住院患者直接口服抗凝药物相互作用的管理。
Management of direct oral anticoagulant drug interactions in hospitalized patients.
机构信息
Department of Pharmacy Services, Brigham and Women's Hospital, 75 Francis Street, Boston, MA, 02115, USA.
出版信息
J Thromb Thrombolysis. 2024 Apr;57(4):598-602. doi: 10.1007/s11239-024-02967-2. Epub 2024 Mar 30.
Moderate-strong CYP3A4 or Pgp inhibitors and inducers alter direct oral anticoagulant (DOAC) pharmacokinetics. Whether the presence of a DOAC drug-drug interaction (DDI) prompts in- hospital changes in management remains unknown. We identified all hospitalized patients at our institution who were admitted with a clinically relevant DOAC DDI from 01/2021 to 06/2021. Clinically relevant DOAC DDIs were defined as those listed in the prescribing information or FDA CYP3A4/Pgp inhibitors clinical indexes. We assessed the prevalence of DOAC DDIs and categorized their management as: drug stopped, drug held, or drug continued. For drugs that were continued we assessed whether the dose of the DOAC or interacting drug was increased, decreased or unchanged during the admission. We ascertained the number of DOAC DDIs that prompted an automated prescribing alert in our electronic health record (EHR). Finally, we conducted a logistic regression model to compare users of DOACs with DDI who had their regimen adjusted versus those without adjustments, focusing on outcomes of rehospitalization and death, adjusting for age and gender. Among 3,725 hospitalizations with a DOAC admission order, 197 (5%) had a clinically relevant DOAC DDI. The DOAC and the interacting drug were continued at discharge for 124 (63%) hospitalizations. The most frequent adjustments were stopping the interacting drug (73%) and stopping the DOAC (15%). Only 7 (4%) of DOAC DDIs prompted an EHR alert. The adjusted odds ratios for rehospitalizations and death, respectively, among patients whose regimens were adjusted compared to those whose were not, were 1.29 (95% CI, 0.67 to 2.48; P = 0.44) and 1.88 (95% CI, 0.91 to 3.89; P = 0.09). Clinically relevant DDIs with DOACs occur infrequently among hospitalized patients and usually are managed without stopping the DOAC. The clinical impact of such DDIs and subsequent adjustments on thrombotic and hemorrhagic outcomes requires further investigation.
中度至强 CYP3A4 或 Pgp 抑制剂和诱导剂会改变直接口服抗凝剂(DOAC)的药代动力学。是否存在 DOAC 药物相互作用(DDI)会促使住院期间改变管理策略尚不清楚。我们确定了 2021 年 1 月至 2021 年 6 月期间在我院住院且存在临床相关 DOAC DDI 的所有患者。临床相关 DOAC DDI 的定义为处方信息或 FDA CYP3A4/Pgp 抑制剂临床索引中列出的那些。我们评估了 DOAC DDI 的患病率,并将其管理分为:停止药物、停止药物或继续药物。对于继续使用的药物,我们评估了在住院期间 DOAC 或相互作用药物的剂量是否增加、减少或不变。我们确定了在我们的电子健康记录(EHR)中提示自动处方警报的 DOAC DDI 的数量。最后,我们进行了逻辑回归模型分析,比较了有 DDI 的 DOAC 使用者与未调整方案的患者,重点关注再住院和死亡的结果,同时调整年龄和性别。在 3725 例有 DOAC 入院医嘱的住院患者中,有 197 例(5%)存在临床相关 DOAC DDI。出院时继续使用 DOAC 和相互作用药物的有 124 例(63%)。最常见的调整是停止相互作用药物(73%)和停止 DOAC(15%)。只有 7 例(4%)的 DOAC DDI 提示 EHR 警报。与未调整方案的患者相比,调整方案的患者再住院和死亡的调整后比值比分别为 1.29(95%CI,0.67 至 2.48;P=0.44)和 1.88(95%CI,0.91 至 3.89;P=0.09)。住院患者中 DOAC 相关的中度至强 CYP3A4 或 Pgp 抑制剂和诱导剂引起的 DDI 发生率较低,通常无需停止 DOAC 即可进行管理。此类 DDI 及其对血栓形成和出血结局的后续调整的临床影响需要进一步研究。
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