Production Processes of Licensed Recombinant Factor VIII Preparations

Berthold G. D Boedeker

doi:10.1055/s-2001-16891

Seminars in Thrombosis and Hemostasis, Inhaltsverzeichnis

Semin Thromb Hemost 2001; 27(4): 385-394
DOI: 10.1055/s-2001-16891

Production Processes of Licensed Recombinant Factor VIII Preparations

Berthold G. D. Boedeker

¹BAYER AG, Wuppertal, Germany

Abstract

ABSTRACT

The state-of-the-art treatment for hemophilia A is replacement therapy with recombinant factor VIII (rFVIII) made possible by genetic engineering advances. Currently, there are four different products licensed and available for hemophilia A patients. All are produced by recombinant mammalian cells in large-scale fermenter cultures, purified to high purity, formulated in stable formulations and freeze dried. The first-generation products Recombinate® and Kogenate® (also sold as Helixate® by Aventis) are characterized as full-length human factor VIII molecules and formulated using human serum albumin as a stabilizer. The second-generation product ReFacto® contains an improved albumin-free sucrose formulation and incorporates advanced antiviral safety procedures in the manufacturing process. It is a truncated B region-deleted form of factor VIII (FVIII) that makes use of a nonhuman peptide linker 14 amino acids in length to connect the 80 and 90 kD subunits. The most recently licensed rFVIII product is the second-generation Kogenate product called KOGENATE®Bayer/Kogenate® FS, which combines the advantages of the human full-length FVIII molecule with an albumin-free, sucrose-based synthetic formulation as well as an improved viral safety profile. In this article, the manufacturing processes for each of the four different products are discussed in detail, focusing on expression systems and cell lines, culture medium, technical culture systems, purification process (including viral removal potential), and final formulation.

KEYWORD

Mammalian cell culture - virus safety - Helixate® - Kogenate® - KOGENATE® - Bayer/Kogenate® - FS - Recombinate® - ReFacto®

Volltext

Referenzen

REFERENCES

1 Kogenate® Product Monograph, Bayer, 1993.
2 Recombinate® Product Monograph, Baxter Hyland, 1992.
3 ReFacto® Product Monograph, Wyeth-Ayerst (Genetic Institute), 1999.
4 KOGENATE® Bayer Product Monograph, Bayer, 2000.
5 Harmening, D M. Clinical Hematology and Fundamentals, 2nd ed. Philadelphia: FA Davis; 1992;0:415-438 .
6 Vehar G A, Keyt B, Eaton D. Structure of human factor VIII. Nature . 1984; 312 337-342
7 Toole J J, Knopf J L, Wozney J M. Molecular cloning of a cDNA encoding human anithemophilic factor. Nature . 1984; 312 342-347
8 White G C, Shoemaker C B. Factor VIII gene and hemophilia A. Blood . 1989; 73 1-12
9 Wood W I, Capon D J, Simonsen C C. Expression of active human factor VIII from recombinant DNA clones. Nature . 1984; 312 330-337
10 Boedeker B GD. The manufacturing of recombinant factor VIII, Kogenate®. Trans Med Rev . 1992; 6 256-260
11 Gomperts E, Lundblad R, Adamson R. The manufacturing of recombinant factor VIII, Recombinate®. Trans Med Rev . 1992; 6 247-251
12 Boedeker B GD, Newcomb R, Yuan P, et. Production of recombinant factor VIII from perfusion cultures: I Large scale fermentation. In: Spier RE, Griffiths JB, Berthold W, eds. Animal Cell Technology: Products of Today, Prospects of Tomorrow Oxford, England: Butterworth-Heinemann 1994: 580-583
13 Boedeker B GD, Potere E, Dove G. Production of recombinant factor VIII from perfusion cultures: II Large scale purification. In: Spier RE, Griffiths JB, Berthold W, eds. Animal Cell Technology: Products of Today, Prospects of Tomorrow Oxford, England: Butterworth-Heinemann 1994: 584-587
14 Horowitz B, Horowitz B, Wiebe M E. Inactivation of viruses in labile blood derivatives: disruption of lipid-enveloped viruses by tri(n-butyl)phosphate detergent combination.Transfusion . 1985; 25 516-522
15 Arnold D. Virus safety considerations for recombinant factor VIII (rFVIII, Kogenate®). Haemophilia . 1995; 1(Suppl 2) 22-23
16 Kaufman R J. Insight into the structure, function and biosynthesis of factor VIII through recombinant DNA technology. Ann Hematol . 1991; 63 155-165
17 Adamson R. Design and operation of a recombinant mammalian cell manufacturing process. Ann Hematol . 1994; 68 S9-S14
18 Kaufmann R J, Wasley L C, Davis M V. Effect of von Willebrand factor coexpression on the synthesis and secretion of factor VIII in CHO cells. Mol Cell Biol . 1989; 9 1233-1242
19 Koplove H M. Cell culture and purification process-purity and safety testing. Ann Hematol . 1994; 68 S15-S20
20 Lawrence J. Recombinate®: viral safety and final product manufacturing testing and specifications. Ann Hematol . 1994; 68 S21-S24
21 Lind P, Larsson K, Spira J. Novel forms of B-domain-deleted recombinant factor VIII molecules. Construction and biochemical characterization. Eur J Biochem . 1995; 232 19-27
22 Berntrop E. Second generation, B-domain deleted recombinant factor VIII. Thromb Haemost . 1997; 78 256-260
23 Österberg T, Fatouros A, Mikaelsson M. Development of a freeze-dried albumin-free formulation for recombinant factor VIII SQ. Pharm Res . 1997; 14 892-898
24 Pollmann H, Aledort L. Albumin-free formulated recombinant factor VIII preparations-how big a step forward?. Thromb Haemost . 1999; 82 1370-1371
25 Snyder M, Carrillo R, Frankenberg R. New manufacturing process for recombinant antihemophilic factor (rFVIII). Thromb Haemost . 1997; 78(Suppl) 509 Abstract
26 Nayar R, Wang D Q, Temple S. Recombinate Kogenate® formulation development. Thromb Haemost . 1997; 78(Suppl) 509 Abstract
27 Abshire T C, Brackmann H H, Scharrer I. Sucrose formulated recombinant human antihemophilic factor VIII is safe and efficacious for treatment of hemophilia A in home therapy. Thromb Haemost . 2000; 83 811-816