青少年抑郁症的治疗是否能降低后期精神病的风险:一项准实验研究,选择性5 -羟色胺再摄取抑制剂治疗在总人口队列中。

IF 6.7
Colm Healy, Kirsite O'Hare, Ulla Lång, Martta Kerkelä, Jonah Byrne, Juha Veijola, Anna Pulakka, Johanna Metsälä, Eero Kajantie, Ian Kelleher
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引用次数: 0

摘要

背景:精神障碍通常以抑郁障碍为前驱,并且已经假设在青年时期治疗抑郁症可能会降低后期精神病的风险。使用准实验方法,我们估计了选择性血清素再摄取抑制剂(SSRIs)治疗青少年抑郁症与后期精神病风险之间的因果关系。方法:我们使用来自多个芬兰国家登记处的数据链接,包括1987年至1997年间出生的所有个体(n = 697,289),以确定18岁之前诊断的抑郁症,诊断三年内累积的SSRI治疗,以及随访结束时诊断的非情感性精神障碍(20-29岁)。我们使用工具变量分析,利用不同医院地区处方的可变性来估计因果关系。采用两阶段最小二乘模型进行分析。敏感性分析检查了混杂因素分层的影响和特定SSRIs的影响。结果:我们最终的样本包括22,666名被诊断为青春期抑郁症的个体,其中60.2% (n = 13,650)使用过SSRIs。10.7%患有抑郁症的青少年后来被诊断为非情感性精神障碍。SSRI治疗青少年抑郁症与发生精神障碍的风险降低无关(1年β = 0.04,CI:-0.01至0.09;2年β = 0.02,CI:-0.06 ~ 0.09;3年β = -0.02,CI:-0.08 ~ 0.05)。结论:我们的准实验研究不支持青少年抑郁症治疗降低后续精神病风险的假设。我们的研究结果质疑了一种假设,即对青少年常见精神健康障碍的治疗可能会影响成年后患严重精神疾病的风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Does treatment of adolescent depression reduce risk of later psychosis: A quasi-experimental study of selective serotonin reuptake inhibitor treatment in a total population cohort.

Background: Psychotic disorders are frequently preceded by depressive disorders, and it has been hypothesized that treatment of depression in youth may reduce risk for later psychosis. Using quasi-experimental methods, we estimated the causal relationship between the treatment of adolescent depression with selective serotonin reuptake inhibitors (SSRIs) and the risk of later psychosis.

Methods: We used data linkage from multiple national Finnish registries for all individuals (n = 697,289) born between 1987 and 1997 to identify depression diagnosed before age 18, cumulative SSRI treatment within three years of diagnosis, and diagnoses of non-affective psychotic disorders by end of follow-up (age 20-29). We used instrumental variable analyses, exploiting variability in prescribing across hospital districts to estimate causal effects. Analyses were conducted using two-stage least squares modelling. Sensitivity analyses examined effects stratified by confounders and effects of specific SSRIs.

Results: Our final sample included 22,666 individuals diagnosed with depression in adolescence, of whom 60.2% (n = 13,650) had used SSRIs. 10.7% of adolescents with depression went on to be diagnosed with a non-affective psychotic disorder. SSRI treatment for adolescent depression was not associated with a reduced risk of developing a psychotic disorder (one-year β = 0.04,CI:-0.01 to 0.09; two-years β = 0.02,CI:-0.06 to 0.09; three-years β = -0.02,CI:-0.08 to 0.05).

Conclusions: Our quasi-experimental investigation does not support the hypothesis that treatment of adolescent depression reduces the subsequent risk of psychosis. Our findings question the assumption that treatment of common mental health disorders in youth may impact the risk of developing severe mental illnesses in adulthood.

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