Your search keyword '"Schiviz A"' showing total 4 results

1. BAX 855, a PEGylated rFVIII product with prolonged half-life

Author

W. Höllriegl, Jürgen Siekmann, P. Matthiessen, E.-M. Muchitsch, Katalin Varadi, Herbert Gritsch, Gerald Schrenk, Peter Turecek, Artur Mitterer, Friedrich Scheiflinger, A. Schiviz, Hartmut J. Ehrlich, Hans-Peter Prof. Schwarz, M. J. Bossard, M. Graninger, Martin Kaliwoda, M. Purtscher, T. Riley, and Hanspeter Rottensteiner

Subjects

Chemistry, Immunogenicity, Hematology, Pharmacology, law.invention, Pharmacokinetics, law, Toxicity, Immunology, PEG ratio, PEGylation, Recombinant DNA, Distribution (pharmacology), Conjugate

Abstract

SummaryA 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

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

Author

P L, Turecek, M J, Bossard, M, Graninger, H, Gritsch, W, Höllriegl, M, Kaliwoda, P, Matthiessen, A, Mitterer, E-M, Muchitsch, M, Purtscher, H, Rottensteiner, A, Schiviz, G, Schrenk, J, Siekmann, K, Varadi, T, Riley, H J, Ehrlich, H P, Schwarz, and F, Scheiflinger

Subjects

Factor VIII, Dose-Response Relationship, Drug, Drug Stability, Drug Design, Liposomes, Humans, Hemophilia A, Recombinant Proteins, Half-Life, Polyethylene Glycols

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. BAX 855, a PEGylated rFVIII product with prolonged half-life

Author

Bossard, M. J., primary, Graninger, M., primary, Gritsch, H., primary, Höllriegl, W., primary, Kaliwoda, M., primary, Matthiessen, P., primary, Mitterer, A., primary, Muchitsch, E.-M., primary, Purtscher, M., primary, Rottensteiner, H., primary, Schiviz, A., primary, Schrenk, G., primary, Siekmann, J., primary, Varadi, K., primary, Riley, T., primary, Ehrlich, H. J., primary, Schwarz, H. P., primary, Scheiflinger, F., primary, and Turecek, P. L., additional

Published

2012

4. BAX 855, a PEGylated rFVIII product with prolonged half-life

Author

Turecek, P. L., Bossard, M. J., Graninger, M., Gritsch, H., Höllriegl, W., Kaliwoda, M., Matthiessen, P., Mitterer, A., Muchitsch, E.-M., Purtscher, M., Rottensteiner, H., Schiviz, A., Schrenk, G., Siekmann, J., Varadi, K., Riley, T., Ehrlich, H. J., Schwarz, H. P., and Scheiflinger, F.

Published

2012