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Translational High-Dimensional Drug Interaction Discovery and Validation Using Health Record Databases and Pharmacokinetics Models

机译:使用健康记录数据库和药代动力学模型的翻译高维药互动发现和验证

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摘要

Polypharmacy increases the risk of drug-drug interactions (DDIs). Combining epidemiological studies with pharmacokinetic modeling, we detected and evaluated high-dimensional DDIs among 30 frequent drugs. Multidrug combinations that increased the risk of myopathy were identified in the US Food and Drug Administration Adverse Event Reporting System (FAERS) and electronic medical record (EMR) databases by a mixture drug-count response model. CYP450 inhibition was estimated among the 30 drugs in the presence of 1 to 4 inhibitors using in vitro / in vivo extrapolation. Twenty-eight three-way and 43 four-way DDIs had significant myopathy risk in both databases and predicted increases in the area under the concentration-time curve ratio (AUCR) 2-fold. The high-dimensional DDI of omeprazole, fluconazole, and clonidine was associated with a 6.41-fold (FAERS) and 18.46-fold (EMR) increased risk of myopathy local false discovery rate (0.005); the AUCR of omeprazole in this combination was 9.35. The combination of health record informatics and pharmacokinetic modeling is a powerful translational approach to detect high-dimensional DDIs.
机译:PolyPharcacency增加了药物 - 药物相互作用的风险(DDIS)。将流行病学研究与药代动力学建模相结合,我们在30次频繁药物中检测到高维DDIS。增加了肌病风险的多药物组合在美国食品和药物管理局的不良事件报告系统(FAEERS)和电子医疗记录(EMR)数据库中确定了混合物药物计数响应模型。在体外/体内推断的1至4个抑制剂存在下,在30种药物中估计CYP450抑制。二十八个三元和43四路DDI在两个数据库中具有显着的肌病风险,并且在浓度 - 时间曲线比(AUCR)& 2倍下的区域的预测增加。奥美唑,氟康唑和克隆酮的高尺寸DDI与6.41倍(陈)和18.46倍(EMR)的肌病局部假发现率的风险增加有关(&0.005);这种组合中奥美拉唑的AUCR为9.35。健康记录信息和药代动力学建模的组合是一种检测高维DDIS的强大翻译方法。

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  • 作者单位

    Indiana Univ Sch Med Ctr Computat Biol &

    Bioinformat Indianapolis IN USA;

    Ohio State Univ Coll Med Dept Biomed Informat Columbus OH 43210 USA;

    Harbin Engn Univ Inst Intelligent Syst &

    Bioinformat Coll Automat Harbin Heilongjiang Peoples;

    Ohio State Univ Coll Med Dept Biomed Informat Columbus OH 43210 USA;

    Indiana Univ Sch Med Ctr Computat Biol &

    Bioinformat Indianapolis IN USA;

    Indiana Univ Sch Med Ctr Computat Biol &

    Bioinformat Indianapolis IN USA;

    Indiana Univ Sch Med Ctr Computat Biol &

    Bioinformat Indianapolis IN USA;

    Indiana Univ Sch Med Ctr Computat Biol &

    Bioinformat Indianapolis IN USA;

    Ohio State Univ Coll Med Dept Biomed Informat Columbus OH 43210 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药理学;
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