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Evaluation of risk factors for elevated tricyclic antidepressant plasma concentrations.

机译:三环类抗抑郁药血浆浓度升高的危险因素评估。

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PURPOSE: To quantify the effect of clinical and demographic factors on the risk of elevated and toxic tricyclic antidepressant (TCA) plasma concentrations (Cp) and to describe the rates of elevated and toxic TCA Cp. METHODS: This matched, case-control study was conducted among adult patients enrolled in a group model HMO who had a TCA Cp laboratory measurement and purchased at least one TCA prescription for either amitriptyline or nortriptyline during the 70 days preceding the TCA Cp measurement. Predictive models of experiencing an elevated or toxic Cp were created using multivariate conditional logistic regression. RESULTS: At least one Cp was drawn in 1057 unique patients with a TCA purchase. Of these, 18.4% (194/1057) patients (cases) had an elevated TCA Cp and were matched to 716 non-elevated Cp patients. Additionally, 27.3% (53/194) of the cases (matched to 196 controls) experienced a toxic TCA Cp. The best fitting model of an elevated TCA Cp included TCA dose category (daily doses >or=150 mg, OR = 4.08; doses of 50 to <100 mg, OR = 0.36; and doses <50 mg, OR = 0.18, p < 0.05 for all comparisons), female gender (OR = 1.78, p < 0.05) and concurrent use of fluoxetine or paroxetine (OR = 1.75, p < 0.05). The best fitting predictive model of a toxic TCA Cp included the same factors as for the predictive model of an elevated TCA Cp. CONCLUSIONS: Recognizing and monitoring predictors of elevated or toxic TCA Cps, including increasing TCA dose, female gender, and concurrent use of fluoxetine or paroxetine, may reduce serious adverse drug reactions and deaths in the TCA-receiving patient population.
机译:目的:量化临床和人口统计学因素对三环抗抑郁药(TCA)血药浓度升高(Cp)风险的影响,并描述三环抗抑郁药(TCA Cp)升高和毒性的发生率。方法:这项配对病例对照研究是针对参加HMO​​组模型的成年患者进行的,这些患者具有TCA Cp实验室测量值,并且在TCA Cp测量前70天内购买了至少一种阿米替林或去甲替林的TCA处方。使用多元条件对数回归建立预测的Cp升高或毒性模型。结果:在购买了TCA的1057位独特患者中,至少抽取了Cp。在这些患者中,有18.4%(194/1057)患者(病例)的TCA Cp升高,并与716例未升高的Cp患者匹配。此外,27.3%(53/194)的病例(与196个对照匹配)经历了毒性TCA Cp。 TCA Cp升高的最佳拟合模型包括TCA剂量类别(每日剂量>或= 150 mg,OR = 4.08; 50至<100 mg,OR = 0.36;剂量<50 mg,OR = 0.18,p <所有比较均为0.05),女性(OR = 1.78,p <0.05)和同时使用氟西汀或帕罗西汀(OR = 1.75,p <0.05)。毒性TCA Cp的最佳拟合预测模型包括与TCA Cp升高的预测模型相同的因素。结论:识别和监测TCA Cps升高或中毒的预测因素,包括增加TCA剂量,女性性别以及同时使用氟西汀或帕罗西汀,可能会减少接受TCA的患者中的严重药物不良反应和死亡。

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