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Blood advances
08 13, 2024;8 (15): 3929-3940.

The combination of Asp519Val/Glu665Val and Lys1813Ala mutations in FVIII markedly increases coagulation potential.

Yuto Nakajima, Akihisa Oda, Nemekhbayar Baatartsogt, Yuji Kashiwakura, Tsukasa Ohmori, Keiji Nogami
Author Information
  1. Yuto Nakajima: Department of Pediatrics, Nara Medical University, Kashihara, Japan. ORCID
  2. Akihisa Oda: Department of Pediatrics, Nara Medical University, Kashihara, Japan. ORCID
  3. Nemekhbayar Baatartsogt: Department of Biochemistry, Jichi Medical University School of Medicine, Shimotsuke, Japan. ORCID
  4. Yuji Kashiwakura: Department of Biochemistry, Jichi Medical University School of Medicine, Shimotsuke, Japan. ORCID
  5. Tsukasa Ohmori: Department of Biochemistry, Jichi Medical University School of Medicine, Shimotsuke, Japan. ORCID
  6. Keiji Nogami: Department of Pediatrics, Nara Medical University, Kashihara, Japan.
PMID: 38820442 DOI: 10.1182/bloodadvances.2023012391

Abstract

ABSTRACT: A2 domain dissociation in activated factor VIII (FVIIIa) results in reduced activity. Previous studies demonstrated that some FVIII mutants (D519V/E665V and K1813A) with delayed A2 dissociation enhanced coagulation potential. We speculated, therefore, that FVIII encompassing a combination of these mutations might further enhance coagulant activity. The aim was to assess the D519V/E665V/K1813A-FVIII mutation as a gain of function. The FVIII mutants, D519V/E665V/K1813A, D519V/E665V, and K1813A were expressed in a baby hamster kidney cell system, and global coagulation potential of these mutants was compared with wild-type (WT) FVIII in vitro and in hemophilia A mice in vivo. Kinetic analyses indicated that the apparent Kd for FIXa on the tenase assembly with D519V/E665V and D519V/E665V/K1813A mutants were lower, and that the generated FXa for D519V/E665V/K1813A was significantly greater than WT-FVIII. WT-FVIII activity after thrombin activation increased by ���12-fold within 5 minutes, and returned to initial levels within 30 minutes. In contrast, The FVIII-related activity of D519V/E665V/K1813A increased further with time after thrombin activation, and showed an ���25-fold increase at 2 hours. The A2 dissociation rate of D519V/E665V/K1813A was ���50-fold slower than the WT in a 1-stage clotting assay. Thrombin generation assays demonstrated that D519V/E665V/K1813A (0.125 nM) exhibited coagulation potential comparable with that of the WT (1 nM). In animal studies, rotational thromboelastometry and tail-clip assays showed that the coagulation potential of D519V/E665V/K1813A (0.25 ��g/kg) was equal to that of the WT (2 ��g/kg). FVIII-D519V/E665V/K1813A mutant could provide an approximately eightfold increase in hemostatic function of WT-FVIII because of increased FVIIIa stability and the association between FVIIIa and FIXa.

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MeSH Term

Animals
Factor VIII
Blood Coagulation
Mice
Humans
Hemophilia A
Mutation
Cricetinae
Thrombin
Amino Acid Substitution
Cell Line
Disease Models, Animal

Chemicals

Factor VIII
Thrombin
Journal Article Research Support, Non-U.S. Gov't

Word Cloud

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