Factor XIII cotreatment with hemostatic agents in hemophilia A increases fibrin α-chain crosslinking

J Thromb Haemost. 2018 Jan;16(1):131-141. doi: 10.1111/jth.13887. Epub 2017 Nov 20.

Abstract

Essentials Factor XIII (FXIII)-mediated fibrin crosslinking is delayed in hemophilia. We determined effects of FXIII cotreatment with hemostatic agents on clot parameters. FXIII cotreatment accelerated FXIII activation and crosslinking of fibrin and α2 -antiplasmin. These data provide biochemical rationale for FXIII cotreatment in hemophilia.

Summary: Background Hemophilia A results from the absence, deficiency or inhibition of factor VIII. Bleeding is treated with hemostatic agents (FVIII, recombinant activated FVII [rFVIIa], anti-inhibitor coagulation complex [FEIBA], or recombinant porcine FVIII [rpFVIII]). Despite treatment, some patients have prolonged bleeding. FXIII-A2 B2 (FXIII) is a protransglutaminase. During clot contraction, thrombin-activated FXIII (FXIIIa) crosslinks fibrin and α2 -antiplasmin, which promotes red blood cell retention and increases clot stability and weight. We hypothesized that FXIII cotreatment in hemophilia would accelerate FXIII activation, leading to increased fibrin crosslinking. Methods FVIII-deficient plasma and whole blood were clotted with or without hemostatic agents (FVIII, rFVIIa, FEIBA, or recombinant B-domain-deleted porcine FVIII [rpFVIII]) and/or FXIII. The effects on FXIII activation, thrombin generation, fibrin and α2 -antiplasmin crosslinking, clot formation and clot weight were measured by western blotting, calibrated automated thrombography, thromboelastography, and clot contraction assays. Results As compared with FVIII-treated hemophilic plasma, FVIII + FXIII cotreatment accelerated FXIIIa formation without increasing thrombin generation. As compared with buffer-treated or FXIII-treated hemophilic plasma, FVIII treatment and FVIII + FXIII cotreatment increased the generation and amount of crosslinked fibrin, including α-chain-rich high molecular weight species and crosslinked α2 -antiplasmin. In the presence of FVIII inhibitors, as compared with hemostatic treatments (rFVIIa, FEIBA, or rpFVIII) alone, FXIII cotreatment increased whole blood clot weight. Conclusion In hemophilia A plasma and whole blood, FXIII cotreatment with hemostatic agents accelerated FXIIIa formation, increased the generation and amount of fibrin α-chain crosslinked species, accelerated α2 -antiplasmin crosslinking, and increased clot weight. FXIII cotreatment with hemostatic therapy may augment hemostasis through increased crosslinking of fibrin and α2 -antiplasmin.

Keywords: factor XIII; fibrin; hemophilia; hemostasis; α2-antiplasmin.

Publication types

  • Comparative Study
  • Research Support, N.I.H., Extramural
  • Research Support, Non-U.S. Gov't

MeSH terms

  • Aged
  • Blood Coagulation / drug effects*
  • Blood Coagulation Factors / adverse effects
  • Blood Coagulation Factors / therapeutic use*
  • Coagulants / adverse effects
  • Coagulants / therapeutic use*
  • Factor VIII / adverse effects
  • Factor VIII / therapeutic use*
  • Factor VIIa / adverse effects
  • Factor VIIa / therapeutic use*
  • Factor XIII / adverse effects
  • Factor XIII / therapeutic use*
  • Female
  • Fibrin / chemistry
  • Fibrin / metabolism*
  • Hemophilia A / blood
  • Hemophilia A / diagnosis
  • Hemophilia A / drug therapy*
  • Humans
  • Male
  • Middle Aged
  • Recombinant Proteins / therapeutic use
  • Time Factors
  • Treatment Outcome
  • alpha-2-Antiplasmin / metabolism

Substances

  • Blood Coagulation Factors
  • Coagulants
  • Recombinant Proteins
  • alpha-2-Antiplasmin
  • F8 protein, human
  • Factor VIII
  • Fibrin
  • Factor XIII
  • anti-inhibitor coagulant complex
  • Factor VIIa

Supplementary concepts

  • Factor 8 deficiency, acquired