Factor VIII with a 237 amino acid B-domain has an extended half-life in F8-knockout mice

E Bloem; D M Karpf; P L Nørby; P B Johansen; M Loftager; H Rahbek-Nielsen; H H Petersen; G E Blouse; L Thim; M Kjalke; G Bolt

doi:10.1111/jth.14355

Factor VIII with a 237 amino acid B-domain has an extended half-life in F8-knockout mice

J Thromb Haemost. 2019 Feb;17(2):350-360. doi: 10.1111/jth.14355. Epub 2019 Jan 25.

Authors

E Bloem¹, D M Karpf¹, P L Nørby¹, P B Johansen¹, M Loftager¹, H Rahbek-Nielsen¹, H H Petersen¹, G E Blouse¹, L Thim¹, M Kjalke¹, G Bolt¹

Affiliation

¹ Novo Nordisk A/S, Novo Nordisk Park, Måløv, Denmark.

PMID: 30525289
DOI: 10.1111/jth.14355

Abstract

Essentials Factor (F)VIII with an intermediate-length B-domain showed higher levels in murine gene therapy. FVIII with different B-domain lengths were analysed. FVIII variants with B-domains between 186 and 240 amino acids (aa) have extended half-life in mice. Reduced cell binding of FVIII with a 237aa B-domain may explain the extended half-life. SUMMARY: Background Factor VIII consists of the A1-domain, A2-domain, B-domain, A3-domain, C1-domain, and C2-domain. FVIII with an intermediate-length B-domain of 226 amino acids (aa) has previously been evaluated in murine gene therapy studies. Objective To characterize FVIII with intermediate-length B-domains in vitro and in vivo in F8-knockout (KO) mice. Methods and results FVIII molecules with B-domains of 186-240aa had longer half-lives in F8-KO mice than FVIII molecules with shorter or longer B-domains. FVIII with a B-domain containing the 225 N-terminal aa fused to the 12 C-terminal aa of the wild-type B-domain (FVIII-237) had a 1.6-fold extended half-life in F8-KO mice as compared with FVIII with a 21aa B-domain (FVIII-21). The in vitro and in vivo activity of FVIII-237 were comparable to those of FVIII-21, as was binding to von Willebrand factor. Cell binding to LDL receptor-related protein 1 (LRP-1)-expressing cells was markedly reduced for FVIII-237 as compared with FVIII-21, whereas the affinity for LRP-1 was not reduced in surface plasmon resonance (SPR) studies. FVIII-21 cell binding and internalization could be inhibited by a fragment consisting of the 226 N-terminal aa of the FVIII B-domain, and SPR analysis suggested that this B-domain fragment might bind with weak affinity to FVIII-21. Conclusion Reduced cell binding of FVIII-237 might explain the observed extended half-life in F8-KO mice. This may contribute to the increased FVIII levels measured in murine gene therapy studies using FVIII constructs with similar B-domain lengths.

Keywords: LDL receptor-related protein-1; factor VIII; half-life; hemophilia A; von Willebrand factor.

MeSH terms

Animals
Cell Line
Coagulants / blood
Coagulants / pharmacokinetics*
Disease Models, Animal
Factor VIII / genetics
Factor VIII / pharmacokinetics*
Gene Knockout Techniques
Half-Life
Hemophilia A / blood
Hemophilia A / drug therapy*
Low Density Lipoprotein Receptor-Related Protein-1 / metabolism
Mice, Knockout
Protein Binding
Protein Domains
Recombinant Proteins / pharmacokinetics

Substances

Coagulants
Low Density Lipoprotein Receptor-Related Protein-1
Lrp1 protein, mouse
Recombinant Proteins
Factor VIII