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Merck

Characterization of protein unable to bind von Willebrand factor in recombinant factor VIII products.

Journal of thrombosis and haemostasis : JTH (2021-02-03)
Haarin Chun, John R Pettersson, Svetlana A Shestopal, Wells W Wu, Ekaterina S Marakasova, Philip Olivares, Stepan S Surov, Mikhail V Ovanesov, Rong-Fong Shen, Andrey G Sarafanov
RESUMEN

Therapeutic products with coagulation factor VIII (FVIII) have a wide range of specific activities, implying presence of protein with altered structure. Previous studies showed that recombinant FVIII products (rFVIII) contain a fraction (FVIIIFT ) unable to bind von Willebrand factor (VWF) and reported to lack activity. Because of loss of function(s), FVIIIFT can be defined as a product-related impurity, whose properties and levels in rFVIII products should be investigated. To isolate and characterize the FVIIIFT fraction in rFVIII products. Protein fractions unable (FVIIIFT ) and able (FVIIIEL ) to bind VWF were isolated from rFVIII products using immobilized VWF affinity chromatography (IVAC) and characterized by gel electrophoresis, immunoblotting, FVIII activity test, surface plasmon resonance, mass spectrometry, and for plasma clearance in mice. A robust IVAC methodology was developed and applied for analysis of 10 rFVIII products marketed in the United States. FVIIIFT was found at various contents (0.4%-21.5%) in all products. Compared with FVIIIEL , FVIIIFT had similar patterns of polypeptide bands by gel electrophoresis, but lower functional activity. In several representative products, FVIIIFT was found to have reduced sulfation at Tyr1680, important for VWF binding, decreased interaction with a low-density lipoprotein receptor-related protein 1 fragment, and faster plasma clearance in mice. These findings provide basic characterization of FVIIIFT and demonstrate a potential for IVAC to control this impurity in rFVIII products to improve their efficacy in therapy of hemophilia A.

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Anti-Factor VIII Antibody, 83 kDa light chain, ascites fluid, Chemicon®