagulation disorder caused by the production and circulation of defective coagulation factor VIII protein. People living with this condition receive either prophylaxis or on-demand treatment, and approximately 30% of patients develop inhibitor antibodies, a serious complication that limits treatment options. Although previous studies performed targeted mutations to identify important residues of FVIII, a detailed understanding of the role of each amino acid and their neighboring residues is still lacking. Here, we addressed this issue by creating a residue interaction network (RIN) where the nodes are the FVIII residues, and two nodes are connected if their corresponding residues are in close proximity in the FVIII protein structure. We studied the characteristics of all residues in this network and found important properties related to disease severity, interaction to other proteins and structural stability. Importantly, we found that the RIN-derived properties were in close agreement with in vitro and clinical reports, corroborating the observation that the patterns derived from this detailed map of the FVIII protein architecture accurately capture the biological properties of FVIII.

Published

2021

20. Activated protein C has a regulatory role in factor VIII function.

Author

Wilhelm AR, Parsons NA, Samelson-Jones BJ, Davidson RJ, Esmon CT, Camire RM, and George LA

Subjects

Animals, Chlorides toxicity, Factor VIII genetics, Female, Ferric Compounds toxicity, Hemophilia A chemically induced, Hemophilia A metabolism, Male, Mice, Mice, Inbred C57BL, Protein C genetics, Recombinant Proteins genetics, Factor VIII metabolism, Hemophilia A pathology, Hemostasis, Protein C metabolism, Recombinant Proteins metabolism

Abstract

Mechanisms thought to regulate activated factor VIII (FVIIIa) cofactor function include A2-domain dissociation and activated protein C (APC) cleavage. Unlike A2-domain dissociation, there is no known phenotype associated with altered APC cleavage of FVIII, and biochemical studies have suggested APC plays a marginal role in FVIIIa regulation. However, the in vivo contribution of FVIIIa inactivation by APC is unexplored. Here we compared wild-type B-domainless FVIII (FVIII-WT) recombinant protein with an APC-resistant FVIII variant (FVIII-R336Q/R562Q; FVIII-QQ). FVIII-QQ demonstrated expected APC resistance without other changes in procoagulant function or A2-domain dissociation. In plasma-based studies, FVIII-WT/FVIIIa-WT demonstrated dose-dependent sensitivity to APC with or without protein S, whereas FVIII-QQ/FVIIIa-QQ did not. Importantly, FVIII-QQ demonstrated approximately fivefold increased procoagulant function relative to FVIII-WT in the tail clip and ferric chloride injury models in hemophilia A (HA) mice. To minimize the contribution of FV inactivation by APC in vivo, a tail clip assay was performed in homozygous HA/FV Leiden (FVL) mice infused with FVIII-QQ or FVIII-WT in the presence or absence of monoclonal antibody 1609, an antibody that blocks murine PC/APC hemostatic function. FVIII-QQ again demonstrated enhanced hemostatic function in HA/FVL mice; however, FVIII-QQ and FVIII-WT performed analogously in the presence of the PC/APC inhibitory antibody, indicating the increased hemostatic effect of FVIII-QQ was APC specific. Our data demonstrate APC contributes to the in vivo regulation of FVIIIa, which has the potential to be exploited to develop novel HA therapeutics., (© 2021 by The American Society of Hematology.)

Published

2021

21. Serpins, New Therapeutic Targets for Hemophilia.

Author

Aymonnier K, Kawecki C, Arocas V, Boulaftali Y, and Bouton MC

Subjects

Animals, Drug Discovery, Hemophilia A blood, Hemophilia A metabolism, Hemophilia B blood, Hemophilia B metabolism, Humans, Serpins blood, Blood Coagulation drug effects, Hemophilia A drug therapy, Hemophilia B drug therapy, Serpins metabolism, Serpins therapeutic use

Abstract

Hemostasis is a tightly regulated process characterized by a finely tuned balance between procoagulant and anticoagulant systems. Among inherited hemostatic conditions, hemophilia is one of the most well-known bleeding disorders. Hemophilia A (HA) and B (HB) are due to deficiencies in coagulation factor VIII (FVIII) or FIX, respectively, leading to unwanted bleeding. Until recently, hemophilia treatment has consisted of prophylactic replacement therapy using plasma-derived or recombinant FVIII in cases of HA or FIX in cases of HB. Because FVIII and FIX deficiencies lead to an imbalance between procoagulant and anticoagulant systems, a recent upcoming strategy implies blocking of endogenous anticoagulant proteins to compensate for the procoagulant factor deficit, thus restoring hemostatic equilibrium. Important physiological proteins of the anticoagulant pathways belong to the serpin (serine protease inhibitor) family and, recently, different experimental and clinical studies have demonstrated that targeting natural serpins could decrease bleeding in hemophilia. Here, we aim to review the different, recent studies demonstrating that blocking serpins such as antithrombin, protein Z-dependent protease inhibitor, and protease nexin-1 or modifying a serpin like α1-antitrypsin could rebalance coagulation in hemophilia. Furthermore, we underline the potential therapeutic use of serpins for the treatment of hemophilia., Competing Interests: M.-C.B. has a patent application related to PN-1 targeting in hemophilia., (Thieme. All rights reserved.)

Published

2021

22. PrimeDesign software for rapid and simplified design of prime editing guide RNAs.

Author

Hsu JY, Grünewald J, Szalay R, Shih J, Anzalone AV, Lam KC, Shen MW, Petri K, Liu DR, Joung JK, and Pinello L

Subjects

Base Pairing, Base Sequence, CRISPR-Associated Protein 9 genetics, CRISPR-Associated Protein 9 metabolism, Clustered Regularly Interspaced Short Palindromic Repeats, Databases, Genetic, Fabry Disease genetics, Fabry Disease metabolism, Fabry Disease pathology, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, HEK293 Cells, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A pathology, Humans, Models, Biological, Muscular Dystrophy, Duchenne genetics, Muscular Dystrophy, Duchenne metabolism, Muscular Dystrophy, Duchenne pathology, Mutation, Nucleic Acid Conformation, Plasmids chemistry, Plasmids metabolism, RNA, Guide, CRISPR-Cas Systems metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, CRISPR-Cas Systems, Gene Editing methods, Genome, Human, RNA, Guide, CRISPR-Cas Systems genetics

Abstract

Prime editing (PE) is a versatile genome editing technology, but design of the required guide RNAs is more complex than for standard CRISPR-based nucleases or base editors. Here we describe PrimeDesign, a user-friendly, end-to-end web application and command-line tool for the design of PE experiments. PrimeDesign can be used for single and combination editing applications, as well as genome-wide and saturation mutagenesis screens. Using PrimeDesign, we construct PrimeVar, a comprehensive and searchable database that includes candidate prime editing guide RNA (pegRNA) and nicking sgRNA (ngRNA) combinations for installing or correcting >68,500 pathogenic human genetic variants from the ClinVar database. Finally, we use PrimeDesign to design pegRNAs/ngRNAs to install a variety of human pathogenic variants in human cells.

Published

2021

23. Pathological mechanism of joint destruction in haemophilic arthropathy.

Author

Zhu H, Meng Y, Tong P, and Zhang S

Subjects

Adult, Arthritis genetics, Arthritis immunology, Arthritis metabolism, Bone Diseases, Metabolic genetics, Bone Diseases, Metabolic immunology, Bone Diseases, Metabolic metabolism, Child, Cytokines genetics, Cytokines immunology, Factor VIII therapeutic use, Gene Expression Regulation, Hemarthrosis genetics, Hemarthrosis immunology, Hemarthrosis metabolism, Hemophilia A genetics, Hemophilia A immunology, Hemophilia A metabolism, Humans, Intercellular Signaling Peptides and Proteins genetics, Intercellular Signaling Peptides and Proteins immunology, Iron immunology, Iron metabolism, Joints immunology, Joints metabolism, Joints pathology, Osteonecrosis genetics, Osteonecrosis immunology, Osteonecrosis metabolism, Quality of Life, Synovitis genetics, Synovitis immunology, Synovitis metabolism, Arthritis pathology, Bone Diseases, Metabolic pathology, Hemarthrosis pathology, Hemophilia A pathology, Osteonecrosis pathology, Synovitis pathology

Abstract

Haemophilic arthropathy (HA), caused by intra-articular haemorrhage, is one of the most common complications in patients with haemophilia. Factor replacement therapy provides missing coagulation factors to prevent children with haemophilia from joint bleeding and decreases their risk for HA. However, haemophilia patients in developing countries are still suffering from HA due to insufficient replacement therapy. Symptoms such as pain and activity limitations caused by HA seriously affect the functional abilities and quality of life of patients with HA, causing a high disability rate in the haemophilia cohort. The pathological mechanism of HA is complicated because the whole pathological mainly involves hypertrophic synovitis, osteopenia, cartilage and bone destruction, and these pathological changes occur in parallel and interact with each other. Inflammation plays an important role in the whole complex pathological process, and iron, cytokines, growth factors and other factors are involved. This review summarizes the pathological mechanism of HA to provide background for clinical and basic research.

Published

2021

24. Population Pharmacokinetics of Clotting Factor Concentrates and Desmopressin in Hemophilia.

Author

Preijers T, Schütte LM, Kruip MJHA, Cnossen MH, Leebeek FWG, van Hest RM, and Mathôt RAA

Subjects

Child, Humans, Blood Coagulation Factors pharmacokinetics, Deamino Arginine Vasopressin pharmacokinetics, Hemophilia A drug therapy, Hemophilia A metabolism

Abstract

Hemophilia A and B are bleeding disorders caused by a deficiency of clotting factor VIII and IX, respectively. Patients with severe hemophilia (< 0.01 IU mL -1 ) and some patients with moderate hemophilia (0.01-0.05 IU mL -1 ) administer clotting factor concentrates prophylactically. Desmopressin (D-amino D-arginine vasopressin) can be applied in patients with non-severe hemophilia A. The aim of administration of factor concentrates or desmopressin is the prevention or cessation of bleeding. Despite weight-based dosing, it has been demonstrated that factor concentrates still exhibit considerable pharmacokinetic variability. Population pharmacokinetic analyses, in which this variability is quantified and explained, are increasingly performed in hemophilia research. These analyses can assist in the identification of important patient characteristics and can be applied to perform patient-tailored dosing. This review aims to present and discuss the population pharmacokinetic analyses that have been conducted to develop population pharmacokinetic models describing factor levels after administration of factor VIII or factor IX concentrates or D-amino D-arginine vasopressin. In total, 33 publications were retrieved from the literature. Two approaches were applied to perform population pharmacokinetic analyses, the standard two-stage approach and non-linear mixed-effect modeling. Using the standard two-stage approach, four population pharmacokinetic models were established describing factor VIII levels. In the remaining 29 analyses, the non-linear mixed-effect modeling approach was applied. NONMEM was the preferred software to establish population pharmacokinetic models. In total, 18 population pharmacokinetic analyses were conducted on the basis of data from a single product. From all available population pharmacokinetic analyses, 27 studies also included data from pediatric patients. In the majority of the population pharmacokinetic models, the population pharmacokinetic parameters were allometrically scaled using actual body weight. In this review, the available methods used for constructing the models, key features of these models, patient population characteristics, and established covariate relationships are described in detail.

Published

2021

25. Genetics and Hemostatic Potential in Persons with Mild to Moderate Hemophilia A with a Discrepancy between One-Stage and Chromogenic FVIII Assays.

Author

Strålfors A, Mikovic D, Schmidt D, Onelöv L, Soutari NMH, Berndtson M, Chaireti R, Holmström M, Antovic JP, and Bruzelius M

Subjects

Adolescent, Adult, Aged, Blood Coagulation Tests methods, DNA Mutational Analysis, Factor VIII metabolism, Female, Hemophilia A blood, Hemophilia A metabolism, Hemostasis, Humans, Male, Middle Aged, Young Adult, Factor VIII genetics, Hemophilia A genetics, Mutation

Abstract

Background:  Factor VIII (FVIII) activity (FVIII:C) can be measured by different methods including one-stage clotting assays (OSAs) and chromogenic assays (CSAs). Discrepancy between FVIII:C assays is known and associated with genetic variations causing mild and moderate hemophilia A (HA). We aimed to study the discrepancy phenomenon and to identify associated genetic alterations. Further, we investigated if hemostatic global assays could discriminate the group with discrepant FVIII:C from them., Methods:  The study contained plasma samples from 45 patients with HA (PwHA) from Hemophilia Centers in Stockholm, Sweden, and Belgrade, Serbia. We measured FVIII:C with OSA and CSA, sequenced the F8 gene, and performed two global hemostatic assays; endogenous thrombin potential and overall hemostatic potential., Results:  Nineteen of 45 PwHA had a more than twofold higher FVIII:C using OSA compared to CSA and were considered discrepant. Thirty-four causal mutations were detected, where of five had not previously been associated with assay discrepancy. These novel mutations were p.Tyr25Cys, p.Phe698Leu, p.Met699Leu, p.Ile1698Thr, and Ala2070Val. We found no difference between discrepant and nondiscrepant cases with either of the global assays., Conclusion:  There was a discrepancy between FVIII:C assays in almost half of the PwHA, which for some could lead to missed HA diagnoses or misclassification of severity. Genotyping confirmed that mutations associated with FVIII:C discrepancy cluster in the A domains of F8 , and five mutations not previously associated with FVIII:C discrepancy was identified. Global hemostatic assays did not contribute to distinguish assay discrepancy in PwHA., Competing Interests: J.P.A. has received research grants from Shire, honoraria from Stago, Siemens, Sysmex, Roche, Baxter, Sobi, and acts on advisory boards for Sobi and Novo Nordisk. M.B. acts on the advisory board for CSL Behring, has had consultant assignments for Novo Nordisk, and received lecturer honoraria from Sobi., (Thieme. All rights reserved.)

Published

2021

26. 2021 clinical trials update: Innovations in hemophilia therapy.

Author

Croteau SE, Wang M, and Wheeler AP

Subjects

Clinical Trials as Topic, Humans, Inflammation genetics, Inflammation metabolism, Inflammation therapy, Blood Coagulation, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A therapy

Abstract

Therapies engineered to prolong clotting factor protein circulation time, manipulate the balance of pro-coagulant and anti-coagulant proteins, or introduce new genetic material to enable endogenous factor protein production dominate the clinical trial landscape of hemophilia. The availability of clotting factor concentrates and the establishment of primary prophylaxis have dramatically improved health outcomes for hemophilia patients. But, the burden of hemostatic therapy remains significant, and many barriers to consistent longitudinal use of prophylaxis exist. Several types of emerging therapeutics including engineered factor concentrates, substitutive therapies, rebalancing therapies, and gene transfer/editing all aim to reduce the challenges of current hemophilia treatment. Emerging treatment options may reduce treatment frequency or need for intravenous administration. They may also introduce new challenges in laboratory assessment of hemostasis. These novel therapies must not introduce significant new health risks and continue to support similar or improved outcomes. The potential ramifications of rebalancing the coagulation cascade, particularly in a stress or inflammatory state, or introduction of new genetic material are not trivial. The focus of this review is to provide an overview of active and recently completed clinical trials as well as emerging preclinical data investigating new therapeutic possibilities for hemophilia patients and potentially other rare bleeding disorders., (© 2020 Wiley Periodicals LLC.)

Published

2021

27. CD4 + T cells engineered with FVIII-CAR and murine Foxp3 suppress anti-factor VIII immune responses in hemophilia a mice.

Author

Fu RY, Chen AC, Lyle MJ, Chen CY, Liu CL, and Miao CH

Subjects

Animals, Antibodies, Monoclonal immunology, Antibodies, Neutralizing immunology, CD4-Positive T-Lymphocytes immunology, Factor VIII genetics, Forkhead Transcription Factors genetics, Forkhead Transcription Factors metabolism, Genetic Therapy methods, HEK293 Cells, Hemophilia A metabolism, Humans, Immune Tolerance immunology, Male, Mice, Mice, Inbred C57BL, Receptors, Chimeric Antigen genetics, Receptors, Chimeric Antigen immunology, Receptors, Chimeric Antigen metabolism, T-Lymphocytes, Regulatory immunology, T-Lymphocytes, Regulatory metabolism, Factor VIII immunology, Forkhead Transcription Factors immunology, Hemophilia A immunology, Hemophilia A therapy, Immunotherapy, Adoptive methods, T-Lymphocytes, Regulatory transplantation

Abstract

Although protein replacement therapy provides effective treatment for hemophilia A patients, about a third of severe patients develop neutralizing inhibitor antibodies to factor VIII. Adoptive transfer of regulatory T cells (Tregs) has shown promise in treating unwanted immune responses. In previous studies, transferred polyclonal Tregs ameliorated the anti-factor VIII immune responses in hemophilia A mice. In addition, factor VIII-primed Tregs demonstrated increased suppressive function. However, antigen-specific Tregs are a small fraction of the total lymphocyte population. To generate large numbers of factor VIII-specific Tregs, the more abundant murine primary CD4 + T cells were lentivirally transduced ex vivo to express Foxp3 and a chimeric antigen receptor specific to factor VIII (F8CAR). Transduced cells significantly inhibited the proliferation of factor VIII-specific effector T cells in suppression assays. To monitor the suppressive function of the transduced chimeric antigen receptor expressing T cells in vivo, engineered CD4 + CD25 + Foxp3 + F8CAR-Tregs were sorted and adoptively transferred into hemophilia A mice that are treated with hydrodynamically injected factor VIII plasmid. Mice receiving engineered F8CAR-Tregs showed maintenance of factor VIII clotting activity and did not develop anti-factor VIII inhibitors, while control CD4 + T cell or PBS recipient mice developed inhibitors and had a sharp decrease in factor VIII activity. These results show that CD4 + cells lentivirally transduced to express Foxp3 and F8CAR can promote factor VIII tolerance in a murine model. With further development and testing, this approach could potentially be applied to human hemophilia patients., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

28. BIVV001 Fusion Protein as Factor VIII Replacement Therapy for Hemophilia A.

Author

Konkle BA, Shapiro AD, Quon DV, Staber JM, Kulkarni R, Ragni MV, Chhabra ES, Poloskey S, Rice K, Katragadda S, Fruebis J, and Benson CC

Subjects

Adult, Dose-Response Relationship, Drug, Factor VIII antagonists & inhibitors, Half-Life, Hemophilia A metabolism, Humans, Injections, Intravenous, Male, Middle Aged, Molecular Structure, Recombinant Fusion Proteins adverse effects, Recombinant Fusion Proteins pharmacokinetics, Young Adult, Factor VIII metabolism, Hemophilia A drug therapy, Recombinant Fusion Proteins administration & dosage

Abstract

Background: Factor VIII replacement products have improved the care of patients with hemophilia A, but the short half-life of these products affects the patients' quality of life. The half-life of recombinant factor VIII ranges from 15 to 19 hours because of the von Willebrand factor chaperone effect. BIVV001 (rFVIIIFc-VWF-XTEN) is a novel fusion protein designed to overcome this half-life ceiling and maintain high sustained factor VIII activity levels. Data are lacking on the safety and pharmacokinetics of single-dose BIVV001., Methods: In this phase 1-2a open-label trial, we consecutively assigned 16 previously treated men (18 to 65 years of age) with severe hemophilia A (factor VIII activity, <1%) to receive a single intravenous injection of recombinant factor VIII at a dose of 25 IU per kilogram of body weight (lower-dose group) or 65 IU per kilogram (higher-dose group). This injection was followed by a washout period of at least 3 days. The patients then received a single intravenous injection of BIVV001 at the same corresponding dose of either 25 IU or 65 IU per kilogram. Adverse events and pharmacokinetic measurements were assessed., Results: No inhibitors to factor VIII were detected and no hypersensitivity or anaphylaxis events were reported up to 28 days after the injection of single-dose BIVV001. The geometric mean half-life of BIVV001 was three to four times as long as that of recombinant factor VIII (37.6 hours vs. 9.1 hours in the lower-dose group and 42.5 vs. 13.2 hours in the higher-dose group); the area under the curve (AUC) for product exposure was six to seven times as great in the two dose groups (4470 hours vs. 638 hours × IU per deciliter in the lower-dose group and 12,800 hours vs. 1960 hours × IU per deciliter in the higher-dose group). After the injection of BIVV001 in the higher-dose group, the mean factor VIII level was in the normal range (≥51%) for 4 days and 17% at day 7, which suggested the possibility of a weekly interval between treatments., Conclusions: In a small, early-phase study involving men with severe hemophilia A, a single intravenous injection of BIVV001 resulted in high sustained factor VIII activity levels, with a half-life that was up to four times the half-life associated with recombinant factor VIII, an increase that could signal a new class of factor VIII replacement therapy with a weekly treatment interval. No safety concerns were reported during the 28-day period after administration. (Funded by Sanofi and Sobi; ClinicalTrials.gov number, NCT03205163.)., (Copyright © 2020 Massachusetts Medical Society.)

Published

2020

29. A bispecific antibody demonstrates limited measurability in routine coagulation assays.

Author

Hartmann R, Feenstra T, Knappe S, Schrenk G, Scheiflinger F, and Dockal M

Subjects

Antibodies, Bispecific chemistry, Antibodies, Monoclonal, Humanized chemistry, Factor VIII analysis, Factor VIII metabolism, Factor X metabolism, Factor Xa metabolism, HEK293 Cells, Hemophilia A metabolism, Humans, Partial Thromboplastin Time methods, Antibodies, Bispecific metabolism, Antibodies, Monoclonal, Humanized metabolism, Blood Coagulation, Blood Coagulation Tests methods, Hemophilia A blood

Abstract

: Accurate monitoring of coagulation, needed for optimal management of patients with haemophilia A with inhibitors, presents a challenge for treating physicians. Although global haemostatic assays may be used in this population, their utility with nonfactor therapies has yet to be established in the clinical setting. The aim of this study was to assess options for potential haemostatic activity monitoring and feasibility for factor VIII (FVIII)-equivalency measurement with a sequence identical analogue (SIA) to emicizumab using different coagulation assays. SIA was analysed using five commercial chromogenic assays and activated partial thromboplastin time (aPTT) assays including clot waveform analysis using five different triggers. Recombinant FVIII served as a comparator in all assays. Thrombin generation in haemophilia A plasma was measured using extrinsic and intrinsic trigger conditions (tissue factor or Factor XIa). Of the five chromogenic assays, a concentration-dependent increase in Factor Xa was observed with one assay, with human Factor IXa and X reagents. The SIA dose-response signal plateaued at therapeutically relevant concentrations and was nonparallel with FVIII reference, thereby not permitting FVIII-equivalence assessment. aPTT varied between reagents, with aPTT normalization occurring at low and below-therapeutic SIA concentrations. SIA [600 nmol/l (90 μg/ml)] only partially restored thrombin generation in individual haemophilia A patient plasma. FVIII-equivalence of SIA could not be determined using standard FVIII protocols and was found to be highly influenced by assay type, analytical conditions and parameters used for calculation. New and/or modified methodology and standard reagents specific for use with nonfactor therapies are required for their utilization in the clinical setting.

Published

2020

30. LPS-induced expression and release of monocyte tissue factor in patients with haemophilia.

Author

Holstein K, Matysiak A, Witt L, Sievers B, Beckmann L, Haddad M, Renné T, Voigtlaender M, and Langer F

Subjects

Adult, Case-Control Studies, Female, Hemophilia A pathology, Humans, Inflammation chemically induced, Inflammation metabolism, Inflammation pathology, Male, Middle Aged, Secretory Pathway drug effects, Severity of Illness Index, Young Adult, Hemophilia A metabolism, Lipopolysaccharides pharmacology, Monocytes drug effects, Monocytes metabolism, Thromboplastin metabolism

Abstract

In haemophilia, thrombin generation and fibrin deposition upon vascular injury critically depend on the tissue factor (TF)-driven coagulation pathway. TF expression by monocytes/macrophages and circulating microvesicles contributes to haemostasis, thrombosis and inflammation. Inflammation is a hallmark of blood-induced joint disease. The aim of this study is to correlate TF production by whole-blood monocytes with inflammatory markers and clinical parameters in patients with moderate-to-severe haemophilia A or B (n = 43) in comparison to healthy males (n = 23). Monocyte TF antigen and microvesicle-associated TF procoagulant activity (MV TF PCA) were measured immediately after blood draw (baseline) and following incubation of whole blood with buffer or lipopolysaccharide (LPS) using two-colour flow cytometry and chromogenic FXa generation assay, respectively. Patients with HIV or uncontrolled HBV/HCV infections were excluded. TF was hardly detectable and not different in baseline and buffer-treaded samples from both groups. Stimulation with LPS, however, induced monocyte TF production, with increased TF-specific mean fluorescence intensity (P = 0.08) and MV TF PCA (P < 0.05) in patients compared to controls. Patients also had elevated hs-CRP and IL-6 serum levels (P < 0.001), which correlated with LPS-induced TF parameters. Further exploratory analyses revealed that the presence of systemic (low-grade) inflammation and boosted LPS-induced monocyte TF production were mainly restricted to patients with clinically controlled HBV and/or HCV infection (n = 16), who were older and also had a significantly worse orthopaedic joint score than patients with no history of viral hepatitis (P < 0.01). Our study delineates a previously unrecognised link between systemic inflammation and inducible monocyte TF production in patients with haemophilia A or B.

Published

2020

31. Role of microRNAs in Hemophilia and Thrombosis in Humans.

Author

Jankowska KI, Sauna ZE, and Atreya CD

Subjects

Blood Coagulation Factors genetics, Blood Coagulation Factors metabolism, Hemophilia A metabolism, Humans, MicroRNAs metabolism, Thrombosis metabolism, Hemophilia A genetics, MicroRNAs genetics, Thrombosis genetics

Abstract

MicroRNAs (miRNA) play an important role in gene expression at the posttranscriptional level by targeting the untranslated regions of messenger RNA (mRNAs). These small RNAs have been shown to control cellular physiological processes including cell differentiation and proliferation. Dysregulation of miRNAs have been associated with numerous diseases. In the past few years miRNAs have emerged as potential biopharmaceuticals and the first miRNA-based therapies have entered clinical trials. Our recent studies suggest that miRNAs may also play an important role in the pathology of genetic diseases that are currently considered to be solely due to mutations in the coding sequence. For instance, among hemophilia A patients there exist a small subset, with normal wildtype genes; i.e., lacking in mutations in the coding and non-coding regions of the F8 gene. Similarly, in many patients with missense mutations in the F8 gene, the genetic defect does not fully explain the severity of the disease. Dysregulation of miRNAs that target mRNAs encoding coagulation factors have been shown to disturb gene expression. Alterations in protein levels involved in the coagulation cascade mediated by miRNAs could lead to bleeding disorders or thrombosis. This review summarizes current knowledge on the role of miRNAs in hemophilia and thrombosis. Recognizing and understanding the functions of miRNAs by identifying their targets is important in identifying their roles in health and diseases. Successful basic research may result in the development and improvement of tools for diagnosis, risk evaluation or even new treatment strategies., Competing Interests: The authors declare no conflict of interest. The findings and conclusions in this review have not been formally disseminated by the Food and Drug Administration and should not be construed as representing any Agency determination or policy.

Published

2020

32. BIVV001, a new class of factor VIII replacement for hemophilia A that is independent of von Willebrand factor in primates and mice.

Author

Seth Chhabra E, Liu T, Kulman J, Patarroyo-White S, Yang B, Lu Q, Drager D, Moore N, Liu J, Holthaus AM, Sommer JM, Ismail A, Rabinovich D, Liu Z, van der Flier A, Goodman A, Furcht C, Tie M, Carlage T, Mauldin R, Dobrowsky TM, Liu Z, Mercury O, Zhu L, Mei B, Schellenberger V, Jiang H, Pierce GF, Salas J, and Peters R

Subjects

Animals, Factor VIII genetics, Hemophilia A metabolism, Hemophilia A pathology, Hemostasis, Humans, Male, Mice, Mice, Inbred C57BL, Primates, von Willebrand Factor genetics, Factor VIII metabolism, Hemophilia A therapy, Hemorrhage prevention & control, Recombinant Fusion Proteins administration & dosage, von Willebrand Factor metabolism

Abstract

Factor VIII (FVIII) replacement products enable comprehensive care in hemophilia A. Treatment goals in severe hemophilia A are expanding beyond low annualized bleed rates to include long-term outcomes associated with high sustained FVIII levels. Endogenous von Willebrand factor (VWF) stabilizes and protects FVIII from degradation and clearance, but it also subjects FVIII to a half-life ceiling of ∼15 to 19 hours. Increasing recombinant FVIII (rFVIII) half-life further is ultimately dependent upon uncoupling rFVIII from endogenous VWF. We have developed a new class of FVIII replacement, rFVIIIFc-VWF-XTEN (BIVV001), that is physically decoupled from endogenous VWF and has enhanced pharmacokinetic properties compared with all previous FVIII products. BIVV001 was bioengineered as a unique fusion protein consisting of a VWF-D'D3 domain fused to rFVIII via immunoglobulin-G1 Fc domains and 2 XTEN polypeptides (Amunix Pharmaceuticals, Inc, Mountain View, CA). Plasma FVIII half-life after BIVV001 administration in mice and monkeys was 25 to 31 hours and 33 to 34 hours, respectively, representing a three- to fourfold increase in FVIII half-life. Our results showed that multifaceted protein engineering, far beyond a few amino acid substitutions, could significantly improve rFVIII pharmacokinetic properties while maintaining hemostatic function. BIVV001 is the first rFVIII with the potential to significantly change the treatment paradigm for severe hemophilia A by providing optimal protection against all bleed types, with less frequent doses. The protein engineering methods described herein can also be applied to other complex proteins., (© 2020 by The American Society of Hematology.)

Published

2020

33. [Switching toward the use of recombinant factor VIII Fc fusion protein Study among 30 patients with severe hemophilia A].

Author

Sattler L, Raissi A, Fornoff D, Gérout AC, Feugeas O, Grunebaum L, and Desprez D

Subjects

Adolescent, Adult, Aged, Blood Coagulation Tests, Factor VIII analysis, Factor VIII pharmacokinetics, Half-Life, Hemophilia A blood, Hemophilia A metabolism, Hemophilia A pathology, Humans, Male, Middle Aged, Patient Satisfaction, Recombinant Fusion Proteins pharmacokinetics, Severity of Illness Index, Thrombin metabolism, Young Adult, Drug Substitution, Factor VIII therapeutic use, Hemophilia A drug therapy, Immunoglobulin Fc Fragments therapeutic use, Recombinant Fusion Proteins therapeutic use

Abstract

Only a few studies on real-world clinical use of recombinant factor VIII -fusionned with Fc (rFVIIIFc, efmoroctocog alpha) have been performed to date, with data on the annual bleeding rate (ABR), the prophylaxis regimen, and FVIII consumption. The aim of our study was to report the real-world clinical application of rFVIIIFc with additional elements, both biological and clinical. A prospective monocentric study has been conducted in the Haemophilia treatment center (HTC) of the Strasbourg university hospital among the severe haemophilia A patients. Thirty male patients were enrolled in the study. After injection of rFVIIIFc, the average time spent above 5%, 2% and 1% of FVIII was respectively almost 3, 4 and 5 days. The average half-life was 15.8 hours. A strong linear correlation between incremental recovery of rFVIIIFc and weight and between rFVIIIFc half-life and basal VWF:Ag level was observed. FVIII activity measurement for rFVIIIFc showed similar results than those previously published. In the follow-up, residual FVIII activity was on average the one of a mild haemophilia patient, corroborated by the results of endogenous thrombin potential of the thrombin generation assay. In clinical practice, rFVIIIFc was well tolerated and patients were mostly satisfied or indifferent of the switch. A single failure was however noticed. No FVIII inhibitor has been detected. Decrease in FVIII consumption was observed, with reduced or unchanged ABR. The switch was an actual success for almost all of the 30 patients, corroborated by satisfactory clinical and biological results.

Published

2020

34. Development and Validation of a Population-Pharmacokinetic Model for Rurioctacog Alfa Pegol (Adynovate ® ): A Report on Behalf of the WAPPS-Hemo Investigators Ad Hoc Subgroup.

Author

Chelle P, Yeung CHT, Croteau SE, Lissick J, Balasa V, Ashburner C, Park YS, Bonanad S, Megías-Vericat JE, Nagao A, Wynn T, Corrales-Medina F, Tran H, Sharathkumar A, Chitlur M, Sarmiento S, Edginton A, and Iorio A

Subjects

Adolescent, Adult, Bayes Theorem, Body Mass Index, Child, Databases, Factual, Factor VIII administration & dosage, Factor VIII therapeutic use, Hemophilia A metabolism, Humans, Infusions, Intravenous, Models, Theoretical, Recombinant Proteins administration & dosage, Recombinant Proteins pharmacokinetics, Recombinant Proteins therapeutic use, Young Adult, Factor VIII pharmacokinetics, Hemophilia A drug therapy, Internet-Based Intervention statistics & numerical data

Abstract

Background and Objective: Rurioctacog alfa pegol (Adynovate) is a modified recombinant factor VIII concentrate used for treating hemophilia A. Aiming to improve treatment tailoring on the Web-Accessible Population Pharmacokinetic Service-Hemophilia (WAPPS-Hemo) platform for patients of all ages treated with Adynovate, we have developed and evaluated a population pharmacokinetic (PopPK) model. On the platform, PopPK models are used as priors for Bayesian forecasting that derive individual PK of hemophilia patients and are subsequently used for personalized dose regimen design., Methods: Factor activity measurements and demographic covariate data from patients infused with Adynovate were extracted from the WAPPS-Hemo database. Evaluations testing the appropriateness of Bayesian forecasting included 10-fold cross validation, a limited sampling analysis (LSA), and an external evaluation using additional independent data extracted from the WAPPS-Hemo database at a later date., Results: The model was constructed using 650 plasma factor activity observations (555 one stage assay and 95 chromogenic assay - 4.6% below limit of quantification) measured in 154 patients from 36 hemophilia centres. A two-compartment model including between subject variability on clearance and central volume was selected as the base model. Covariates were fat free mass on clearance and central volume, age on clearance and assay type on activity. The final model was well-suited to predict PK parameters of new individuals (n = 26) from sparse observations., Conclusions: The development of a PopPK model for Adynovate using real-world data increases the covariate space (e.g. age) beyond what is possible from clinical trial data. This model is available on the WAPPS-Hemo platform for tailoring treatment in hemophilia A patients.

Published

2020

35. Physiological Roles of the von Willebrand Factor-Factor VIII Interaction.

Author

Kiouptsi K and Reinhardt C

Subjects

Factor VIII chemistry, Hemophilia A metabolism, Humans, von Willebrand Diseases metabolism, von Willebrand Factor chemistry, Cardiovascular Physiological Phenomena, Factor VIII metabolism, von Willebrand Factor metabolism

Abstract

Von Willebrand factor (VWF) and coagulation factor VIII (FVIII) circulate as a complex in plasma and have a major role in the hemostatic system. VWF has a dual role in hemostasis. It promotes platelet adhesion by anchoring the platelets to the subendothelial matrix of damaged vessels and it protects FVIII from proteolytic degradation. Moreover, VWF is an acute phase protein that has multiple roles in vascular inflammation and is massively secreted from Weibel-Palade bodies upon endothelial cell activation. Activated FVIII on the other hand, together with coagulation factor IX forms the tenase complex, an essential feature of the propagation phase of coagulation on the surface of activated platelets. VWF deficiency, either quantitative or qualitative, results in von Willebrand disease (VWD), the most common bleeding disorder. The deficiency of FVIII is responsible for Hemophilia A, an X-linked bleeding disorder. Here, we provide an overview on the role of the VWF-FVIII interaction in vascular physiology.

Published

2020

36. Is the Detection of Factor IX Inhibitors in Hemophilia B Orphan than Factor VIII Inhibitors in Hemophilia A? A Concise, Systematic Review.

Author

Mansouritorghabeh H and Mohades ST

Subjects

Blood Coagulation, Blood Coagulation Tests, Factor IX metabolism, Factor VIII metabolism, Hemophilia A blood, Hemophilia B blood, Humans, Factor IX antagonists & inhibitors, Factor VIII antagonists & inhibitors, Hemophilia A metabolism, Hemophilia B metabolism

Abstract

Objective: Development of inhibitors in hemophilia A and B comprise significant challenge for patients, hematologists, and health provider systems. It has recommended by the World Federation of Hemophilia (WFH) to check inhibitors every 3-4 months. The incidence of inhibitor in hemophilia B is lower than hemophilia A. Here, it tried to unravel whether the detection of inhibitors in hemophilia B neglected compared to hemophilia A or not?, Methods: A comprehensive review carried out using six international and local medical search engines on published contributions about inhibitors in hemophilia A and B in Iran., Results: From 699 titles, 12 relevant papers were selected. The mean of factor VIII inhibitors in hemophilia A was 14.8%. The mean of factor IX inhibitors in hemophilia B was 6%. The minimum and maximum reported percentages of factor VIII inhibitors were 4% and 19.6%, while the minimum and maximum of reported percentages of factor IX inhibitors were 0% and 11.8%, respectively. The inhibitors in hemophilia A had reported in 6 papers. One paper had covered the inhibitors in hemophilia B. There were five papers on inhibitors in both hemophilia A and B. The comparison between the reported patients showed that 3020 patients with hemophilia A and 314 patients with hemophilia B had studied., Conclusion: Consistent with the lower frequency of hemophilia B and the lower development of inhibitors in hemophilia B compared to hemophilia A, it was concluded that hemophilia B had not neglected in Iran. It seems to be rational that each country, check rates of detection of inhibitors in hemophilia B to identify whether it has neglected or not., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2020

37. Molecular Engineering of Adeno-Associated Virus Capsid Improves Its Therapeutic Gene Transfer in Murine Models of Hemophilia and Retinal Degeneration.

Author

Mary B, Maurya S, Kumar M, Bammidi S, Kumar V, and Jayandharan GR

Subjects

Animals, Cell Line, Cell Line, Tumor, Disease Models, Animal, Gene Expression genetics, Gene Transfer Techniques, Genetic Therapy methods, Genetic Vectors genetics, Green Fluorescent Proteins genetics, HeLa Cells, Hemophilia A metabolism, Humans, Liver metabolism, Mice, Mice, Inbred C57BL, Retina metabolism, Retinal Degeneration metabolism, Transduction, Genetic methods, Transgenes genetics, Capsid metabolism, Capsid Proteins genetics, Dependovirus genetics, Hemophilia A genetics, Retinal Degeneration genetics

Abstract

Recombinant adeno-associated virus (AAV)-based gene therapy has been promising, but several host-related transduction or immune challenges remain. For this mode of therapy to be widely applicable, it is crucial to develop high transduction and permeating vectors that infect the target at significantly low doses. Because glycosylation of capsid proteins is known to be rate limiting in the life cycle of many viruses, we reasoned that perturbation of glycosylation sites in AAV2 capsid will enhance gene delivery. In our first set experiments, pharmacological modulation of the glycosylation status in host cells, modestly decreased (1-fold) AAV2 packaging efficacy while it improved their gene expression (∼74%) in vitro. We then generated 24 mutant AAV2 vectors modified to potentially create or disrupt a glycosylation site in its capsid. Three of them demonstrated a 1.3-2.5-fold increase in transgene expression in multiple cell lines (HeLa, Huh7, and ARPE-19). Hepatic gene transfer of these vectors in hemophilia B mice, resulted in a 2-fold increase in human coagulation factor (F)IX levels, while its T/B-cell immunogenic response was unaltered. Subsequently, intravitreal gene transfer of glycosylation site-modified vectors in C57BL6/J mice demonstrated an increase in green fluorescence protein expression (∼2- to 4-fold) and enhanced permeation across retina. Subretinal administration of these modified vectors containing RPE65 gene further rescued the photoreceptor response in a murine model of Leber congenital amarousis. Our studies highlight the translational potential of glycosylation site-modified AAV2 vectors for hepatic and ocular gene therapy applications.

Published

2019

38. Concizumab promotes haemostasis via a tissue factor-factor VIIa-dependent mechanism supporting prophylactic treatment of haemophilia: Results from a rabbit haemophilia bleeding model.

Author

Lauritzen B and Hilden I

Subjects

Animals, Disease Models, Animal, Factor VIIa metabolism, Female, Hemophilia A blood, Hemophilia A complications, Hemophilia A metabolism, Hemorrhage blood, Hemorrhage complications, Hemorrhage metabolism, Rabbits, Thromboplastin metabolism, Antibodies, Monoclonal, Humanized therapeutic use, Hemophilia A drug therapy, Hemorrhage drug therapy, Hemostasis drug effects

Published

2019

39. Real-life experience in switching to new extended half-life products at European haemophilia centres.

Author

Peyvandi F, Garagiola I, Boscarino M, Ryan A, Hermans C, and Makris M

Subjects

Europe, Factor IX metabolism, Factor IX therapeutic use, Factor VIII metabolism, Factor VIII therapeutic use, Half-Life, Humans, Surveys and Questionnaires, Hemophilia A drug therapy, Hemophilia A metabolism, Hemophilia B drug therapy, Hemophilia B metabolism, Recombinant Proteins metabolism, Recombinant Proteins therapeutic use

Abstract

The concept of replacement therapy in haemophilia is changing significantly thanks to the switch from standard products to extended half-life products. These novel drugs are showing beneficial effects overcoming current prophylaxis limitations by reducing the infusion frequency, maintaining a higher trough level to ensure a lower risk of bleeding, and making treatment significantly less distressing to patients by improving the quality of life. Real-life data on the efficacy of novel drugs and their impact on routine management of haemophilia A and B patients are still limited. This manuscript reports the results of a European survey conducted by the European Association for Haemophilia and Allied Disorders (EAHAD) at the beginning of 2018 on the clinical management of patients using extended half-life recombinant FVIII and FIX fusion products, since at the time of the survey none of the PEGylated products were available yet. We report data on the efficacy of these novel drugs by 33 European haemophilia centres that have already switched to extended half-life fusion products, showing a significant reduction in the number of infusions and a satisfactory trough levels in the clinical care of haemophilia patients, with a greater impact for haemophilia B., (© 2019 John Wiley & Sons Ltd.)

Published

2019

40. The central role of thrombin in bleeding disorders.

Author

Negrier C, Shima M, and Hoffman M

Subjects

Animals, Blood Platelets metabolism, Blood Platelets pathology, Hemophilia A blood, Hemophilia A metabolism, Hemophilia A pathology, Hemophilia A therapy, Hemorrhage metabolism, Hemorrhage pathology, Hemorrhage therapy, Hemorrhagic Disorders metabolism, Hemorrhagic Disorders pathology, Hemorrhagic Disorders therapy, Humans, Thrombin analysis, Hemorrhage blood, Hemorrhagic Disorders blood, Hemostasis, Thrombin metabolism

Abstract

Maintaining normal hemostasis relies on a regulated system of procoagulant and anticoagulant pathways, and disruption of these processes leads to the loss of hemostatic control, with the potential for excessive bleeding or thrombosis. Evaluation of bleeding disorders has conventionally been achieved by laboratory assays that measure the activity of individual coagulation factors. While such assays have proven effective for detecting abnormalities of the coagulation system and aiding diagnosis, inherent limitations prevent them from capturing a complete picture of hemostatic function. An improved understanding of thrombin activity and its central role in hemostasis and bleeding disorders has led to the clinical development of global assays that are more physiologically relevant than traditional assays; furthermore, these global assays are able to monitor responses to therapy. In this review, we provide an overview of the role of thrombin in hemostasis, and describe the clinical benefits of thrombin monitoring in patients with bleeding disorders. Moreover, we discuss recent advances in thrombin-targeting therapeutic strategies that aim to correct thrombin deficiency and prevent bleeding in patients with hemophilia and other rare bleeding disorders., (Published by Elsevier Ltd.)

Published

2019

41. Mechanisms of vascular permeability and remodeling associated with hemarthrosis in factor VIII-deficient mice.

Author

Cooke EJ, Wyseure T, Zhou JY, Gopal S, Nasamran CA, Fisch KM, Manon-Jensen T, Karsdal MA, Mosnier LO, and von Drygalski A

Subjects

Animals, Disease Models, Animal, Factor VIII administration & dosage, Factor VIII genetics, Female, Hemarthrosis genetics, Hemarthrosis physiopathology, Hemarthrosis prevention & control, Hemophilia A drug therapy, Hemophilia A genetics, Hemophilia A physiopathology, Hemostasis, Hemostatics administration & dosage, Male, Mice, Inbred BALB C, Mice, Knockout, Time Factors, Capillary Permeability drug effects, Factor VIII metabolism, Hemarthrosis metabolism, Hemophilia A metabolism, Synovial Membrane blood supply, Vascular Remodeling drug effects

Abstract

Background: Vascular remodeling associated with hemophilic arthropathy (HA) may contribute to bleed propagation, but the mechanisms remain poorly understood., Objectives: To explore molecular mechanisms of HA and the effects of hemostasis correction on synovial vascular remodeling after joint injury in hypocoagulable mice., Methods: Factor VIII (FVIII)-deficient mice +/- FVIII treatment and hypocoagulable wild-type mice ( Hypo BALB/c) were subjected to subpatellar puncture. Hypo BALB/c mice were treated with warfarin and anti-FVIII before injury, after which warfarin was continued for 2 weeks or reversed +/- continuous anti-FVIII until harvest. Synovial vascularity was analyzed at baseline and 2 to 4 weeks post injury by histology, musculoskeletal ultrasound with power Doppler (microvascular flow), and Evans blue extravasation (vascular permeability). Synovial gene expression and systemic markers of vascular collagen turnover were studied in FVIII-deficient mice by RNA sequencing and enzyme-linked immunosorbent assay., Results: Vascular changes occurred in FVIII-deficient and Hypo BALB/c mice after injury with minimal effect of hemostasis correction. Increased vascular permeability was only significant in FVIII-deficient mice, who exhibited more pronounced vascular remodeling than Hypo BALB/c mice despite similar bleed volumes. FVIII-deficient mice exhibited a strong transcriptional response in synovium that was only partially affected by FVIII treatment and involved genes relating to angiogenesis and extracellular matrix remodeling, with vascular collagen turnover markers detected systemically., Conclusions: Intact hemostasis at the time of hemarthrosis and during healing are both critical to prevent vascular remodeling, which appears worse with severe and prolonged FVIII deficiency. Unbiased RNA sequencing revealed potential targets for intervention and biomarker development to improve management of HA., (© 2019 International Society on Thrombosis and Haemostasis.)

Published

2019

42. Induction of activated T follicular helper cells is critical for anti-FVIII inhibitor development in hemophilia A mice.

Author

Jing W, Chen J, Cai Y, Chen Y, Schroeder JA, Johnson BD, Cui W, and Shi Q

Subjects

Animals, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Disease Models, Animal, Factor VIII genetics, Factor VIII therapeutic use, Germinal Center cytology, Germinal Center immunology, Germinal Center metabolism, Hemophilia A drug therapy, Hemophilia A genetics, Hemophilia A metabolism, Immunization, Immunophenotyping, Lymphocyte Depletion, Mice, Mice, Knockout, Programmed Cell Death 1 Receptor metabolism, Receptors, CXCR5 genetics, Receptors, CXCR5 metabolism, Antibodies, Neutralizing immunology, Factor VIII immunology, Hemophilia A immunology, Lymphocyte Activation immunology, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Helper-Inducer metabolism

Abstract

The development of neutralizing anti-FVIII antibodies (inhibitors) is a major complication of FVIII protein replacement therapy in patients with hemophilia A (HA). Although multiple lines of evidence indicate that the immune response against FVIII is CD4 T-cell-dependent and many FVIII-derived CD4 epitopes have already been discovered, the role of T follicular helper (TFH) cells in FVIII inhibitor development is unknown. TFH cells, a newly identified subset of CD4 T cells, are characterized by expression of the B-cell follicle-homing receptor CXCR5 and PD-1. In this study, we show for the first time that IV FVIII immunization induces activation and accumulation and/or expansion of PD-1+CXCR5+ TFH cells in the spleen of FVIII-deficient (FVIIInull) mice. FVIII inhibitor-producing mice showed increased germinal center (GC) formation and increased GC TFH cells in response to FVIII immunization. Emergence of TFH cells correlated with titers of anti-FVIII inhibitors. Rechallenge with FVIII antigen elicited recall responses of TFH cells. In vitro FVIII restimulation resulted in antigen-specific proliferation of splenic CD4+ T cells from FVIII-primed FVIIInull mice, and the proliferating cells expressed the TFH hallmark transcription factor BCL6. CXCR5+/+ TFH-cell-specific deletion impaired anti-FVIII inhibitor production, confirming the essential role of CXCR5+/+ TFH cells for the generation of FVIII-neutralizing antibodies. Together, our results demonstrate that the induction of activated TFH cells in FVIIInull mice is critical for FVIII inhibitor development, suggesting that inhibition of FVIII-specific TFH-cell activation may be a promising strategy for preventing anti-FVIII inhibitor formation in patients with HA., (© 2019 by The American Society of Hematology.)

Published

2019

43. Hemophilia A and B mice, but not VWF -/- mice, display bone defects in congenital development and remodeling after injury.

Author

Taves S, Sun J, Livingston EW, Chen X, Amiaud J, Brion R, Hannah WB, Bateman TA, Heymann D, and Monahan PE

Subjects

Animals, Blood Coagulation Tests, Bone and Bones metabolism, Hemophilia A genetics, Hemophilia A pathology, Hemophilia B genetics, Hemophilia B pathology, Humans, Interleukin-6 genetics, Male, Mice, Mice, Knockout, Osteoclasts metabolism, Osteoclasts pathology, Osteoporosis genetics, Osteoporosis pathology, Phenotype, RANK Ligand genetics, Sp7 Transcription Factor genetics, Factor IX genetics, Factor VIII genetics, Hemophilia A metabolism, Hemophilia B metabolism, von Willebrand Factor genetics

Abstract

While joint damage is the primary co-morbidity of hemophilia, osteoporosis and osteopenia are also observed. Coagulation factor VIII deficient (FVIII -/- ) mice develop an osteoporotic phenotype in the absence of induced hemarthrosis that is exacerbated two weeks after an induced joint injury. Here we have compared comprehensively the bone health of clotting factor VIII, factor IX, and Von Willebrand Factor knockout (FVIII -/- , FIX -/- , and VWF -/- respectively) mice both in the absence of joint hemorrhage and following induced joint injury. We found FVIII -/- and FIX -/- mice, but not VWF -/- mice, developmentally have an osteoporotic phenotype. Unilateral induced hemarthrosis causes further bone damage in both FVIII -/- and FIX -/- mice, but has little effect on VWF -/- bone health, indicating that the FVIII.VWF complex is not required for normal bone remodeling in vivo. To further investigate the bone healing following hemarthrosis in hemophilia we examined a two week time course using microCT, serum chemistry, and histological analysis. Elevated ratio of osteoprotegerin (OPG)/receptor activator of nuclear factor-kappa B ligand (RANKL), increased osterix + osteoblastic cells, and decreased smoothness of the cortical bone surface were evident within several days of injury, indicative of acute heterotopic mineralization along the cortical surface. This was closely followed by increased interleukin-6 (IL-6) levels, increased osteoclast numbers, and significant trabecular bone loss. Uncoupled and disorganized bone formation and resorption continued for the duration of the study resulting in significant deterioration of the joint. Further elucidation of the shared mechanisms underlying abnormal bone homeostasis in the absence of FVIII or FIX is needed to guide evidence-based approaches to the screening and treatment of the prevalent bone defects in hemophilia A and B.

Published

2019

44. Genetic-Based Approaches to Inherited Metabolic Liver Diseases.

Author

Zabaleta N, Hommel M, Salas D, and Gonzalez-Aseguinolaza G

Subjects

Animals, Clinical Trials as Topic, Dependovirus genetics, Dependovirus metabolism, Gene Transfer Techniques, Genetic Vectors chemistry, Genetic Vectors metabolism, Hemophilia A genetics, Hemophilia A metabolism, Hemophilia A pathology, Hemophilia B genetics, Hemophilia B metabolism, Hemophilia B pathology, Hepatocytes metabolism, Hepatocytes pathology, Humans, Lentivirus genetics, Lentivirus metabolism, Liver metabolism, Liver pathology, Liver Diseases genetics, Liver Diseases metabolism, Liver Diseases pathology, Liver Transplantation, Metabolic Diseases genetics, Metabolic Diseases metabolism, Metabolic Diseases pathology, Gene Editing methods, Genetic Therapy methods, Hemophilia A therapy, Hemophilia B therapy, Liver Diseases therapy, Metabolic Diseases therapy

Abstract

In vertebrates, the liver is the central metabolic organ of the body, which carries out an estimated 500 functions that range from general detoxification to protein synthesis, bile production, metabolism of fats, carbohydrates, proteins, bilirubin, vitamin and mineral storage and it even has an immune function. Hepatocytes are considered the professional liver cells, which carry out all of these functions. With such a variety of tasks to perform, it is not surprising that more than 400 rare monogenic disorders of hepatic origin have been described. For many of these, liver transplantation remains the only curative strategy, however, this is limited by organ availability and requires lifelong immune suppression. The fact that liver transplantation is curative led to the assumption that the restoration of the expression of the defective gene would result in the resolution of the disease. Indeed, liver-directed gene therapy trials for hemophilia A and B have demonstrated the potential of gene therapy to provide long-lasting clinical benefit in the treatment of monogenic liver disorders. Thus, liver-directed gene therapy and gene editing strategies have emerged as promising alternatives to transplantation in inherited monogenic liver disorders. Herein, we review the advances and limitations of gene therapy for such disorders, covering therapeutic strategies based on gene addition and gene editing and the exciting clinical results obtained with the use of ribonucleic acid as therapeutic molecules.

Published

2019

45. A systems pharmacokinetic/pharmacodynamic model for concizumab to explore the potential of anti-TFPI recycling antibodies.

Author

Yuan D, Rode F, and Cao Y

Subjects

Animals, Blood Coagulation drug effects, Endosomes metabolism, Haplorhini, Hemophilia A metabolism, Humans, Models, Biological, Rabbits, Antibodies, Monoclonal pharmacokinetics, Antibodies, Monoclonal, Humanized pharmacokinetics, Lipoproteins metabolism

Abstract

Concizumab is a humanized monoclonal antibody in clinical investigation directed against membrane-bound and soluble tissue factor pathway inhibitor (mTFPI and sTFPI) for treatment of hemophilia. Concizumab displays a non-linear pharmacokinetic (PK) profile due to mTFPI-mediated endocytosis and necessitates a high dose and frequent dosing to suppress the abundant sTFPI, a negative regulator of coagulation. Recycling antibodies that can dissociate bound mTFPI/sTFPI in endosomes for degradation and rescue antibody from degradation have a potential in reducing the dose by extending antibody systemic persistence and sTFPI suppression. We developed a systems PK/pharmacodynamics (PD) model with nested endosome compartments to simulate the effect of decreased antibody binding to mTFPI/sTFPI in endosomes on antibody clearance and sTFPI suppression for exploring the potential of anti-TFPI recycling antibodies in reducing the dose. A dynamic model-building strategy was taken. A reduced PK/PD model without the endosome compartments was developed to optimize unknown target turnover parameters using concizumab PK data. The optimized parameters were then employed in the systems PK/PD model for simulations. The obtained systems PK/PD model adequately described the PK of concizumab in rabbits, monkeys, and humans and the PD in humans. The systems PK/PD model predicted that an anti-TFPI recycling antibody with a 100-fold higher mTFPI/sTFPI dissociation constant in endosomes than concizumab can extend sTFPI suppression from 12 days to 1 month. Thus, the systems PK/PD model provides a quantitative platform for guiding the engineering and translational development of anti-TFPI recycling antibodies., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

46. Performance evaluation of Revohem ™ FVIII chromogenic and Revohem ™ FIX chromogenic in the CS-5100 autoanalyser.

Author

Suzuki A, Suzuki N, Kanematsu T, Shinohara S, Arai N, Kikuchi R, and Matsushita T

Subjects

Automation, Laboratory methods, Blood Coagulation Tests methods, Hemophilia A blood, Hemophilia A diagnosis, Hemophilia A metabolism, Hemophilia B blood, Hemophilia B diagnosis, Hemophilia B metabolism, Humans, Lupus Coagulation Inhibitor blood, Lupus Coagulation Inhibitor metabolism, Reproducibility of Results, Sensitivity and Specificity, von Willebrand Diseases blood, von Willebrand Diseases diagnosis, von Willebrand Diseases metabolism, Automation, Laboratory instrumentation, Blood Coagulation Tests instrumentation, Chromogenic Compounds metabolism, Factor IX metabolism, Factor VIII metabolism

Abstract

Introduction: Chromogenic substrate assay (CSA) reagents Revohem ™ FVIII and Revohem ™ FIX are now available as in vitro diagnostic reagents for autoanalysers in Japan. In this study, we evaluated the performance of these reagents in the CS-5100 automated coagulation analyser., Methods: We assessed within-run and between-day imprecision, on-board stability and frozen-storage stability of Revohem FVIII and FIX. Sensitivity to lupus anticoagulant (LA) was examined using LA-positive patient plasma. Correlations were analysed using plasma samples from normal individuals and patients with haemophilia A (HA) or B (HB) or von Willebrand disease (VWD)., Results: Imprecision was <2% for Revohem FVIII and <6.5% for Revohem FIX. On-board storage of Revohem FVIII resulted in a <10% decrease in FVIII levels from baseline at 24 hours, whereas Revohem FIX showed a >10% decrease at 8 hours. Revohem FVIII showed good stability while frozen for 22 days. Although Revohem FIX showed degradation due to freeze-thawing, a new calibration improved stability up to 22 days. Interference from LA was not observed with Revohem FVIII or FIX. The FVIII CSA-CSA correlation was excellent in normal (r = 0.9924), HA (r = 0.9945) and VWD (r = 0.9914). The FVIII CSA-OSA correlation was good in normal (r = 0.8468) and excellent in HA (r = 0.975) and VWD (r = 0.9936). The FIX CSA-OSA correlation was fair in normal (r = 0.4791) and excellent in HB (r = 0.9501)., Conclusion: Revohem FVIII and FIX both showed excellent performance in the CS-5100 analyser. These reagents could be useful in routine laboratory testing for diagnosing and treating haemophilia., (© 2019 John Wiley & Sons Ltd.)

Published

2019

47. Genetic determinants of VWF clearance and FVIII binding modify FVIII pharmacokinetics in pediatric hemophilia A patients.

Author

Swystun LL, Ogiwara K, Rawley O, Brown C, Georgescu I, Hopman W, Labarque V, Male C, Thom K, Blanchette VS, Carcao MD, and Lillicrap D

Subjects

Adolescent, Blood Coagulation Tests, Child, Factor VIII therapeutic use, Female, Genetic Variation, Genotype, Half-Life, Hemophilia A blood, Hemophilia A drug therapy, Humans, Male, Metabolic Clearance Rate genetics, Protein Binding, Proteolysis, Blood Coagulation genetics, Factor VIII pharmacokinetics, Hemophilia A genetics, Hemophilia A metabolism, von Willebrand Factor genetics, von Willebrand Factor metabolism

Abstract

Factor VIII (FVIII) pharmacokinetic (PK) properties show high interpatient variability in hemophilia A patients. Although previous studies have determined that age, body mass index, von Willebrand factor antigen (VWF:Ag) levels, and ABO blood group status can influence FVIII PK, they do not account for all observed variability. In this study, we aim to describe the genetic determinants that modify the FVIII PK profile in a population of 43 pediatric hemophilia A patients. We observed that VWF:Ag and VWF propeptide (VWFpp)/VWF:Ag, but not VWFpp, were associated with FVIII half-life. VWFpp/VWF:Ag negatively correlated with FVIII half-life in patients with non-O blood type, but no correlation was observed for type O patients, suggesting that von Willebrand factor (VWF) half-life, as modified by the ABO blood group, is a strong regulator of FVIII PK. The FVIII-binding activity of VWF positively correlated with FVIII half-life, and the rare or low-frequency nonsynonymous VWF variants p.(Arg826Lys) and p.(Arg852Glu) were identified in patients with reduced VWF:FVIIIB but not VWF:Ag. Common variants at the VWF , CLEC4M , and STAB2 loci, which have been previously associated with plasma levels of VWF and FVIII, were associated with the FVIII PK profile. Together, these studies characterize the mechanistic basis by which VWF clearance and ABO glycosylation modify FVIII PK in a pediatric population. Moreover, this study is the first to identify non- VWF and non- ABO variants that modify FVIII PK in pediatric hemophilia A patients., (© 2019 by The American Society of Hematology.)

Published

2019

48. Clinical pattern of hemophilia and causes of variability.

Author

Mingot-Castellano ME

Subjects

Blood Coagulation, Factor IX metabolism, Factor VIII metabolism, Hemophilia A metabolism, Hemorrhage blood, Hemorrhage metabolism, Humans, Factor IX analysis, Factor VIII analysis, Hemophilia A blood

Abstract

: In persons with hemophilia, the severity and spontaneity of bleeding episodes depends on the degree of factor deficiency present in the patients. Severe hemophilia is classically characterized by a factor VIII (FVIII) or factor IX (FIX) coagulant activity below 1% of normal (spontaneous and severe bleeds). Moderate hemophilia is associated with factor activity between 1 and 5% of normal (milder spontaneous and traumatic bleeds). Finally, mild hemophilia has factor activity in excess of 5% of normal (traumatic bleeds in general). Nonetheless, this classification is rather simplistic. It is a known fact that there are subjects with identical clotting factor levels who have different bleeding phenotypes. We will analyze different factors to justify this.

Published

2019

49. Direct comparison of two extended-half-life recombinant FVIII products: a randomized, crossover pharmacokinetic study in patients with severe hemophilia A.

Author

Shah A, Solms A, Wiegmann S, Ahsman M, Berntorp E, Tiede A, Iorio A, Mancuso ME, Zhivkov T, and Lissitchkov T

Subjects

Adolescent, Adult, Aged, Cross-Over Studies, Humans, Male, Middle Aged, Factor VIII administration & dosage, Factor VIII pharmacokinetics, Hemophilia A blood, Hemophilia A drug therapy, Hemophilia A metabolism, Polyethylene Glycols administration & dosage, Polyethylene Glycols pharmacokinetics, Recombinant Fusion Proteins administration & dosage, Recombinant Fusion Proteins pharmacokinetics

Abstract

BAY 94-9027 is an extended-half-life, recombinant factor VIII (rFVIII) product conjugated with a 60-kDa branched polyethylene glycol (PEG) molecule indicated for use in previously treated patients (aged ≥ 12 years) with hemophilia A. This randomized, open-label, two-way crossover study compared the pharmacokinetics (PK) of BAY 94-9027 and rFVIII Fc fusion protein (rFVIIIFc) in patients with hemophilia A. Patients aged 18-65 years with FVIII < 1% and ≥ 150 exposure days to FVIII were randomized to receive intravenous single-dose BAY 94-9027 60 IU/kg followed by rFVIIIFc 60 IU/kg or vice versa, with ≥ 7-day wash-out between doses. FVIII activity was measured by one-stage assay. PK parameters, including area under the curve from time 0 to the last data point (AUC last , primary parameter), half-life, and clearance were calculated. Eighteen patients were randomized and treated. No adverse events were observed. In the analysis set excluding one outlier, geometric mean (coefficient of variation [%CV, 95% confidence interval {CI}]) AUC last was significantly higher for BAY 94-9027 versus rFVIIIFc (2940 [37.8, 2440-3550] IU h/dL versus 2360 [31.8, 2010-2770] IU h/dL, p = 0.0001). A population PK model was developed to simulate time to reach FVIII threshold levels; median time to 1 IU/dL was approximately 13 h longer for BAY 94-9027 versus rFVIIIFc after a single infusion of 60 IU/kg. In conclusion, BAY 94-9027 had a superior PK profile versus rFVIIIFc. ClinicalTrials.gov : NCT03364998.

Published

2019

50. Role of factor VIII-binding capacity of endogenous von Willebrand factor in the development of factor VIII inhibitors in patients with severe hemophilia A.

Author

Repessé Y, Costa C, Palla R, Moshai EF, Borel-Derlon A, D'Oiron R, Rothschild C, El-Beshlawy A, Elalfy M, Ramanan V, Eshghi P, Oldenburg J, Pavlova A, Rosendaal FR, Peyvandi F, Kaveri SV, and Lacroix-Desmazes S

Subjects

Alleles, Area Under Curve, Factor VIII therapeutic use, Genotype, Hemophilia A diagnosis, Hemophilia A drug therapy, Humans, Polymorphism, Single Nucleotide, ROC Curve, von Willebrand Factor genetics, Factor VIII adverse effects, Factor VIII metabolism, Hemophilia A immunology, Hemophilia A metabolism, Isoantibodies immunology, von Willebrand Factor metabolism

Published

2019