Bérard Anick, Gaedigk Andrea, Sheehy Odile, Chambers Christina, Roth Mark, Bozzo Pina, Johnson Diana, Kao Kelly, Lavigne Sharon, Wolfe Lori, Quinn Dee, Dieter Kristen, Zhao Jin-Ping
Faculty of Pharmacy, University of MontrealMontreal, QC, Canada.
Research Center, CHU Sainte-JustineMontreal, QC, Canada.
Front Pharmacol. 2017 Jul 17;8:402. doi: 10.3389/fphar.2017.00402. eCollection 2017.
Polymorphic expression of drug metabolizing enzymes affects the metabolism of antidepressants, and thus can contribute to drug response and/or adverse events. Pregnancy itself can affect CYP2D6 activity with profound variations determined by genotype. To investigate the association between genotype and the risk of antidepressant discontinuation, dosage modification, and the occurrence of maternal , Antidepressants, Depression during pregnancy. Data from the Organization of Teratology Information Specialists (OTIS) Antidepressants in Pregnancy Cohort, 2006-2010, were used. Women were eligible if they were within 14 completed weeks of pregnancy at recruitment and exposed to an antidepressant or having any exposures considered non-teratogenic. Gestational antidepressant usage was self-reported and defined as continuous/discontinued use, and non-use; dosage modification was further documented. Maternal depression and anxiety were measured every trimester using the telephone interviewer-administered Edinburgh Postnatal Depression Scale and the Beck Anxiety Inventory, respectively. Saliva samples were collected and used for genotype analyses. Logistic regression models were used to calculate crude and adjusted odds ratios (OR) with 95% confidence intervals. A total of 246 pregnant women were included in the study. The majority were normal metabolizers (NM, = 204, 83%); 3.3% ( = 8) were ultrarapid metabolizers (UM), 5.7% ( = 14) poor metabolizers (PM), and 8.1% ( = 20) intermediate metabolizers (IM). Among study subjects, 139 women were treated with antidepressants at the beginning of pregnancy, and 21 antidepressant users (15%) discontinued therapy during pregnancy. Adjusting for depressive symptoms, and other potential confounders, the risk of discontinuing antidepressants during pregnancy was nearly four times higher in slow metabolizers (poor or intermediate metabolizers) compared to those with a faster metabolism rate (normal or ultrarapid metabolizers), aOR = 3.57 (95% CI: 1.15-11.11). Predicted CYP2D6 metabolizer status did not impact dosage modifications. Compared with slow metabolizers, significantly higher proportion of women in the fast metabolizer group had depressive symptom in the first trimester (19.81 vs. 5.88%, = 0.049). Almost 21% of treated women remained depressed during pregnancy (14.4% NM-UM; 6.1% PM-IM). Prior knowledge of genotype may help to identify pregnant women at greater risk of antidepressant discontinuation. Twenty percent of women exposed to antidepressants during pregnancy remained depressed, indicating an urgent need for personalized treatment of depression during pregnancy.
药物代谢酶的多态性表达会影响抗抑郁药的代谢,进而可能导致药物反应和/或不良事件。妊娠本身会影响CYP2D6的活性,其变化程度由基因型决定。为了研究基因型与抗抑郁药停药风险、剂量调整以及母亲发生抑郁症、妊娠期抑郁症之间的关联。使用了2006 - 2010年畸形学信息专家组织(OTIS)妊娠队列中抗抑郁药的数据。如果女性在招募时怀孕14周以内且暴露于抗抑郁药或有任何被认为非致畸性的暴露,则符合入选条件。妊娠期抗抑郁药的使用情况通过自我报告确定,分为持续/停药使用和未使用;剂量调整有进一步记录。分别在每个孕期通过电话访谈员管理的爱丁堡产后抑郁量表和贝克焦虑量表测量母亲的抑郁和焦虑情况。收集唾液样本用于基因型分析。使用逻辑回归模型计算粗比值比(OR)和调整后的比值比(95%置信区间)。该研究共纳入246名孕妇。大多数为正常代谢者(NM,n = 204,83%);3.3%(n = 8)为超快代谢者(UM),5.7%(n = 14)为慢代谢者(PM),8.1%(n = 20)为中间代谢者(IM)。在研究对象中,139名女性在妊娠开始时接受抗抑郁药治疗,21名抗抑郁药使用者(15%)在孕期停药。在调整抑郁症状和其他潜在混杂因素后,与代谢较快的人群(正常或超快代谢者)相比,慢代谢者(慢或中间代谢者)在孕期停用抗抑郁药的风险几乎高出四倍,调整后的比值比 = 3.57(95%置信区间:1.15 - 11.11)。预测的CYP2D6代谢者状态不影响剂量调整。与慢代谢者相比,超快代谢者组中在孕早期有抑郁症状的女性比例显著更高(19.81%对5.88%,P = 0.049)。近21%接受治疗的女性在孕期仍处于抑郁状态(超快代谢者 - 正常代谢者为14.4%;慢代谢者 - 中间代谢者为6.1%)。了解基因型可能有助于识别抗抑郁药停药风险更高的孕妇。20%在孕期暴露于抗抑郁药的女性仍处于抑郁状态,这表明孕期抑郁症的个性化治疗迫在眉睫。
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