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The influence of fibrate initiation on INR and warfarin dose in patients receiving chronic warfarin therapy

机译:纤维酸盐对慢性华林治疗患者INR和华法林剂量的影响

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Several drug interaction compendia report a risk of warfarin potentiation after initiation of a fibrate; however, the evidence of this interaction is limited. The objective of this study was to evaluate warfarin dose and international normalized ratio (INR) response among a large sample of patients receiving chronic warfarin who initiated a fibrate. This was a retrospective, one-sample, pre-to-post study. Adult patients who were receiving chronic warfarin therapy at the time of gemfibrozil or fenofibrate dispensing between 1/1/2000 and 3/31/2016 were included. Patients had at least one and two therapeutic INRs during the 90 days prior to (baseline) and after (follow-up), respectively, fibrate initiation. Comparison of stable warfarin dose:INR ratio between the baseline and follow-up periods and assessment of safety outcomes during follow-up were performed. There were 321 patients included. Patients were predominantly male (62.6%) with an indication of atrial fibrillation (44.2%). The mean warfarin dose:INR ratio was equivalent between the baseline and follow-up periods (13.4 mg/INR [+/- 6.9] vs. 13.5 mg/INR [+/- 7.5], respectively, p = 0.711). Rates of thromboembolism, bleeding, and all-cause mortality in the 90-day follow up were 0, 0.6, and 1.2%, respectively. Although individual patients may have labile INRs after fibrate initiation, no significant interaction between fibrate and warfarin in a large sample of real world patients was identified. The utility of additional INR monitoring after fibrate initiation in otherwise stable patients receiving chronic warfarin therapy is unclear.
机译:几种药物互动素质在发起敌纤维后,报告了华法林潜力的风险;然而,这种互动的证据是有限的。本研究的目的是评估Warfarin剂量和国际标准化比率(INR)反应在接受发起母纤维的慢性华法林的大型患者中。这是回顾性,一个样本,预先研究。包括在1/1/2000和31 / 31/2016之间的Gemfibrozil或Fenofibrate分配时接受慢性华法林治疗的成年患者。患者在(基线)之前的90天和(随访)之前至少有一个和两种治疗性INRS,纤维酸盐开始。稳定华法林剂量的比较:进行基线与后续期间与随访期间安全结果之间的INR比率。包括321名患者。患者主要是雄性(62.6%),表征心房颤动(44.2%)。平均华法林剂量:基线和随访期之间的INR比率相当于(13.4mg / InR [+/- 6.9],分别为p = 0.711)。 90天后续血栓栓塞,出血和全因死亡率分别为0,0.6和1.2%。虽然在纤维酸盐发生后,个体患者可能有不稳定的INR,但鉴定了在大型现实世界患者的大型样本中没有显着的相互作用。额外INR监测在接受慢性华法林治疗的较稳定患者中匹配后额外的INR监测尚不清楚。

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