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DOI: 10.1160/TH14-06-0485
Low-molecular-weight heparin to prevent postpartum venous thromboembolism
A pilot randomised placebo-controlled trial Financial support: National Institutes of Health Research grant # NIH 1R34HL107725–01 and Canadian Institutes of Health Research grant #MOP 106641. Dr. Rodger is supported by a Heart and Stroke Foundation Career Investigator Award and a University of Ottawa, Faculty of Medicine Chair in Venous Thrombosis and Thrombophilia. Dr. Kahn is supported by a National Research Scholar award from the Fonds de recherche santé Québec. The funders played no role in the design, conduct, analysis or interpretation for the pilot trial.Publication History
Received:
02 June 2014
Accepted after major revision:
16 August 2014
Publication Date:
27 November 2017 (online)
Summary
The risk of venous thromboembolism (VTE) is elevated in the postpartum period. Low-molecular-weight heparin (LMWH) reduces the risk of VTE in many settings but is costly, inconvenient and increases bleeding. Randomised controlled trials (RCT) are required to determine if LMWH prophylaxis provides a clinical benefit in high-risk postpartum women. We sought to determine if a placebo-controlled RCT was feasible. We conducted a multi-national, double-blind pilot RCT in “high risk” postpartum women comparing 21 days of prophylactic dose LMWH to identical saline placebo injections. The primary pilot outcome was mean number of recruited women per centre per month. The planned primary outcome for the full trial was symptomatic objectively confirmed VTE or asymptomatic proximal deep-vein thrombosis diagnosed by a screening bilateral leg vein ultrasound at day 21. In six centres, a total of 1,346 potentially eligible women were approached to participate; 968 were ineligible, leaving 378 (31.5%) eligible patients. Of these, only 25 (6.6%) were randomised at a rate of 0.7 per centre per month. The primary reasons for declining participation were to avoid study injections and being too overwhelmed to participate in research. None of the participants had a VTE during follow-up. In conclusion, despite an adequate number of eligible participants, our double-blind RCT design was not feasible due to a very low consent rate. Other experimental approaches may be necessary to generate evidence in this important area of research.
Keywords
Low-molecular-weight heparin - postpartum - randomised controlled trial - thromboprophylaxis - venous thromboembolism* PROSPER Investigators are listed in the Appendix.
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