Abstract

The acute vascular disease deep vein thrombosis (DVT) requires oral anticoagulants to prevent progression. Monitoring therapeutic efficacy of direct oral anticoagulants (DOAC), including rivaroxaban, is problematic as no reliable test is available. Advances in rheometry have led to the development of a functional coagulation biomarker using Gel Point (GP) analysis which assesses clot structure formation. The biomarker measures incipient clot formation time (TGP) and quantifies fibrin clot structure in terms of fractal dimension (df). This study aimed to investigate clot structure formation in first time DVT and the effect of rivaroxaban treatment. This prospective observational cohort study measured the GP and standard laboratory markers at three sample points: pre-treatment and at 20 and 60 days following 15 mg BD and 20 mg OD rivaroxaban respectively. Forty DVT patients (mean age 64 years [SD±14.8]; 23 males, 17 female) were recruited. The results show that DVT vs non-DVT patients did not have a significantly different GP profile (df: 1.72±0.06 vs 1.70±0.06 and TGP: 267±68 sec vs 262±73 sec) with both within the defined healthy index. In addition, rivaroxaban therapy increased TGP to 392 s (±135 s) after 20 days, and subsequently increased to 395 s (±194 s) at 60 days but did not significantly increase df (from 1.69±0.05 to 1.71±0.06). The results indicate in this cohort of DVT patients there was no underlying hypercoagulable effect as determined by gel point analysis. Furthermore, the anticoagulant effect of rivaroxaban prolonged clotting, suggesting a protective effect against clot formation, without significantly reducing clot microstructural properties.

Highlights

  • What does this paper add? First time Deep vein thrombosis (DVT) do not demonstrate abnormal clot characteristics Gel point analysis quantifies the effect of rivaroxaban and alteration in dosage Rivaroxaban’s effect on clotting time remained consistently prolonged

  • In this study we assessed the effect of rivaroxaban on viscoelastic and microstructural properties of the blood using Gel Point (GP) analysis in first time DVT patients

  • The changes in df would appear to be small but we have previously reported that these changes correlate with large changes in clot mass observed through Scanning electron microscopy (SEM) imaging.[30]

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Summary

Introduction

In anticoagulation we hypothesised that the GP analysis will be capable of identifying the forgoing effects of rivaroxaban in first time DVT patients To investigate this hypothesis, the present study aimed to determine changes in clot structure in a cohort of patients with suspected first time DVT compared to non-DVT patients.

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