The 1.7 Å X-Ray Crystal Structure of the Porcine Factor VIII C2 Domain and Binding Analysis to Anti-Human C2 Domain Antibodies and Phospholipid Surfaces

Authors

P. Clint Spiegel, Western Washington UniversityFollow
Caileen M. Brison, Western Washington University
Steven M. Mullen, Western Washington University
Michelle E. Wuerth, Western Washington University
Kira Podolsky, Western Washington University
Matthew Cook, Western Washington University
Jacob A. Herman, Western Washington University
Justin D. Walter, Western Washington University
Shannon L. Meeks, Emory University

Document Type

Article

Publication Date

3-16-2015

Keywords

Crystal structure, Hemophilia, Binding analysis

Abstract

The factor VIII C2 domain is essential for binding to activated platelet surfaces as well as the cofactor activity of factor VIII in blood coagulation. Inhibitory antibodies against the C2 domain commonly develop following factor VIII replacement therapy for hemophilia A patients, or they may spontaneously arise in cases of acquired hemophilia. Porcine factor VIII is an effective therapeutic for hemophilia patients with inhibitor due to its low cross-reactivity; however, the molecular basis for this behavior is poorly understood. In this study, the X-ray crystal structure of the porcine factor VIII C2 domain was determined, and superposition of the human and porcine C2 domains demonstrates that most surface-exposed differences cluster on the face harboring the “non-classical” antibody epitopes. Furthermore, antibody-binding results illustrate that the “classical” 3E6 antibody can bind both the human and porcine C2 domains, although the inhibitory titer to human factor VIII is 41 Bethesda Units (BU)/mg IgG versus 0.8 BU/mg IgG to porcine factor VIII, while the non-classical G99 antibody does not bind to the porcine C2 domain nor inhibit porcine factor VIII activity. Further structural analysis of differences between the electrostatic surface potentials suggest that the C2 domain binds to the negatively charged phospholipid surfaces of activated platelets primarily through the 3E6 epitope region. In contrast, the G99 face, which contains residue 2227, should be distal to the membrane surface. Phospholipid binding assays indicate that both porcine and human factor VIII C2 domains bind with comparable affinities, and the human K2227A and K2227E mutants bind to phospholipid surfaces with similar affinities as well. Lastly, the G99 IgG bound to PS-immobilized factor VIII C2 domain with an apparent dissociation constant of 15.5 nM, whereas 3E6 antibody binding to PS-bound C2 domain was not observed.

Publication Title

PLoS One

Issue

pone.0122447

Required Publisher's Statement

https://doi.org/10.1371/journal.pone.0122447

Recommended Citation

Brison CM, Mullen SM, Wuerth ME, Podolsky K, Cook M, Herman JA, et al. (2015) The 1.7 Å X-Ray Crystal Structure of the Porcine Factor VIII C2 Domain and Binding Analysis to Anti-Human C2 Domain Antibodies and Phospholipid Surfaces. PLoS ONE 10(3): e0122447. https://doi.org/10.1371/journal.pone.0122447

Subjects - Topical (LCSH)

Blood coagulation factor VIII--Structures; Blood coagulation factor VIII antibodies; Blood coagulation factors; Phospholipid antibodies; Hemophilia--Treatment

Genre/Form

articles

Type

Text

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Language

English

Format

application/pdf