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In vitro comparison of the effect of two factor XI (FXI) concentrates on thrombin generation in major FXI deficiency
Pike, G N; Cumming, A M; Hay, C R; Sempasa, B; Sutherland, M; Thachil, J; Burthem, J; Bolton-Maggs, P H
Haemophilia. 2015;.
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Abstract
INTRODUCTION: Bleeding risk in factor XI (FXI) deficiency following surgery may be reduced by treatment with either of two FXI concentrates, but indications for their use are unclear and treatment has been associated with thrombosis. AIM: To quantify and compare the effects of two different FXI concentrates on thrombin generation (TG) in major FXI deficiency (FXI:C < 15 IU dL-1 ). METHODS: Thrombin generation was measured in controls (n = 50), FXI-deficient individuals pre and post in vitro spiking with FXI concentrates (n = 10), and in ex vivo samples following treatment with FXI concentrate (n = 3). RESULTS: Thrombin generation was significantly impaired in FXI deficiency but improved following FXI replacement in vitro and in vivo. LFB Hemoleven(R) had greater effect on TG than BPL FXI concentrate in vitro (equivalent in vivo doses 10, 20 and 30 U kg-1 ): higher endogenous thrombin potential (ETP) (P < 0.0001), peak height (P < 0.01) velocity (P < 0.0002) and shorter lag time and time to peak (both P < 0.003). Some measurements with LFB Hemoleven(R) exceeded the reference range. At lower dose (5 U kg-1 ), BPL FXI concentrate normalized all TG parameters and LFB Hemoleven(R) normalized the ETP but exceeded the reference range with other parameters. CONCLUSION: Both FXI concentrates improve TG in vitro in major FXI deficiency but differ in dose response, and for both products, doses lower than previously recommended normalized TG in vitro. Comparison of in vitro spiked and ex vivo samples suggest that in vitro results could be used to estimate an expected in vivo response to FXI replacement.
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- Related website http://www.ncbi.nlm.nih.gov/pubmed/26558335
- Pike, G N Cumming, A M Hay, C R M Sempasa, B Sutherland, M Thachil, J Burthem, J Bolton-Maggs, P H B Haemophilia. 2015 Nov 11. doi: 10.1111/hae.12846.