Rethinking lead-in strategies: evaluation of full vs. reduced dose factor Xa inhibitors in acute VTE

Authors

Natasha Jolakoski, Henry Ford Health
Sarah Grazia, Henry Ford Health
Clare Brewster
Brehanna Edwards
Danielle Rosas
Diana Penev
Whitney Anderson
Stephanie B. Edwin, Henry Ford HealthFollow
Shannon Carabetta
Bradley J. Haan, Henry Ford HealthFollow
Thomas C. Breedan, Henry Ford HealthFollow
Megan Laux
Kathaleen Watson
Andrew Harpenau
Rachel Bruns
Josephine Varda
Kathleen Koopman
Meagan Paylor
Christopher Giuliano, Henry Ford HealthFollow

Recommended Citation

Jolakoski N, Grazia S, Brewster C, Edwards B, Rosas D, Penev D, Anderson W, Edwin SB, Carabetta S, Haan B, Breedan T, Laux M, Watson K, Harpenau A, Bruns R, Varda J, Koopman K, Paylor M, and Guiliano C. Rethinking lead-in strategies: evaluation of full vs. reduced dose factor Xa inhibitors in acute VTE. J Thromb Thrombolysis 2025.

Document Type

Article

Publication Date

12-1-2025

Publication Title

Journal of thrombosis and thrombolysis

Keywords

Anticoagulation; Bleeding; Deep vein thrombosis; Factor xa inhibitor; Pulmonary embolism; Venous thromboembolism

Abstract

Oral factor Xa inhibitors are preferred treatments for venous thromboembolism (VTE). While apixaban and rivaroxaban require an initial lead-in period, clinicians may reduce the period if patients have received prior therapeutic parenteral anticoagulation, although supporting evidence is limited. The purpose of this study is to evaluate bleeding and thrombotic events associated with reducing factor Xa inhibitor lead-in duration in patients who have received prior parenteral anticoagulation. This multicenter retrospective cohort study was conducted across 29 hospitals and included adult patients hospitalized with a new diagnosis of VTE who received at least 24 h of therapeutic parenteral anticoagulation before starting apixaban or rivaroxaban. Patients with active bleeding on admission, anticoagulation prior to admission, antiphospholipid syndrome, severe liver disease, or contraindicated medications were excluded. The primary outcome was time to VTE recurrence within six months. Cox proportional hazard model was used to control for potential confounding factors and a sensitivity analysis was performed using propensity matching. Among 1,424 patients included, 1,068 received a full lead-in and 356 a reduced lead-in regimen. No significant difference in time to recurrent VTE (HR 0.53; 95% CI, 0.20-1.37;p = 0.19) or major bleeding (HR 0.69; 95% CI, 0.31-1.56;p = 0.45) was observed after controlling for confounding factors. No difference in recurrent VTE and major bleeding persisted after propensity matching. Among patients transitioning from parenteral anticoagulation to oral factor Xa inhibitors, a reduced lead-in duration was not associated with increased VTE recurrence or major bleeding.

PubMed ID

41326919

ePublication

ePub ahead of print