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使用贝叶斯核机器回归检测药物混合物的单变量、双变量和总体效应。

Detecting univariate, bivariate, and overall effects of drug mixtures using Bayesian kernel machine regression.

作者信息

Bather Jemar R, Han Larry, Bennett Alex S, Elliott Luther, Goodman Melody S

机构信息

Center for Anti-Racism, Social Justice & Public Health, New York University School of Global Public Health, New York, NY, USA.

Department of Biostatistics, New York University School of Global Public Health, New York, NY, USA.

出版信息

Am J Drug Alcohol Abuse. 2024 Sep 2;50(5):623-630. doi: 10.1080/00952990.2024.2380463. Epub 2024 Jul 23.

Abstract

Innovative analytic approaches to drug studies are needed to understand better the co-use of opioids with non-opioids among people using illicit drugs. One approach is the Bayesian kernel machine regression (BKMR), widely applied in environmental epidemiology to study exposure mixtures but has received far less attention in substance use research. To describe the utility of the BKMR approach to study the effects of drug substance mixtures on health outcomes. We simulated data for 200 individuals. Using the Vale and Maurelli method, we simulated multivariate non-normal drug exposure data: xylazine (mean = 300 ng/mL, SD = 100 ng/mL), fentanyl (mean = 200 ng/mL, SD = 71 ng/mL), benzodiazepine (mean = 300 ng/mL, SD = 55 ng/mL), and nitazene (mean = 200 ng/mL, SD = 141 ng/mL) concentrations. We performed 10,000 MCMC sampling iterations with three Markov chains. Model diagnostics included trace plots, r-hat values, and effective sample sizes. We also provided visual relationships of the univariate and bivariate exposure-response and the overall mixture effect. Higher levels of fentanyl and nitazene concentrations were associated with higher levels of the simulated health outcome, controlling for age. Trace plots, r-hat values, and effective sample size statistics demonstrated BKMR stability across multiple Markov chains. Our understanding of drug mixtures tends to be limited to studies of single-drug models. BKMR offers an innovative way to discern which substances pose a greater health risk than other substances and can be applied to assess univariate, bivariate, and cumulative drug effects on health outcomes.

摘要

需要创新的药物研究分析方法,以更好地了解使用非法药物人群中阿片类药物与非阿片类药物的联合使用情况。一种方法是贝叶斯核机器回归(BKMR),它在环境流行病学中广泛应用于研究暴露混合物,但在药物使用研究中受到的关注要少得多。为了描述BKMR方法在研究药物物质混合物对健康结果影响方面的效用。我们模拟了200个人的数据。使用Vale和Maurelli方法,我们模拟了多变量非正态药物暴露数据:赛拉嗪(均值 = 300 ng/mL,标准差 = 100 ng/mL)、芬太尼(均值 = 200 ng/mL,标准差 = 71 ng/mL)、苯二氮䓬(均值 = 300 ng/mL,标准差 = 55 ng/mL)和硝氮烯(均值 = 200 ng/mL,标准差 = 141 ng/mL)浓度。我们用三个马尔可夫链进行了10000次MCMC抽样迭代。模型诊断包括轨迹图、r-hat值和有效样本量。我们还提供了单变量和双变量暴露-反应以及总体混合物效应的可视化关系。在控制年龄的情况下,较高水平的芬太尼和硝氮烯浓度与较高水平的模拟健康结果相关。轨迹图、r-hat值和有效样本量统计表明BKMR在多个马尔可夫链上具有稳定性。我们对药物混合物的理解往往局限于单药物模型的研究。BKMR提供了一种创新方法,以辨别哪些物质比其他物质构成更大的健康风险,并可用于评估单变量、双变量和累积药物对健康结果的影响。

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