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Use of antidepressants with pharmacogenetic prescribing guidelines in a 10-year depression cohort of adult primary care patients

机译:在10年的成人初级护理患者中使用抗抑郁药与药物发生的指导原则

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Objective To describe the usage patterns of antidepressants with publishedCYP2D6- andCYP2C19-based prescribing guidelines among depressed primary care patients and estimate the proportion of patients taking antidepressants not recommended for them based on theirCYP2C19andCYP2D6genotype-predicted metabolizer status. Methods Medication use and pharmacogenetic testing results were collected on 128 primary care patients enrolled in a 10-year depression cohort study. At each 12-month interval, we calculated the proportion of patients that: (1) reported use of one or more of the 13 antidepressant medications (i.e. amitriptyline, citalopram, escitalopram, clomipramine, desipramine, doxepin, fluvoxamine, imipramine, nortriptyline, paroxetine, sertraline, trimipramine, venlafaxine) with publishedCYP2D6- andCYP2C19-based prescribing guidelines, (2) were taking an antidepressant that was not recommended for them based on theirCYP2C19andCYP2D6genotype-predicted metabolizer phenotype, and (3) switched medications from the previous 12-month interval. Results The annual proportion of individuals taking an antidepressant with aCYP2D6- andCYP2C19-based prescribing guidelines ranged from 45 to 84%. The proportion of participants that used an antidepressant that was not recommended for them, based on availableCYP2D6andCYP2C19metabolizer phenotype, ranged from 18 to 29% and these individuals tended to switch medications more frequently (10%) compared to their counterparts taking medication aligned with their metabolizer phenotype (6%). Conclusion One-quarter of primary care patients used an antidepressant that was not recommended for them based onCYP2D6- andCYP2C19-based prescribing guidelines and switching medications tended to be more common in this group. Studies to determine the impact ofCYP2D6andCYP2C19genotyping on reducing gene-antidepressant mismatches are warranted.
机译:目的描述抑郁型初级护理患者的出版物的抗抑郁药的用法模式,并估计基于INCYP2C19AdcyP2D6Genotype预测的代谢物状态的不推荐给予抗抑郁药的患者比例。方法收集了在10年抑郁群体研究中注册的128名初级护理患者的药物使用和药物发生测试结果。在每12个月间隔,我们计算了以下患者的比例:(1)报告使用13种抗抑郁药物中的一种或多种(即amitiptyline,西酞普兰,亚太经产申请,氯鱼胺,脱脂,Doxepin,Fluvoxamine,Imipramine,Nortriptyline,Paroxetine具有PublishedCyp2D6-和Cyp2C19的处方指南的塞拉甲酮,甲脂蛋白甘露嘧胺,venlafaxine,(2)是基于其COP2C19andcyP2D6Genotype预测的代谢物表型,而不是向其推荐的抗抑郁药,以及来自前12个月间隔的(3)切换药物。结果患有ACYP2D6-ANDCYP2C19的处方指南的抗抑郁药的年度比例范围为45%至84%。使用不推荐给它们的抗抑郁药的参与者的比例,基于afifablecyp2d6andcyp2c19metabolizer表型,而这些个体与他们的代谢物表型相比更频繁地(10%)更频繁地切换药物(10%) (6%)。结论四分之一的初级护理患者使用不推荐的抗抑郁药,这些抗抑郁药是基于onCyp2D6-Andcyp2C19的处方指南,并在该组中切换药物往往更常见。有必要研究确定Cyp2D6Andcyp2C19G12G12G12G12G12G12G12G12G12G12G12G19Gancoctics关于还原基因 - 抗抑郁药错配的影响。

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