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Metabolomics biomarkers to predict acamprosate treatment response in alcohol-dependent subjects

机译:代谢组学生物标志物预测酒精依赖受试者的阿坎酸治疗反应

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摘要

Precision medicine for alcohol use disorder (AUD) allows optimal treatment of the right patient with the right drug at the right time. Here, we generated multivariable models incorporating clinical information and serum metabolite levels to predict acamprosate treatment response. The sample of 120 patients was randomly split into a training set (n = 80) and test set (n = 40) five independent times. Treatment response was defined as complete abstinence (no alcohol consumption during 3 months of acamprosate treatment) while nonresponse was defined as any alcohol consumption during this period. In each of the five training sets, we built a predictive model using a least absolute shrinkage and section operator (LASSO) penalized selection method and then evaluated the predictive performance of each model in the corresponding test set. The models predicted acamprosate treatment response with a mean sensitivity and specificity in the test sets of 0.83 and 0.31, respectively, suggesting our model performed well at predicting responders, but not non-responders (i.e. many non-responders were predicted to respond). Studies with larger sample sizes and additional biomarkers will expand the clinical utility of predictive algorithms for pharmaceutical response in AUD.
机译:酒精使用障碍症(AUD)的精准药物可在正确的时间以正确的药物对正确的患者进行最佳治疗。在这里,我们生成了包含临床信息和血清代谢物水平的多变量模型,以预测阿坎酸治疗反应。将120名患者的样本随机分成五个独立的训练组(n = 80)和测试组(n = 40)。治疗反应定义为完全戒酒(阿坎酸治疗3个月内无酒精消耗),而无反应则定义为在此期间任何酒精消耗。在这五个训练集中的每个训练集中,我们使用最小绝对收缩和截面算子(LASSO)惩罚选择方法构建了一个预测模型,然后在相应的测试集中评估了每个模型的预测性能。该模型预测测试集中的阿坎酸治疗反应的平均敏感性和特异性分别为0.83和0.31,这表明我们的模型在预测反应者方面表现良好,但对非反应者表现良好(即,许多无反应者被预测为反应)。具有更大样本量和更多生物标志物的研究将扩大用于澳元药物反应的预测算法的临床应用。

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