4.1 Article

Direct Oral to Parenteral Anticoagulants: Strategies for Inpatient Transition

期刊

JOURNAL OF CLINICAL PHARMACOLOGY
卷 61, 期 1, 页码 32-40

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WILEY
DOI: 10.1002/jcph.1694

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apixaban; anticoagulants; bleeding; factor Xa inhibitors; inpatients; rivaroxaban

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This study compared the impact on bleeding rates of a delayed, clinically driven strategy versus a standard per-package-insert strategy for transitioning from a direct oral anticoagulant to a parenteral anticoagulant. The primary endpoint showed a higher incidence of major bleeding in the delayed group compared to the standard group. Patients in both groups who experienced bleeding had a higher severity of illness and higher median DOAC anti-factor Xa concentrations.
The primary objective of this study was to describe the impact on bleeding rates of 2 different strategies for transitioning from a direct oral anticoagulant (DOAC) to a parenteral anticoagulant: a delayed, clinically driven strategy versus the standard per-package-insert strategy. This was a single-center descriptive cohort study conducted at a large academic medical center. Included patients were 18 years or older, admitted as an inpatient, and had received at least 1 dose of a DOAC prior to initiation of therapeutic parenteral anticoagulation. The primary end point was the incidence of major bleeds on the transition from a DOAC to a parenteral anticoagulant via a standard versus an intentionally delayed strategy. The secondary outcomes evaluated renal function, reason for delay, DOAC anti-factor Xa concentration, international normalized ratio values, blood product administration, and thrombotic complications. A total of 300 patients were included. The primary end point of bleeding was higher in the delayed group than the standard group, 25% and 12%, respectively (odds ratio, 0.39;P< .05). In both groups, patients who bled had a higher severity of illness, a greater incidence of acute kidney injury, and, when available, higher median DOAC anti-factor Xa concentrations. Despite a more conservative approach, patients in the delayed group experienced more bleeding, most likely attributable to a higher severity of illness, which highlights emerging challenges of inpatient anticoagulation management. Further prospective studies analyzing DOAC pharmacodynamics and pharmacokinetics in acutely ill patients are warranted.

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