Your search keyword '"Muchitsch EM"' showing total 5 results

1. The biological efficacy profile of BAX 855, a PEGylated recombinant factor VIII molecule.

Author

Valentino LA, Cong L, Enockson C, Song X, Scheiflinger F, Muchitsch EM, Turecek PL, and Hakobyan N

Subjects

Animals, Disease Models, Animal, Hemorrhage prevention & control, Humans, Mice, Recombinant Proteins administration & dosage, Factor VIII administration & dosage, Hemophilia A drug therapy

Abstract

Prophylaxis prevents joint and other bleeding episodes in patients with haemophilia A. Development of new factor concentrates with longer circulating half-lives may encourage patients to start, continue or resume prophylaxis. The aim of this study was to compare the pharmacodynamic effect of a PEGylated full-length recombinant factor VIII (rFVIII) concentrate with that of an unmodified rFVIII concentrate with respect to the duration of prophylactic efficacy in a murine model of haemophilic joint bleeding. Mice were pretreated with BAX 855 or unmodified rFVIII at specified times before right knee puncture to induce haemarthrosis; left knee joints served as controls. Joint bleeding was evaluated using a combination of visual and histological assessments. Administration of a single dose of unmodified rFVIII before joint puncture prevented haemarthrosis in mice up to 24 h, whereas pretreatment with BAX 855 protected the joint from bleeding up to 48 h. This pharmacodynamic study showed prolonged efficacy of BAX 855 compared to ADVATE in a haemophilia A mouse joint bleeding model. This finding supports the possibility of using BAX 855 to increase FVIII trough levels and/or extend the dosing interval in patients with haemophilia A on prophylaxis, which may potentially improve prophylactic efficacy and long-term adherence., (© 2014 John Wiley & Sons Ltd.)

Published

2015

2. BAX 855, a PEGylated rFVIII product with prolonged half-life. Development, functional and structural characterisation.

Author

Turecek PL, Bossard MJ, Graninger M, Gritsch H, Höllriegl W, Kaliwoda M, Matthiessen P, Mitterer A, Muchitsch EM, Purtscher M, Rottensteiner H, Schiviz A, Schrenk G, Siekmann J, Varadi K, Riley T, Ehrlich HJ, Schwarz HP, and Scheiflinger F

Subjects

Dose-Response Relationship, Drug, Drug Stability, Factor VIII pharmacokinetics, Half-Life, Hemophilia A metabolism, Humans, Recombinant Proteins administration & dosage, Recombinant Proteins chemistry, Recombinant Proteins pharmacokinetics, Drug Design, Factor VIII administration & dosage, Factor VIII chemistry, Hemophilia A drug therapy, Liposomes chemistry, Polyethylene Glycols chemistry

Abstract

A longer acting recombinant FVIII is expected to serve patients' demand for a more convenient prophylactic therapy. We have developed BAX 855, a PEGylated form of Baxter's rFVIII product ADVATE™ based on the ADVATE™ manufacturing process. The conjugation process for preparing BAX 855 uses a novel PEG reagent. The production process was adjusted to yield a rFVIII conjugate with a low PEGylation degree of about 2 moles PEG per FVIII molecule. This optimised modification degree resulted in an improved PK profile for rFVIII without compromising its specific activity. PEGylation sites were identified by employing various HPLC- and MS-based methods. These studies not only indicated that about 60% of the PEG chains are localised to the B-domain, which is cleaved off upon physiological activation during the coagulation process, but also demonstrated an excellent lot to lot consistency with regard to PEGylation site distribution. Detailed biochemical characterization further showed that PEGylated FVIII retained all the physiological functions of the FVIII molecule with the exception of binding to the LRP clearance receptor which was reduced for BAX 855 compared to ADVATE™. This might provide an explanation for the prolonged circulation time of BAX 855 as reduced receptor binding might slow-down clearance. Preclinical studies showed improved pharmacokinetic behaviour and clinically relevant prolonged efficacy compared to ADVATE™ without any signs of toxicity or elevated immunogenicity. The comprehensive preclinical data package formed the basis for approval of the phase 1 clinical study by European authorities which started in 2011.

Published

2012

3. Maintenance and break of immune tolerance against human factor VIII in a new transgenic hemophilic mouse model.

Author

van Helden PM, Unterthurner S, Hermann C, Schuster M, Ahmad RU, Schiviz AN, Weiller M, Antoine G, Turecek PL, Muchitsch EM, Schwarz HP, and Reipert BM

Subjects

Animals, Antibody Formation genetics, Antibody Formation physiology, Disease Models, Animal, Factor VIII antagonists & inhibitors, Female, Hemophilia A immunology, Hemophilia A pathology, Humans, Immune Tolerance physiology, Immunologic Memory physiology, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Models, Biological, Species Specificity, Factor VIII genetics, Factor VIII immunology, Hemophilia A genetics, Immune Tolerance genetics, Immunologic Memory genetics

Abstract

Replacement of the missing factor VIII (FVIII) is the current standard of care for patients with hemophilia A. However, the short half-life of FVIII makes frequent treatment necessary. Current efforts focus on the development of longer-acting FVIII concentrates by introducing chemical and genetic modifications to the protein. Any modification of the FVIII protein, however, risks increasing its immunogenic potential to induce neutralizing antibodies (FVIII inhibitors), and this is one of the major complications in current therapy. It would be highly desirable to identify candidates with a high risk for increased immunogenicity before entering clinical development to minimize the risk of exposing patients to such altered FVIII proteins. In the present study, we describe a transgenic mouse line that expresses a human F8 cDNA. This mouse is immunologically tolerant to therapeutic doses of native human FVIII but is able to mount an antibody response when challenged with a modified FVIII protein that possesses altered immunogenic properties. In this situation, immunologic tolerance breaks down and antibodies develop that recognize both the modified and the native human FVIII. The applicability of this new model for preclinical immunogenicity assessment of new FVIII molecules and its potential use for basic research are discussed.

Published

2011

4. Modulation of factor VIII-specific memory B cells.

Author

Reipert BM, Allacher P, Hausl C, Pordes AG, Ahmad RU, Lang I, Ilas J, Windyga J, Klukowska A, Muchitsch EM, and Schwarz HP

Subjects

Adolescent, Adult, Animals, Antibodies immunology, Antigens, CD immunology, B-Lymphocytes cytology, CD40 Ligand immunology, Cell Differentiation, Child, Factor VIII administration & dosage, Factor VIII antagonists & inhibitors, Hemophilia A therapy, Humans, Lymphocyte Activation immunology, Mice, Spleen cytology, Spleen immunology, Young Adult, B-Lymphocytes immunology, Factor VIII immunology, Hemophilia A immunology, Immunologic Memory immunology

Abstract

The development of inhibitory antibodies against factor VIII (FVIII) is the major complication in patients with haemophilia A who are treated with FVIII products. Memory B cells play an essential role in maintaining established antibody responses. Upon re-exposure to the same antigen, they are rapidly re-stimulated to proliferate and differentiate into antibody-secreting plasma cells (ASC) that secrete high-affinity antibodies. It is, therefore, reasonable to believe that memory B cells have to be eradicated or inactivated for immune tolerance induction therapy to be successful in patients with haemophilia A and FVIII inhibitors. The aim of our studies was the development of strategies to prevent FVIII-specific memory B cells from becoming re-stimulated. We established a 6-day in vitro culture system that enabled us to study the regulation of FVIII-specific murine memory-B-cell re-stimulation. We tested the impact of the blockade of co-stimulatory interactions, of different concentrations of FVIII and of ligands for toll-like receptors (TLR). The blockade of B7-CD28 and CD40-CD40 ligand interactions prevented FVIII-specific murine memory B cells from becoming re-stimulated by FVIII in vitro and in vivo. Furthermore, high concentrations of FVIII blocked re-stimulation of FVIII-specific murine memory B cells. Triggering of TLR7 amplified re-stimulation by low concentrations of FVIII and prevented blockade by high concentrations of FVIII. We conclude that we defined modulators that either amplify or inhibit the re-stimulation of FVIII-specific murine memory B cells. Currently, we are investigating whether the same modulators operate in patients with haemophilia A and FVIII inhibitors.

Published

2010

5. Phenotypic expression of murine hemophilia.

Author

Muchitsch EM, Turecek PL, Zimmermann K, Pichler L, Auer W, Richter G, Gritsch H, and Schwarz HP

Subjects

Animals, Mice, Mice, Inbred C57BL, Factor VIII genetics, Hemophilia A genetics, Hemophilia A physiopathology, Mice, Knockout

Published

1999