Pierre Desaunay, Léa-Gabrielle Eude, Michel Dreyfus, Cénéric Alexandre, Sophie Fedrizzi, Joachim Alexandre, Faruk Uguz, Fabian Guénolé
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Meta-analyses (MAs), which increase the statistical power and precision of results, have gained interest for assessing the safety of antidepressant drugs during pregnancy.</p><p><strong>Objective: </strong>We aimed to provide a meta-review of MAs assessing the benefits and risks of antidepressant drug use during pregnancy.</p><p><strong>Methods: </strong>Following Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines, a literature search on PubMed and Web of Science databases was conducted on 25 October, 2021, on MAs assessing the association between antidepressant drug use during pregnancy and health outcomes for the pregnant women, embryo, fetus, newborn, and developing child. Study selection and data extraction were carried out independently and in duplicate by two authors. The methodological quality of included studies was evaluated with the AMSTAR-2 tool. Overlap among MAs was assessed by calculating the corrected covered area. Data were presented in a narrative synthesis, using four levels of evidence.</p><p><strong>Results: </strong>Fifty-one MAs were included, all but one assessing risks. These provided evidence for a significant increase in the risks for major congenital malformations (selective serotonin reuptake inhibitors, paroxetine, fluoxetine, no evidence for sertraline; eight MAs), congenital heart defects (paroxetine, fluoxetine, sertraline; 11 MAs), preterm birth (eight MAs), neonatal adaptation symptoms (eight MAs), and persistent pulmonary hypertension of the newborn (three MAs). There was limited evidence (only one MA for each outcome) for a significant increase in the risks for postpartum hemorrhage, and with a high risk of bias, for stillbirth, impaired motor development, and intellectual disability. There was inconclusive evidence, i.e., discrepant results, for an increase in the risks for spontaneous abortion, small for gestational age and low birthweight, respiratory distress, convulsions, feeding problems, and for a subsequent risk for autism with an early antidepressant drug exposure. Finally, MAs provided no evidence for an increase in the risks for gestational hypertension, preeclampsia, and for a subsequent risk for attention-deficit/hyperactivity disorder. Only one MA assessed benefits, providing limited evidence for preventing relapse in severe or recurrent depression. Effect sizes were small, except for neonatal symptoms (small to large). Results were based on MAs in which overall methodological quality was low (AMSTAR-2 score = 54.8% ± 12.9%, [19-81%]), with a high risk of bias, notably indication bias. 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引用次数: 3
摘要
背景:几十年来,妊娠期间抗抑郁药物的处方一直在稳步增加。荟萃分析(meta - analysis, MAs)提高了结果的统计能力和准确性,在评估妊娠期间抗抑郁药物的安全性方面引起了人们的兴趣。目的:我们旨在提供一项荟萃综述,评估妊娠期间使用抗抑郁药物的益处和风险。方法:遵循PRISMA (Preferred Reporting Items for Systematic Reviews and meta - analysis)指南,于2021年10月25日对PubMed和Web of Science数据库进行文献检索,以评估妊娠期抗抑郁药物使用与孕妇、胚胎、胎儿、新生儿和发育中的儿童健康结局之间的关系。研究选择和数据提取是由两位作者独立进行的,一式两份。采用AMSTAR-2工具评价纳入研究的方法学质量。通过计算修正的覆盖面积来评估MAs之间的重叠。数据以叙事综合的方式呈现,使用四个层次的证据。结果:纳入51例MAs,除1例外均为风险评估。这些为重大先天性畸形的风险显著增加提供了证据(选择性血清素再摄取抑制剂、帕罗西汀、氟西汀,舍曲林无证据;8个MAs),先天性心脏缺陷(帕罗西汀,氟西汀,舍曲林;11个MAs)、早产(8个MAs)、新生儿适应症状(8个MAs)和新生儿持续性肺动脉高压(3个MAs)。有限的证据(每个结果只有一个MA)表明产后出血的风险显著增加,并且存在较高的偏倚风险,包括死产、运动发育受损和智力残疾。对于自然流产、胎龄小、出生体重低、呼吸窘迫、抽搐、喂养问题的风险增加,以及早期接触抗抑郁药物后的自闭症风险,没有确凿的证据,即结果不一致。最后,MAs没有提供证据表明妊娠期高血压、先兆子痫以及随后的注意缺陷/多动障碍的风险增加。只有一个MA评估了益处,提供了有限的证据来预防严重或复发性抑郁症的复发。除新生儿症状外,效应量很小(从小到大)。结果基于总体方法学质量较低的MAs (AMSTAR-2评分= 54.8%±12.9%,[19-81%]),偏倚风险较高,特别是指指偏倚。校正后的覆盖面积为3.27%,对应有轻微的重叠。结论:本荟萃综述对临床实践和未来研究具有启示意义。首先,这些结果表明抗抑郁药物应该作为怀孕期间的二线治疗(根据指南,在一线心理治疗之后)。通过遵守不鼓励使用帕罗西汀和氟西汀的指南,可以预防重大先天性畸形的风险。其次,为了减少异质性和偏倚,未来的ma应该调整产妇精神疾病和抗抑郁药物剂量,并通过暴露时间进行分析。
Benefits and Risks of Antidepressant Drugs During Pregnancy: A Systematic Review of Meta-analyses.
Background: The prescription of antidepressant drugs during pregnancy has been steadily increasing for several decades. Meta-analyses (MAs), which increase the statistical power and precision of results, have gained interest for assessing the safety of antidepressant drugs during pregnancy.
Objective: We aimed to provide a meta-review of MAs assessing the benefits and risks of antidepressant drug use during pregnancy.
Methods: Following Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines, a literature search on PubMed and Web of Science databases was conducted on 25 October, 2021, on MAs assessing the association between antidepressant drug use during pregnancy and health outcomes for the pregnant women, embryo, fetus, newborn, and developing child. Study selection and data extraction were carried out independently and in duplicate by two authors. The methodological quality of included studies was evaluated with the AMSTAR-2 tool. Overlap among MAs was assessed by calculating the corrected covered area. Data were presented in a narrative synthesis, using four levels of evidence.
Results: Fifty-one MAs were included, all but one assessing risks. These provided evidence for a significant increase in the risks for major congenital malformations (selective serotonin reuptake inhibitors, paroxetine, fluoxetine, no evidence for sertraline; eight MAs), congenital heart defects (paroxetine, fluoxetine, sertraline; 11 MAs), preterm birth (eight MAs), neonatal adaptation symptoms (eight MAs), and persistent pulmonary hypertension of the newborn (three MAs). There was limited evidence (only one MA for each outcome) for a significant increase in the risks for postpartum hemorrhage, and with a high risk of bias, for stillbirth, impaired motor development, and intellectual disability. There was inconclusive evidence, i.e., discrepant results, for an increase in the risks for spontaneous abortion, small for gestational age and low birthweight, respiratory distress, convulsions, feeding problems, and for a subsequent risk for autism with an early antidepressant drug exposure. Finally, MAs provided no evidence for an increase in the risks for gestational hypertension, preeclampsia, and for a subsequent risk for attention-deficit/hyperactivity disorder. Only one MA assessed benefits, providing limited evidence for preventing relapse in severe or recurrent depression. Effect sizes were small, except for neonatal symptoms (small to large). Results were based on MAs in which overall methodological quality was low (AMSTAR-2 score = 54.8% ± 12.9%, [19-81%]), with a high risk of bias, notably indication bias. The corrected covered area was 3.27%, which corresponds to a slight overlap.
Conclusions: This meta-review has implications for clinical practice and future research. First, these results suggest that antidepressant drugs should be used as a second-line treatment during pregnancy (after first-line psychotherapy, according to the guidelines). The risk of major congenital malformations could be prevented by observing guidelines that discourage the use of paroxetine and fluoxetine. Second, to decrease heterogeneity and bias, future MAs should adjust for maternal psychiatric disorders and antidepressant drug dosage, and perform analyses by timing of exposure.
期刊介绍:
Pediatric Drugs promotes the optimization and advancement of all aspects of pharmacotherapy for healthcare professionals interested in pediatric drug therapy (including vaccines). The program of review and original research articles provides healthcare decision makers with clinically applicable knowledge on issues relevant to drug therapy in all areas of neonatology and the care of children and adolescents. The Journal includes:
-overviews of contentious or emerging issues.
-comprehensive narrative reviews of topics relating to the effective and safe management of drug therapy through all stages of pediatric development.
-practical reviews covering optimum drug management of specific clinical situations.
-systematic reviews that collate empirical evidence to answer a specific research question, using explicit, systematic methods as outlined by the PRISMA statement.
-Adis Drug Reviews of the properties and place in therapy of both newer and established drugs in the pediatric population.
-original research articles reporting the results of well-designed studies with a strong link to clinical practice, such as clinical pharmacodynamic and pharmacokinetic studies, clinical trials, meta-analyses, outcomes research, and pharmacoeconomic and pharmacoepidemiological studies.
Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in Pediatric Drugs may be accompanied by plain language summaries to assist readers who have some knowledge of, but not in-depth expertise in, the area to understand important medical advances.