Polypharmacy and Drug Interactions in the COVID-19 Pandemic.

Q4 Biochemistry, Genetics and Molecular Biology
Ricardo Enrique Barcia, Guillermo Alberto Keller, Natalia Bello, Francisco Azzato, Roberto Alejandro Diez, Guido Giunti
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引用次数: 0

Abstract

The COVID-19 pandemic generated a great impact on health systems. We compared evolution, polypharmacy, and potential drug-drug interactions (P-DDIs) in COVID-19 and non-COVID-19 hospitalizations during first wave of pandemic. Prescriptions for hospitalized patients ≥ 18 years (COVID-19 and non-COVID-19 rooms) between April and September 2020 were included. The computerized medical decision support system SIMDA and the physician order entry system Hdc.DrApp.la were used. Patients in COVID-19 rooms were divided into detectable and non-detectable, according to real-time reverse transcription polymerase chain reaction (RT-PCR). Number of drugs, prescribed on day 1, after day 1, and total; polypharmacy, excessive polypharmacy, and P-DDIs were compared. 1,623 admissions were evaluated: 881 COVID-19, 538 detectable and 343 non-detectable, and 742 non-COVID-19. Mortality was 15% in COVID-19 and 13% in non-COVID-19 (RR [non-COVID-19 vs. COVID-19]: 0.84 [95% CI] [0.66-1.07]). In COVID-19, mortality was 19% in detectable and 9% in non-detectable (RR: 2.07 [1.42-3.00]). Average number of drugs was 4.54/patient (SD ± 3.06) in COVID-19 and 5.92/patient (±3.24) in non-COVID-19 (p<0.001) on day 1 and 5.57/patient (±3.93) in COVID-19 and 9.17/patient (±5.27) in non-COVID-19 (p<0.001) throughout the hospitalization. 45% received polypharmacy in COVID-19 and 62% in non-COVID-19 (RR: 1.38 [1.25-1.51]) and excessive polypharmacy 7% in COVID-19 and 14% in non-COVID-19 (RR: 2.09 [1.54-2.83]). The frequency of total P-DDIs was 0.31/patient (±0.67) in COVID-19 and 0.40/patient (±0.94) in non-COVID-19 (p=0.022). Hospitalizations in the COVID-19 setting are associated with less use of drugs, less polypharmacy and less P-DDIs. Detectable patients had higher mortality.

COVID-19 大流行中的多重用药和药物相互作用。
COVID-19 大流行对医疗系统产生了巨大影响。我们比较了第一波大流行期间 COVID-19 和非 COVID-19 住院病人的用药演变、多重用药和潜在的药物相互作用(P-DDIs)。纳入了 2020 年 4 月至 9 月期间≥ 18 岁住院患者(COVID-19 和非 COVID-19 病房)的处方。使用了计算机化医疗决策支持系统 SIMDA 和医嘱输入系统 Hdc.DrApp.la。根据实时反转录聚合酶链反应(RT-PCR),COVID-19病房的患者分为可检测到和不可检测到两种。比较了第 1 天、第 1 天后的处方药数量和总数;多药、过度多药和 P-DDIs 的情况。共对 1623 例入院患者进行了评估:其中 881 例为 COVID-19,538 例可检测到,343 例无法检测到,742 例为非 COVID-19。COVID-19 死亡率为 15%,非 COVID-19 死亡率为 13%(RR [非 COVID-19 vs. COVID-19]:0.84 [95% CI] [0.66-1.07])。在 COVID-19 中,可检测到的死亡率为 19%,不可检测到的死亡率为 9%(RR:2.07 [1.42-3.00])。住院第 1 天,COVID-19 患者的平均用药次数为 4.54 次/人(SD ± 3.06),非 COVID-19 患者为 5.92 次/人(±3.24)(p<0.001);整个住院期间,COVID-19 患者的平均用药次数为 5.57 次/人(±3.93),非 COVID-19 患者为 9.17 次/人(±5.27)(p<0.001)。在 COVID-19 中,45% 的患者接受了多种药物治疗,而在非 COVID-19 中,62% 的患者接受了多种药物治疗(RR:1.38 [1.25-1.51]);在 COVID-19 中,7% 的患者接受了过度的多种药物治疗,而在非 COVID-19 中,14% 的患者接受了过度的多种药物治疗(RR:2.09 [1.54-2.83])。COVID-19 的总 P-DDIs 频率为 0.31/患者(±0.67),非 COVID-19 为 0.40/患者(±0.94)(P=0.022)。在 COVID-19 环境中住院与用药少、多药疗法少和 P-DDIs 少有关。可检测患者的死亡率较高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Prague medical report
Prague medical report Medicine-Medicine (all)
CiteScore
1.10
自引率
0.00%
发文量
19
审稿时长
20 weeks
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