Effect of Gene-Based Warfarin Dosing on Anticoagulation Control and Clinical Events in a Real-World Setting

The and genotypes are associated with anticoagulation control and the clinical events in warfarin therapy. However, the clinical utility of gene-based warfarin dosing (GBWD) is controversial. We compared the anticoagulation control and clinical events related to warfarin with GBWD to those with clin...

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Published inFrontiers in pharmacology Vol. 10; p. 1527
Main Authors Zhang, Jinhua, Wu, Tingting, Chen, Wenjun, Fu, Jinglan, Xia, Xiaotong, Chen, Liangwan
Format Journal Article
LanguageEnglish
Published Switzerland Frontiers Media S.A 17.01.2020
Subjects
CYP2C9
pharmacogenetics
Pharmacology
precision medicine
VKORC1
warfarin
VKORC1
CYP2C9
precision medicine
pharmacogenetics
warfarin
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Summary:The and genotypes are associated with anticoagulation control and the clinical events in warfarin therapy. However, the clinical utility of gene-based warfarin dosing (GBWD) is controversial. We compared the anticoagulation control and clinical events related to warfarin with GBWD to those with clinically fixed dosing (CFD). A retrospective cohort study was conducted in a real-world setting. Of the 915 patients who were reviewed, 844 patients met the study-entry criteria; 413 cases were guided by GBWD using the International Warfarin Pharmacogenetic Consortium algorithm; 431 cases were guided by CFD (2.5 mg/day). The primary outcomes were the time needed to achieve the therapeutic International Normalized Ratio (INR) and the time in the therapeutic range (TTR) during a 3-month timeframe. The time needed to achieve the therapeutic INR (in days) for patients in the GBWD group was shorter than that for patients in the CFD group (10.21 ± 4.68 14.31 ± 8.26, P < 0.001). The overall TTR (Day 4-90) was significantly different between the GBWD group and CFD group (56.86 ± 10.72 vs. 52.87 ± 13.92, P = 0.007).In subgroup analysis, the TTR was also significantly different between the GBWD group and CFD group during the first month of treatment (Day 4-14: 54.28 ± 21.90 47.01 ± 26.25, = 0.012; Day 15-28: 59.60 ± 20.12 51.71 ± 18.96, = 0.001). However, no significant difference in the TTR was observed after 29 days of treatment. These data suggest that GBWD provided clinical benefits.
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Edited by: Nathalie K. Zgheib, American University of Beirut, Lebanon
This article was submitted to Pharmacogenetics and Pharmacogenomics, a section of the journal Frontiers in Pharmacology
Reviewed by: Vijay Suppiah, University of South Australia, Australia; Benjamin D. Horne, Intermountain Healthcare, United States
ISSN:1663-9812
1663-9812
DOI:10.3389/fphar.2019.01527