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开发一种量化QTc延长风险的模型以加强药物安全性评估:一项回顾性分析。

Developing a Model for Quantifying QTc-Prolongation Risk to Enhance Medication Safety Assessment: A Retrospective Analysis.

作者信息

Giovannoni Luis, Kullak-Ublick Gerd A, Jetter Alexander

机构信息

Department of Clinical Pharmacology and Toxicology, University Hospital Zurich, University of Zurich, Rämistrasse 100, 8091 Zurich, Switzerland.

Tox Info Suisse, National Poison Center, Associated Institute of the University of Zurich, Freiestrasse 16, 8032 Zurich, Switzerland.

出版信息

J Pers Med. 2024 Jan 31;14(2):172. doi: 10.3390/jpm14020172.

Abstract

There are currently no established methods to predict quantitatively whether the start of a drug with the potential to prolong the QTc interval poses patients at risk for relevant QTc prolongation. Therefore, this retrospective study aimed to pave the way for the development of models for estimating QTc prolongation in patients newly exposed to medications with QTc-prolonging potential. Data of patients with a documented QTc prolongation after initiation of a QTc-prolonging drug were extracted from hospital charts. Using a standard model-building approach, general linear mixed models were identified as the best models for predicting both the extent of QTc prolongation and its absolute value after the start of a QTc-time-prolonging drug. The cohort consisted of 107 adults with a mean age of 64.2 years. Patients were taking an average of 2.4 drugs associated with QTc prolongation, with amiodarone, propofol, pipamperone, ondansetron, and mirtazapine being the most frequently involved. There was a significant but weak correlation between measured and predicted absolute QTc values under medication (r = 0.262, < 0.05), as well as for QTc prolongation (r = 0.238, < 0.05). As the developed models are based on a relatively small number of subjects, further research is necessary to ensure their applicability and reliability in real-world scenarios. Overall, this research contributes to the understanding of QTc prolongation and its association with medications, providing insight into the development of predictive models. With improvements, these models could potentially aid healthcare professionals in assessing the risk of QTc prolongation before adding a new drug and in making informed decisions in clinical settings.

摘要

目前尚无既定方法可定量预测具有延长QTc间期潜力的药物开始使用后,患者是否有发生相关QTc延长的风险。因此,这项回顾性研究旨在为开发用于估计新接触具有QTc延长潜力药物的患者QTc延长情况的模型铺平道路。从医院病历中提取了开始使用QTc延长药物后记录有QTc延长的患者数据。使用标准的模型构建方法,通用线性混合模型被确定为预测QTc延长药物开始使用后QTc延长程度及其绝对值的最佳模型。该队列由107名成年人组成,平均年龄为64.2岁。患者平均服用2.4种与QTc延长相关的药物,其中胺碘酮、丙泊酚、匹泮哌隆、昂丹司琼和米氮平最为常见。用药期间测量的和预测的绝对QTc值之间存在显著但较弱的相关性(r = 0.262,<0.05),QTc延长情况也是如此(r = 0.238,<0.05)。由于所开发的模型基于相对较少的受试者,因此有必要进行进一步研究以确保其在实际场景中的适用性和可靠性。总体而言,这项研究有助于理解QTc延长及其与药物的关联,为预测模型的开发提供了见解。通过改进,这些模型可能有助于医疗保健专业人员在添加新药之前评估QTc延长的风险,并在临床环境中做出明智的决策。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a1f9/10890600/88d966501e08/jpm-14-00172-g001.jpg

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