Your search keyword '"Ragni, Margaret V."' showing total 26 results

1. Lack of factor VIII detection in humans and dogs with an intron 22 inversion challenges hypothesis regarding inhibitor risk.

Author

Vir P, Gunasekera D, Dorjbal B, McDaniel D, Agrawal A, Merricks EP, Ragni MV, Leissinger CA, Stering AI, Lieuw K, Nichols TC, and Pratt KP

Subjects

Humans, Animals, Dogs, RNA, Messenger metabolism, RNA, Messenger genetics, Proteomics methods, Blood Coagulation Factor Inhibitors blood, Blood Coagulation Factor Inhibitors immunology, Chromosome Inversion, Exons, Factor VIII genetics, Factor VIII immunology, Introns, Hemophilia A genetics, Hemophilia A blood, Endothelial Cells metabolism, Liver metabolism

Abstract

Background: Almost half of severe hemophilia A (HA) cases are caused by an intron 22 inversion (Int22Inv) mutation, which truncates the 26-exon F8 messenger RNA (mRNA) after exon 22. Another F8 transcript, F8 B , is initiated from within F8-intron-22. F8 B mRNA consists of a short exon spliced to exons 23 to 26 and is expressed in multiple human cell types. It has been hypothesized that Int22Inv patients have self-tolerance to partial factor (F)VIII proteins expressed from these 2 transcripts. FVIII is expressed in endothelial cells, primarily in the liver and lungs. Several studies have reported FVIII expression in other cell types, although this has been controversial., Objectives: To determine if partial FVIII proteins are expressed from intron 22-inverted and/or F8 B mRNA and if FVIII is expressed in nonendothelial cells., Methods: A panel of FVIII-specific antibodies was validated and employed to label FVIII in cells and tissues and for immunoprecipitation followed by western blots and mass spectrometry proteomics analysis., Results: Immunofluorescent staining localized FVIII to endothelial cells in liver sections from non-HA but not HA-Int22Inv dogs. Neither FVIII nor FVIII B was detected in human peripheral blood mononuclear cells, B cell or T cell lines, or cell lines expanded from peripheral blood mononuclear cells, whereas FVIII antigen and activity were readily detected in primary nonhemophilic liver sinusoidal endothelial cells., Conclusion: If FVIII is expressed in nonendothelial cells or if partial FVIII proteins are expressed in HA-Int22Inv, the concentrations are below the detection limits of these sensitive assays. Our results argue against promotion of immune tolerance through expression of partial FVIII proteins in Int-22Inv patients., Competing Interests: Declaration of competing interests K.P.P. is an inventor on patents related to FVIII immunogenicity. The other authors report no conflicts. The opinions or assertions contained herein are the private ones of the author and are not to be construed as official or reflecting the views of the Department of Defense or the Uniformed Services University of the Health Sciences., (Copyright © 2024 International Society on Thrombosis and Haemostasis. Published by Elsevier Inc. All rights reserved.)

Published

2024

2. Long-term clinical outcomes of prophylaxis with an rFVIIIFc or rFIXFc in adults aged ≥50 years with hemophilia A or B.

Author

Quon D, Jackson S, Alvarez-Román MT, Khan U, Casiano S, Ragni MV, and Rangarajan S

Subjects

Humans, Middle Aged, Aged, Treatment Outcome, Male, Recombinant Fusion Proteins therapeutic use, Female, Immunoglobulin Fc Fragments therapeutic use, Hemophilia A drug therapy, Hemophilia B drug therapy, Factor VIII therapeutic use

Published

2024

3. Multiyear Factor VIII Expression after AAV Gene Transfer for Hemophilia A.

Author

George LA, Monahan PE, Eyster ME, Sullivan SK, Ragni MV, Croteau SE, Rasko JEJ, Recht M, Samelson-Jones BJ, MacDougall A, Jaworski K, Noble R, Curran M, Kuranda K, Mingozzi F, Chang T, Reape KZ, Anguela XM, and High KA

Subjects

Adolescent, Adult, Follow-Up Studies, Genotype, Glucocorticoids adverse effects, Glucocorticoids therapeutic use, Hemophilia A genetics, Hemophilia A prevention & control, Hepatocytes metabolism, Humans, Immunosuppression Therapy, Male, Middle Aged, Young Adult, Dependovirus, Factor VIII genetics, Factor VIII metabolism, Genetic Therapy, Genetic Vectors, Hemophilia A blood

Abstract

Background: The goal of gene therapy for patients with hemophilia A is to safely impart long-term stable factor VIII expression that predictably ameliorates bleeding with the use of the lowest possible vector dose., Methods: In this phase 1-2 trial, we infused an investigational adeno-associated viral (AAV) vector (SPK-8011) for hepatocyte expression of factor VIII in 18 men with hemophilia A. Four dose cohorts were enrolled; the lowest-dose cohort received a dose of 5  × 10 11 vector genomes (vg) per kilogram of body weight, and the highest-dose cohort received 2 × 10 12 vg per kilogram. Some participants received glucocorticoids within 52 weeks after vector administration either to prevent or to treat a presumed AAV capsid immune response. Trial objectives included evaluation of the safety and preliminary efficacy of SPK-8011 and of the expression and durability of factor VIII., Results: The median safety observation period was 36.6 months (range, 5.5 to 50.3). A total of 33 treatment-related adverse events occurred in 8 participants; 17 events were vector-related, including 1 serious adverse event, and 16 were glucocorticoid-related. Two participants lost all factor VIII expression because of an anti-AAV capsid cellular immune response that was not sensitive to immune suppression. In the remaining 16 participants, factor VIII expression was maintained; 12 of these participants were followed for more than 2 years, and a one-stage factor VIII assay showed no apparent decrease in factor VIII activity over time (mean [±SD] factor VIII activity, 12.9±6.9% of the normal value at 26 to 52 weeks when the participants were not receiving glucocorticoids vs. 12.0±7.1% of the normal value at >52 weeks after vector administration; 95% confidence interval [CI], -2.4 to 0.6 for the difference between matched pairs). The participants had a 91.5% reduction (95% CI, 88.8 to 94.1) in the annualized bleeding rate (median rate, 8.5 events per year [range, 0 to 43.0] before vector administration vs. 0.3 events per year [range, 0 to 6.5] after vector administration)., Conclusions: Sustained factor VIII expression in 16 of 18 participants who received SPK-8011 permitted discontinuation of prophylaxis and a reduction in bleeding episodes. No major safety concerns were reported. (Funded by Spark Therapeutics and the National Heart, Lung, and Blood Institute; ClinicalTrials.gov numbers, NCT03003533 and NCT03432520.)., (Copyright © 2021 Massachusetts Medical Society.)

Published

2021

4. Hemophilia as a blueprint for gene therapy.

Author

Ragni MV

Subjects

Humans, Factor IX genetics, Factor VIII genetics, Genetic Therapy, Hemophilia A genetics, Hemophilia A therapy

Abstract

Advances in hemophilia gene therapy could enable progress in other inherited disorders.

Published

2021

5. Factor VIII concentrate dosing with lean body mass, ideal body weight and total body weight in overweight and obesity: A randomized, controlled, open-label, 3 × 3 crossover trial.

Author

Seaman CD, Yabes JG, Lalama CM, and Ragni MV

Subjects

Adult, Body Weight, Cross-Over Studies, Humans, Ideal Body Weight, Male, Obesity complications, Overweight complications, Factor VIII, Hemophilia A drug therapy

Abstract

Introduction: Obesity alters the pharmacokinetic (PK) properties of drugs making it difficult to determine the appropriate dose when administering weight-based medications. Alternative descriptors of body weight, such as lean body mass (LBM) and ideal body weight (IBW), are sometimes used in these situations., Methods: We performed a single-centre, randomized, controlled, open-label, 3 × 3 crossover trial to determine whether recombinant factor VIII (rFVIII) dosing based on LBM and IBW achieves a targeted FVIII recovery with better precision than based on total body weight (TBW) in overweight and obese, adult males with haemophilia A. Participants were randomized to 1 of 6 possible FVIII concentrate dosing sequence scenarios (TBW, LBM and IBW). Recombinant FVIII was administered on 3 separate weeks following a washout period of at least 72 hours., Results: A total of 19 participants were randomized and completed the study. FVIII recovery was lower at 30 minutes post-rFVIII infusion in LBM vs TBW and IBW vs TBW-based dosing, mean difference -0.38 (95% CI: -0.56, -0.20) and -0.28 (95% CI: -0.47, -0.10) IU/dL per IU/kg, respectively. In LBM vs TBW and IBW vs TBW-based dosing, there was a non-significant increase in the proportion of participants with a targeted FVIII recovery of 2.00 ± 0.20 IU/dl per IU/kg, OR = 1.93 (95% CI: 0.44, 8.55) and OR = 3.65 (0.80, 16.72), respectively., Discussion: Based on our study's findings, overweight and obese patients with haemophilia A may benefit from an individualized PK analysis using LBM and IBW to determine the most accurate, and potentially cost-effective, method of achieving targeted FVIII recovery., (© 2021 John Wiley & Sons Ltd.)

Published

2021

6. Exploring the Complex Role of Coagulation Factor VIII in Chronic Liver Disease.

Author

Pradhan-Sundd T, Gudapati S, Kaminski TW, and Ragni MV

Subjects

Animals, Disease Models, Animal, Disease Progression, Down-Regulation, Humans, Biomarkers metabolism, Factor VIII metabolism, Liver Diseases metabolism

Abstract

Chronic liver disease is one of the leading causes of death in the United States. Coagulopathy is often a sequela of chronic liver disease, however, the role and regulation of coagulation components in chronic liver injury remain poorly understood. Clinical and experimental evidence indicate that misexpression of the procoagulant factor VIII (FVIII) is associated with chronic liver disease. Nevertheless, the molecular mechanism of FVIII-induced chronic liver injury progression remains unknown. This review provides evidence supporting a pathologic role for FVIII in the development of chronic liver disease using both experimental and clinical models., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

7. Observational study of recombinant factor VIII-Fc, rFVIIIFc, in hemophilia A.

Author

Ebbert PT, Xavier F, Malec LM, Seaman CD, and Ragni MV

Subjects

Half-Life, Humans, Immune Tolerance, Factor VIII therapeutic use, Hemophilia A drug therapy

Abstract

Introduction: rFVIIIFc (Eloctate) is an extended-half-life recombinant factor VIII-Fc fusion protein that may promote factor VIII (FVIII) tolerance through Fc immunoregulatory properties. Yet, little is known regarding its immunogenicity in patients with hemophilia A (HA) or in HA with inhibitors (HA-I), including tolerized, immune tolerance induction (ITI)-refractory, or ITI-naïve., Methods: We reviewed medical records of 60 patients, including 2 previously-untreated patients (PUPs) and 58 previously-treated patients (PTPs), cared for between 01/01/06 and 06/01/17, on whom anti-FVIII antibody data were available before and after initiating rFVIIIFc. Continuous data were analyzed by student's t-test, and discrete data by chi square or Fisher's exact test., Results: After initiating rFVIIIFc, one of two HA PUPs developed a low-responding (LR) inhibitor after 10 exposures, which resolved (anti-VIII<0.6 B.U.) within 8 additional exposures, while none of 41 HA PTPS developed an inhibitor. Among 19 HA-I PTPs with detectable inhibitors prior to rFVIIIFc, 5 developed an anamnestic response to rFVIIIFc, including 1 of 8 (12.5%) low-responding (LR), and 4 of 9 (44.9%) high-responding (HR), of whom 3 were ITI-naïve and 1 ITI-refractory. Inhibitors resolved in 4 HR within 2 months of continuing rFVIIIFc (median) but persisted in 1 LR at low titer. The remaining 11 HA-I PTPs, including 4 HR and seven LR, had no detectable inhibitor at the time of or after initiating rFVIIIFc., Discussion: rFVIIIFc was immunogenic in HA PUPs and in HA-I PTPs persistently ITI-naïve or ITI-refractory, with inhibitor resolution in the majority. rFVIIIFc immunogenicity appears to be similar to other FVIII products., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

8. 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

9. The national blueprint for future factor VIII inhibitor clinical trials: NHLBI State of the Science (SOS) Workshop on factor VIII inhibitors.

Author

Ragni MV and George LA

Subjects

Genetic Therapy, Health Workforce, Hemophilia A drug therapy, Hemophilia A genetics, Hemophilia A immunology, Humans, Inventions, Clinical Trials as Topic, Education, Factor VIII immunology

Abstract

Introduction: Inhibitor formation is a major complication of haemophilia for which clinical trials are planned. Despite emerging novel haemostatic agents, challenges of rare disease trials are limited subjects and lack of an organized research organization with strategic resources and partnerships., Aim: The charge to Working Group 1 was to establish scientific priorities and innovative implementation strategies to conduct inhibitor prevention and eradication trials. To determine feasibility of trial design and strategic resources and partnerships to be leveraged, two clinical trial concepts were considered., Results: For the Inhibitor Prevention Trial, we considered adaptive design with early stopping rules, dynamic randomization and Master Protocol models to reduce sample size; and registries to provide concurrent controls and natural history data. For the Inhibitor Eradication Trial using gene therapy, an adaptive design was considered in a small number of subjects, and, if safe and meeting regulatory requirements, enrolment would be expanded. A Haemophilia Clinical Trials Group (HCTG) infrastructure was envisioned, with uniform procedures and standardized outcomes, data collection and assays, within which trial concepts would be developed, vetted and prioritized by a Steering Committee, and submitted to NIH and other research sponsors for review and funding. Mechanistic studies would be embedded within the trials, early stage investigators trained and mentored, and the research infrastructure established within the haemophilia centre (HTC) network and supported by partnerships with foundations, community, federal partners and industry., Conclusion: The success of inhibitor trials will depend on innovative trial design and an organized HCTG research infrastructure, leveraged through community partnerships., (Publication 2019. This article is a U.S. Government work and is in the public domain in the USA.)

Published

2019

10. Mimicking Factor VIII to Manage the Factor VIII-Deficient State.

Author

Ragni MV

Subjects

Factor VIII, Hemophilia A

Published

2018

11. Platelet VIII pack evades immune detection.

Author

Ragni MV

Subjects

Animals, Autoantibodies immunology, Blood Coagulation Factor Inhibitors immunology, Blood Platelets immunology, Factor VIII immunology, Hemophilia A immunology, Platelet Transfusion

Abstract

In this issue of Blood, Chen et al demonstrate that platelets expressing factor VIII (FVIII) shield FVIII from immune detection. In the naive FVIII null hemophilia A (HA) mouse, platelet-derived VIII prevents both a primary and memory anti-FVIII immune response, and together with total body irradiation, suppresses anti-FVIII immune response.

Published

2016

12. New and Emerging Agents for the Treatment of Hemophilia: Focus on Extended Half-Life Recombinant Clotting Proteins.

Author

Ragni MV

Subjects

Factor IX administration & dosage, Factor VIII administration & dosage, Half-Life, Hemophilia A metabolism, Humans, Factor IX metabolism, Factor IX therapeutic use, Factor VIII metabolism, Factor VIII therapeutic use, Hemophilia A drug therapy, Recombinant Proteins metabolism

Abstract

Hemophilia A and B are X-linked disorders caused by deficient or defective clotting factor VIII (FVIII) or IX factor (FIX) proteins, and characterized by spontaneous or traumatic bleeding into joints and muscles. Previous use of plasma and plasma-derived clotting factors that lacked appropriate viral inactivation steps in manufacturing led to significant morbidity associated with transfusion-transmitted HIV and hepatitis C virus (HCV). The development of recombinant proteins revolutionized their treatment, and, with no new HIV or HCV infection via clotting proteins for nearly 30 years, greatly improved their lifespan, which now approaches that of the general population, and with the same risks for aging complications. Novel long-acting factor proteins are being licensed to extend FVIII and FIX half-life, thereby reducing infusion frequency and potentially bleed frequency and associated morbidity. Further, novel therapeutics which take advantage of new technologies, including siRNA, monoclonal antibody, and small peptide inhibition technologies, have the potential to simplify treatment and improve outcomes for those with inhibitors.

Published

2015

13. Hepatic stellate cell-conditioned myeloid cells provide a novel therapy for prevention of factor VIII antibody formation in mice.

Author

Bhatt S, Shen GQ, Li Y, Qian S, Ragni MV, and Lu L

Subjects

Animals, Base Sequence, DNA Primers, Mice, Mice, Inbred C57BL, Polymerase Chain Reaction, Autoantibodies biosynthesis, Factor VIII immunology, Hemophilia A immunology, Hepatic Stellate Cells cytology, Myeloid Cells cytology

Abstract

A major complication of factor VIII (F.VIII) infusion therapies for the treatment of hemophilia A is the formation of antibodies (inhibitors) against F.VIII, a T-cell-dependent, B-cell-mediated process. To date, attempts to inhibit formation of the inhibitors have been limited in success. We have shown that hepatic stellate cells (HSCs) promote the development of myeloid-derived suppressor cells (MDSCs). The HSC-induced MDSCs are potent regulators of T-cell and B-cell responses. Here we show that MDSCs can be propagated from hemophilia A mouse bone marrow cells in coculture with HSCs. These cells exhibit a suppressive phenotype and display a marked ability to inhibit T-cell proliferation induced by dendritic cells in response to F.VIII. MDSCs can also inhibit proliferation and activation of B cells stimulated by immunoglobulin M and interleukin 4. Administration of HSC-induced MDSCs induces CD4(+) T cell and B220(+) B-cell hyporesponsiveness to F.VIII and reduces inhibitor formation in hemophilia A mice. These results suggest that MDSCs could serve as a form of immunotherapy for preventing inhibitor formation via induction of immune tolerance., (Copyright © 2015 ISEH - International Society for Experimental Hematology. Published by Elsevier Inc. All rights reserved.)

Published

2015

14. Design of the INHIBIT trial: preventing inhibitors by avoiding 'danger', prolonging half-life and promoting tolerance.

Author

Ragni MV and Malec LM

Subjects

Child, Child, Preschool, Factor VIII administration & dosage, Factor VIII immunology, Half-Life, Humans, Immune Tolerance drug effects, Immunity, Cellular drug effects, Immunoglobulin Fc Fragments administration & dosage, Immunoglobulin Fc Fragments immunology, Recombinant Fusion Proteins administration & dosage, Recombinant Fusion Proteins immunology, T-Lymphocytes drug effects, T-Lymphocytes immunology, Factor VIII therapeutic use, Hemophilia A drug therapy, Immunoglobulin Fc Fragments therapeutic use, Recombinant Fusion Proteins therapeutic use

Abstract

Inhibitor formation is among the most serious complications of hemophilia treatment. With the US FDA licensure of the novel long-lasting recombinant factor VIII (FVIII) Fc fusion protein, Eloctate, which prolongs FVIII half-life, we propose an innovative approach to prevent inhibitor formation. In this paper, we describe a multicenter, Phase II, single-arm, 48-week trial, the INHIBIT trial, to determine if Eloctate, begun before a bleed and continued as once weekly prophylaxis, will reduce inhibitor formation in children with hemophilia A. We hypothesize that avoiding 'danger,' that is, immune activation by a bleed at first factor exposure and prolonging FVIII half-life will prevent inhibitors and promote FVIII-specific T-cell tolerance. If successful, this approach will suggest a new paradigm in clinical practice.

Published

2014

15. Factor VIII brand and immunogenicity.

Author

Ragni MV

Subjects

Humans, Male, Factor VIII immunology, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemophilia A epidemiology, Hemophilia A immunology, Isoantibodies blood

Published

2014

16. Phase 3 study of recombinant factor VIII Fc fusion protein in severe hemophilia A.

Author

Mahlangu J, Powell JS, Ragni MV, Chowdary P, Josephson NC, Pabinger I, Hanabusa H, Gupta N, Kulkarni R, Fogarty P, Perry D, Shapiro A, Pasi KJ, Apte S, Nestorov I, Jiang H, Li S, Neelakantan S, Cristiano LM, Goyal J, Sommer JM, Dumont JA, Dodd N, Nugent K, Vigliani G, Luk A, Brennan A, and Pierce GF

Subjects

Adolescent, Adult, Aged, Child, Drug Administration Schedule, Factor VIII pharmacokinetics, Hemorrhage drug therapy, Hemorrhage prevention & control, Humans, Male, Middle Aged, Recombinant Fusion Proteins pharmacokinetics, Time Factors, Treatment Outcome, Young Adult, Factor VIII therapeutic use, Hemophilia A drug therapy, Immunoglobulin Fc Fragments therapeutic use, Recombinant Fusion Proteins therapeutic use

Abstract

This phase 3 pivotal study evaluated the safety, efficacy, and pharmacokinetics of a recombinant FVIII Fc fusion protein (rFVIIIFc) for prophylaxis, treatment of acute bleeding, and perioperative hemostatic control in 165 previously treated males aged ≥12 years with severe hemophilia A. The study had 3 treatment arms: arm 1, individualized prophylaxis (25-65 IU/kg every 3-5 days, n = 118); arm 2, weekly prophylaxis (65 IU/kg, n = 24); and arm 3, episodic treatment (10-50 IU/kg, n = 23). A subgroup compared recombinant FVIII (rFVIII) and rFVIIIFc pharmacokinetics. End points included annualized bleeding rate (ABR), inhibitor development, and adverse events. The terminal half-life of rFVIIIFc (19.0 hours) was extended 1.5-fold vs rFVIII (12.4 hours; P < .001). Median ABRs observed in arms 1, 2, and 3 were 1.6, 3.6, and 33.6, respectively. In arm 1, the median weekly dose was 77.9 IU/kg; approximately 30% of subjects achieved a 5-day dosing interval (last 3 months on study). Across arms, 87.3% of bleeding episodes resolved with 1 injection. Adverse events were consistent with those expected in this population; no subjects developed inhibitors. rFVIIIFc was well-tolerated, had a prolonged half-life compared with rFVIII, and resulted in low ABRs when dosed prophylactically 1 to 2 times per week.

Published

2014

17. von Willebrand factor: factor VIII protector and friend.

Author

Ragni MV

Subjects

Animals, Humans, Factor VIII antagonists & inhibitors, Factor VIII chemistry, von Willebrand Factor chemistry

Published

2012

18. Safety and prolonged activity of recombinant factor VIII Fc fusion protein in hemophilia A patients.

Author

Powell JS, Josephson NC, Quon D, Ragni MV, Cheng G, Li E, Jiang H, Li L, Dumont JA, Goyal J, Zhang X, Sommer J, McCue J, Barbetti M, Luk A, and Pierce GF

Subjects

Adult, Dose-Response Relationship, Drug, Factor VIII administration & dosage, Factor VIII adverse effects, Half-Life, Hemophilia A blood, Hemophilia A metabolism, Humans, Immunoglobulin Fc Fragments administration & dosage, Immunoglobulin Fc Fragments adverse effects, Infusion Pumps, Male, Metabolic Clearance Rate, Middle Aged, Receptors, Fc administration & dosage, Receptors, Fc metabolism, Recombinant Fusion Proteins administration & dosage, Recombinant Fusion Proteins adverse effects, Time Factors, Young Adult, von Willebrand Factor analysis, Factor VIII pharmacokinetics, Factor VIII therapeutic use, Hemophilia A drug therapy, Immunoglobulin Fc Fragments therapeutic use, Receptors, Fc therapeutic use, Recombinant Fusion Proteins pharmacokinetics, Recombinant Fusion Proteins therapeutic use

Abstract

Current factor VIII (FVIII) products display a half-life (t(1/2)) of ∼ 8-12 hours, requiring frequent intravenous injections for prophylaxis and treatment of patients with hemophilia A. rFVIIIFc is a recombinant fusion protein composed of a single molecule of FVIII covalently linked to the Fc domain of human IgG(1) to extend circulating rFVIII t(1/2). This first-in-human study in previously treated subjects with severe hemophilia A investigated safety and pharmacokinetics of rFVIIIFc. Sixteen subjects received a single dose of rFVIII at 25 or 65 IU/kg followed by an equal dose of rFVIIIFc. Most adverse events were unrelated to study drug. None of the study subjects developed anti-rFVIIIFc antibodies or inhibitors. Across dose levels, compared with rFVIII, rFVIIIFc showed 1.54- to 1.70-fold longer elimination t(1/2), 1.49- to 1.56-fold lower clearance, and 1.48- to 1.56-fold higher total systemic exposure. rFVIII and rFVIIIFc had comparable dose-dependent peak plasma concentrations and recoveries. Time to 1% FVIII activity above baseline was ∼ 1.53- to 1.68-fold longer than rFVIII across dose levels. Each subject showed prolonged exposure to rFVIIIFc relative to rFVIII. Thus, rFVIIIFc may offer a viable therapeutic approach to achieve prolonged hemostatic protection and less frequent dosing in patients with hemophilia A. This trial was registered at www.clinicaltrials.gov as NCT01027377.

Published

2012

19. Rationale for a randomized controlled trial comparing two prophylaxis regimens in adults with severe hemophilia A: the Hemophilia Adult Prophylaxis Trial.

Author

Ragni MV

Subjects

Adult, Drug Administration Schedule, Factor VIII genetics, Factor VIII metabolism, Hemophilia A economics, Hemorrhage prevention & control, Humans, Joints blood supply, Male, Quality of Life, Range of Motion, Articular, Recombinant Proteins genetics, Recombinant Proteins metabolism, Recombinant Proteins therapeutic use, Factor VIII therapeutic use, Hemophilia A drug therapy

Abstract

A major goal of comprehensive hemophilia care is to prevent occurrence of bleeds by prophylaxis or regular preventive factor, one or more times weekly. Although prophylaxis is effective in reducing bleeding and joint damage in children, whether it is necessary to continue into adulthood is not known. The purpose of this article is to describe a Phase III randomized controlled trial to evaluate prophylaxis comparing two dose regimens in adults with severe hemophilia A. I hypothesize that adults with mature cartilage and joints are less susceptible to joint bleeds and joint damage, and that once-weekly recombinant factor VIII prophylaxis, with up to two rescue doses per week, is as effective as thrice-weekly prophylaxis in reducing bleeding frequency, but less costly and more acceptable, with higher quality of life. The ultimate goal of this project is to determine whether once-weekly prophylaxis is any worse than thrice-weekly prophylaxis in reducing joint bleeding frequency, while potentially utilizing less factor, at lower cost, leading to a better quality of life. This is an innovative concept, as it challenges the current paradigm of thrice-weekly prophylaxis in adults, which is based on dosing in children. Furthermore, this trial will assess interdose thrombin generation, a novel tissue factor-based assay of hemostasis, to determine if individualized thrombin generation can predict more individualized prophylaxis dosing, which would be practice changing.

Published

2011

20. FVIII, CD4, and liaisons dangereuses.

Author

Ragni MV

Subjects

Adolescent, Adult, Age Factors, Child, Child, Preschool, Databases, Factual, Female, HIV Seropositivity blood, HIV Seropositivity epidemiology, HIV Seropositivity therapy, Hemophilia A epidemiology, Hemophilia A therapy, Humans, Incidence, Male, Retrospective Studies, Risk Factors, United Kingdom epidemiology, Blood Coagulation Factor Inhibitors blood, Factor VIII antagonists & inhibitors, Hemophilia A blood

Published

2011

21. Factor VIII-pulsed dendritic cells reduce anti-factor VIII antibody formation in the hemophilia A mouse model.

Author

Ragni MV, Wu W, Liang X, Hsieh CC, Cortese-Hassett A, and Lu L

Subjects

Animals, Antibodies blood, Cytokines blood, Disease Models, Animal, Factor VIII administration & dosage, Lymphocyte Activation, Mice, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Regulatory immunology, Thymidine pharmacokinetics, Antibody Formation, Dendritic Cells immunology, Factor VIII immunology, Hemophilia A immunology

Abstract

Objective: Hemophilia inhibitor formation is a T-cell-dependent immune response to infused factor VIII (F.VIII). As immature dendritic cells (DCre) regulate immune response and promote tolerance, we evaluated F.VIII-pulsed DCre, propagated from bone marrow in the presence of granulocyte-macrophage colony-stimulating factor and transforming growth factor-beta, in achieving F.VIII tolerance., Materials and Methods: The effects of intravenous F.VIII-pulsed DCre in C57BL/6 hemophilia A mice were determined by total F.VIII inhibitory antibodies, T-cell proliferation, thymidine uptake, cytokine profile, and surface molecule expression., Results: After tail vein injection of 2.5 U recombinant F.VIII (rF.VIII) on day 0, 2, and 4, anti-F.VIII antibody peaked on day 6, and increased further on day 17 following rF.VIII rechallenge on day 12, 14, and 16, with increased T-cell proliferative response to in vitro F.VIII. When mice were pretreated with 2 x 10(6) F.VIII-pulsed immature DCre (deficient nuclear factor-kappaB nuclear protein binding, low CD80, low CD86, high interleukin [IL]-10 phenotype) 7 days before rF.VIII challenge, anti-F.VIII was reduced on day 6 and on day 8, 0.1 +/- 0.0 (Bethesda units/mL) vs control phosphate-buffered saline-treated hemophilia A mice, 2.0 +/- 0.1 Bethesda units/mL, p < 0.01. Rechallenge with rF.VIII on day 12 produced no increase in anti-F.VIII antibody response. This was associated with high serum IL-10 and low IL-2 levels by enzyme-linked immunosorbent assay, and splenic T-cell hyporesponsiveness to F.VIII, with IL-10 production, high FoxP3 expression by quantitative polymerase chain reaction, and T regulatory cell expansion, confirmed in ovalbumin-T-cell receptor transgenic mice., Conclusions: These findings suggest F.VIII-pulsed DCre reduce anti-F.VIII antibody formation in hemophilia A mice by induction of regulatory T-cell-mediated hyporesponsiveness of T-helper cells to F.VIII.

Published

2009

22. Extrahepatic factor VIII production in transplant recipient of hemophilia donor liver.

Author

Madeira CL, Layman ME, de Vera RE, Fontes PA, and Ragni MV

Subjects

Aged, Humans, Liver metabolism, Liver Cirrhosis, Alcoholic therapy, Male, Middle Aged, Factor VIII biosynthesis, Hemophilia A, Liver Transplantation

Published

2009

23. Phase 1 trial of FVIII gene transfer for severe hemophilia A using a retroviral construct administered by peripheral intravenous infusion.

Author

Powell JS, Ragni MV, White GC 2nd, Lusher JM, Hillman-Wiseman C, Moon TE, Cole V, Ramanathan-Girish S, Roehl H, Sajjadi N, Jolly DJ, and Hurst D

Subjects

Adolescent, Adult, DNA, Viral analysis, Factor VIII metabolism, Genetic Vectors adverse effects, Genetic Vectors pharmacokinetics, Humans, Infusions, Intravenous, Leukocytes, Mononuclear physiology, Male, Middle Aged, Severity of Illness Index, Factor VIII genetics, Genetic Therapy, Genetic Vectors administration & dosage, Hemophilia A therapy, Retroviridae genetics

Abstract

In a phase 1 dose escalation study, 13 subjects with hemophilia A received by peripheral intravenous infusion a retroviral vector carrying a B-domain-deleted human factor VIII (hFVIII) gene. Infusions were well tolerated. Tests for replication competent retrovirus have been negative. Polymerase chain reaction (PCR) analyses demonstrate the persistence of vector gene sequences in peripheral blood mononuclear cells in 3 of 3 subjects tested. Factor VIII was measured in serial samples using both a one-stage clotting assay and a chromogenic assay. While no subject had sustained FVIII increases, 9 subjects had FVIII higher than 1% on at least 2 occasions 5 or more days after infusion of exogenous FVIII, with isolated levels that ranged from 2.3% to 19%. Pharmacokinetic parameters of exogenous FVIII infused into subjects 13 weeks after vector infusion showed an increased half-life (T1/2; P <.02) and area under the curve (AUC, P <.04) compared with prestudy values. Bleeding frequency decreased in 5 subjects compared with historical rates. These results demonstrate that this retroviral vector (hFVIII(V)) is safe and, in some subjects, persists more than a year in peripheral blood mononuclear cells, with measurable factor VIII levels and with increased available FVIII activity (increased T1/2 and AUC) after infusion of exogenous FVIII concentrate.

Published

2003

24. Safety of the new generation recombinant factor concentrates.

Author

Schlesinger KW and Ragni MV

Subjects

Factor VIIa, Female, Humans, Male, Factor IX adverse effects, Factor IX economics, Factor IX therapeutic use, Factor VII adverse effects, Factor VII economics, Factor VII therapeutic use, Factor VIII adverse effects, Factor VIII economics, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemophilia A genetics, Hemophilia A physiopathology, Hemophilia B drug therapy, Hemophilia B genetics, Hemophilia B physiopathology, Recombinant Proteins adverse effects, Recombinant Proteins economics, Recombinant Proteins therapeutic use

Abstract

Haemophilia A and B are X-linked disorders resulting from deficiency of Factor VIII and IX, respectively. Clinical sequellae of Factor VIII or IX deficiency include spontaneous and traumatic haemorrhages into joints, soft tissues, and muscles. The cornerstone of therapy has been replacement of the deficient factor, historically with pooled-plasma derivatives. The unfortunate blood-borne infection transmission (such as HIV, hepatitis B and C viruses), inhibitor formation, immunosuppression, and, in certain cases, thrombosis by these products has spawned major advances and innovations in the manufacture of clotting products. Recombinant technology has virtually eliminated transmissible disease risk; yet, the presence of albumin in second and third generation recombinant products raises, at the least, theoretical risk of prions and parvovirus B19. Other non-infectious complications, including inhibitor formation, allergic reactions, and thrombosis, remain formidable concerns. Despite this, recombinant factors remain the most attractive treatment approach for haemophilia. Future improvement awaits the development of safe and effective gene transfer technology.

Published

2002

25. Hemophilia A subjects with an intron-22 gene inversion mutation show CD4+ T-effector responses to multiple epitopes in FVIII.

Author

Gunasekera, Devi, Vir, Pooja, Karim, Ahmad Faisal, Ragni, Margaret V., and Pratt, Kathleen P.

Subjects

MONONUCLEAR leukocytes, GENETIC mutation, EPITOPES, BLOOD coagulation factor VIII antibodies, HEMOPHILIA

Abstract

Background: Almost half of severe hemophilia A (HA) is caused by an intron 22 inversion mutation (Int22Inv), which disrupts the 26-exon F8 gene. Inverted F8 mRNA exons 1-22 are transcribed, while F8B mRNA, containing F8 exons 23-26, is transcribed from a promoter within intron 22. Neither FVIII activity nor FVIII antigen (cross-reacting material, CRM) are detectable in plasma of patients with an intron-22 inversion. Objectives: To test the hypothesis that (putative) intracellular synthesis of FVIII proteins encoded by inverted F8 and F8B mRNAs confers T-cell tolerance to almost the entire FVIII sequence, and to evaluate the immunogenicity of the region encoded by the F8 exon 22-23 junction sequence. Patients/Methods: Peripheral blood mononuclear cells (PBMCs) from 30 severe or moderate HA subjects (17 with an Int22Inv mutation) were tested by ELISPOT assays to detect cytokine secretion in response to FVIII proteins and peptides and to map immunodominant T-cell epitopes. Potential immunogenicity of FVIII sequences encoded by the F8 exon 22-23 junction region was also tested using peptide-MHCII binding assays. Results: Eight of the Int22Inv subjects showed robust cytokine secretion from PBMCs stimulated with FVIII proteins and/or peptides, consistent with earlier publications from the Conti-Fine group. Peptide ELISPOT assays identified immunogenic regions of FVIII. Specificity for sequences encoded within F8 mRNA exons 1-22 and F8B mRNA was confirmed by staining Int22Inv CD4+ T cells with peptide-loaded HLA-Class II tetramers. FVIII peptides spanning the F8 exon 22-23 junction (encoding M2124-V2125) showed limited binding to MHCII proteins and low immunogenicity, with cytokine secretion from only one Int22Inv subject. Conclusions: PBMCs from multiple subjects with an Int22Inv mutation, with and without a current FVIII inhibitor, responded to FVIII epitopes. Furthermore, the FVIII region encoded by the exon 22-23 junction sequence was not remarkably [ABSTRACT FROM AUTHOR]

Published

2023

26. Gene Therapy for Bleeding Disorders

Author

Monahan, Paul E., Abajas, Yasmina L., Abutalib, Syed A., editor, Connors, Jean M., editor, and Ragni, Margaret V., editor

Published

2016