Molecular Therapy: Methods & Clinical Development (Dec 2020)

Minimal Essential Human Factor VIII Alterations Enhance Secretion and Gene Therapy Efficiency

  • Wenjing Cao,
  • Biao Dong,
  • Franziska Horling,
  • Jenni A. Firrman,
  • Johannes Lengler,
  • Matthias Klugmann,
  • Maurus de la Rosa,
  • Wenman Wu,
  • Qizhao Wang,
  • Hongying Wei,
  • Andrea R. Moore,
  • Sean A. Roberts,
  • Carmen J. Booth,
  • Werner Hoellriegl,
  • Dong Li,
  • Barbara Konkle,
  • Carol Miao,
  • Birgit M. Reipert,
  • Friedrich Scheiflinger,
  • Hanspeter Rottensteiner,
  • Weidong Xiao

Journal volume & issue
Vol. 19
pp. 486 – 495

Abstract

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One important limitation for achieving therapeutic expression of human factor VIII (FVIII) in hemophilia A gene therapy is inefficient secretion of the FVIII protein. Substitution of five amino acids in the A1 domain of human FVIII with the corresponding porcine FVIII residues generated a secretion-enhanced human FVIII variant termed B-domain-deleted (BDD)-FVIII-X5 that resulted in 8-fold higher FVIII activity levels in the supernatant of an in vitro cell-based assay system than seen with unmodified human BDD-FVIII. Analysis of purified recombinant BDD-FVIII-X5 and BDD-FVIII revealed similar specific activities for both proteins, indicating that the effect of the X5 alteration is confined to increased FVIII secretion. Intravenous delivery in FVIII-deficient mice of liver-targeted adeno-associated virus (AAV) vectors designed to express BDD-FVIII-X5 or BDD-FVIII achieved substantially higher plasma FVIII activity levels for BDD-FVIII-X5, even when highly efficient codon-optimized F8 nucleotide sequences were employed. A comprehensive immunogenicity assessment using in vitro stimulation assays and various in vivo preclinical models of hemophilia A demonstrated that the BDD-FVIII-X5 variant does not exhibit an increased immunogenicity risk compared to BDD-FVIII. In conclusion, BDD-FVIII-X5 is an effective FVIII variant molecule that can be further developed for use in gene- and protein-based therapeutics for patients with hemophilia A.

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