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Lancet Psychiatry. 2024 Jun;11(6):461-471. doi: 10.1016/S2215-0366(24)00060-9. Epub 2024 Apr 18.
3
The Avon Longitudinal Study of Parents and Children (ALSPAC): a 2022 update on the enrolled sample of mothers and the associated baseline data.雅芳亲子纵向研究(ALSPAC):2022年母亲入组样本及相关基线数据更新
Wellcome Open Res. 2023 Sep 6;7:283. doi: 10.12688/wellcomeopenres.18564.1. eCollection 2022.
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Empirically driven transdiagnostic stages in the development of mood, anxiety and psychotic symptoms in a cohort of youth followed from birth.从出生起就对该队列中的年轻人的情绪、焦虑和精神病症状进行了实证驱动的跨诊断阶段研究。
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Age at onset of mental disorders worldwide: large-scale meta-analysis of 192 epidemiological studies.全球精神障碍发病年龄:192 项流行病学研究的大规模荟萃分析。
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从童年到青年期跨诊断阶段的进展。

Progression of Transdiagnostic Stages From Childhood to Young Adulthood.

作者信息

Ratheesh Aswin, Chen Yufan, Hammond Dylan, Aitken Zoe, Shah Jai, Iorfino Frank, Scott Jan, Hickie Ian, Davey Chris, Chanen Andrew, Berk Michael, McGorry Patrick, Marwaha Steven, Thompson Andrew, Nelson Barnaby

机构信息

Discipline of Psychiatry and Mental Health, University of New South Wales, Sydney, New South Wales, Australia.

Centre for Youth Mental Health, University of Melbourne, Melbourne, Victoria, Australia.

出版信息

JAMA Psychiatry. 2025 Sep 24. doi: 10.1001/jamapsychiatry.2025.2648.

DOI:10.1001/jamapsychiatry.2025.2648
PMID:40991272
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12461601/
Abstract

IMPORTANCE

Transdiagnostic clinical staging models for mental disorders are receiving increased attention. However, their underlying assumptions are underresearched; for example, it is not clear whether the observed progression across stages occurs independently of preexisting risk factors.

OBJECTIVES

To test the likelihood of progression from stage 0 (familial risk) in childhood to stage 1a (mild symptoms) in adolescence and subsequently to stage 1b (clinically significant symptoms) in young adulthood, accounting for confounders, and to explore potential mediators.

DESIGN, SETTING, AND PARTICIPANTS: This prospective cohort study included participants from the Avon Longitudinal Study of Parents and Children (ALSPAC). ALSPAC included pregnant women and their offspring residing in Avon, United Kingdom, between 1991 and 1992, with a proportion of offspring followed up into young adulthood. Eligible participants provided data on stage determinants and potential confounders from birth until age 24 years. Data were collected from 1991 to 2015 and analyzed from January 2002 to June 2025.

EXPOSURES

Exposures were clinical stages 0 and 1a in separate tests of association with stages 1a and 1b, respectively. Criteria for stage 0 were the presence of schizophrenia or severe depression in a first-degree relative. Criteria for stage 1a were the presence of 1 to 2 symptoms of depression, anxiety, or psychosis at ages 12 to 13 years.

MAIN OUTCOMES AND MEASURES

Outcomes were stage 1a in adolescence and stage 1b in young adulthood. Criteria for stage 1b were at least moderate symptoms of depression, anxiety, or psychosis, with associated functional impact at ages 18 to 24 years. Confounders were sex assigned at birth, obstetric risk, parental social class, ethnicity, family adversity, temperament, early life events, and neurocognition, measured in childhood.

RESULTS

Among those with complete data at all 3 time points (1375 participants; weighted, 7342), 796 participants (57.9%; weighted, 51.5%) were female and 579 (42.1%; weighted, 48.5%) were male. After adjusting for potential confounders, there was an association between stage 0 in childhood and stage 1a in adolescence (3860 participants; weighted, 7388 participants; odds ratio [OR], 1.65, 95% CI, 1.30-2.11) and between stage 1a in adolescence and stage 1b in young adulthood (1661 participants; weighted, 7466 participants; OR, 2.07; 95% CI, 1.07-4.01). Level of neuroticism in adolescence mediated 18% of the association between stage 1a in adolescence and stage 1b in young adulthood.

CONCLUSIONS AND RELEVANCE

In this cohort study, young people with mental health problems meeting criteria for early clinical stages were at heightened risk of developing subsequent stages, independent of early life risk factors. This study supports the assumption of progression underlying clinical staging models for mental disorders.

摘要

重要性

精神障碍的跨诊断临床分期模型正受到越来越多的关注。然而,其潜在假设尚未得到充分研究;例如,尚不清楚观察到的各阶段进展是否独立于先前存在的风险因素。

目的

检验从儿童期的0期(家族风险)进展到青春期的1a期(轻度症状),随后进展到青年期的1b期(具有临床意义的症状)的可能性,同时考虑混杂因素,并探索潜在的中介因素。

设计、设置和参与者:这项前瞻性队列研究纳入了阿冯父母与儿童纵向研究(ALSPAC)的参与者。ALSPAC包括1991年至1992年间居住在英国阿冯的孕妇及其后代,部分后代随访至青年期。符合条件的参与者提供了从出生到24岁的阶段决定因素和潜在混杂因素的数据。数据收集时间为1991年至2015年,分析时间为2002年1月至2025年6月。

暴露因素

在分别与1a期和1b期的关联测试中,暴露因素分别为0期和1a期临床阶段。0期标准为一级亲属患有精神分裂症或重度抑郁症。1a期标准为在12至13岁时出现1至2种抑郁、焦虑或精神病症状。

主要结局和测量指标

结局为青春期的1a期和青年期的1b期。1b期标准为在18至24岁时至少有中度抑郁、焦虑或精神病症状,并伴有相关功能影响。混杂因素包括出生时指定的性别、产科风险、父母社会阶层、种族、家庭逆境、气质、早期生活事件和儿童期测量的神经认知。

结果

在所有3个时间点都有完整数据的参与者中(1375名参与者;加权后为7342名),796名参与者(57.9%;加权后为51.5%)为女性,579名(42.1%;加权后为48.5%)为男性。在调整潜在混杂因素后,儿童期的0期与青春期的1a期之间存在关联(3860名参与者;加权后为7388名参与者;比值比[OR]为1.65,95%置信区间为1.30 - 2.11),青春期的1a期与青年期的1b期之间也存在关联(1661名参与者;加权后为7466名参与者;OR为2.07;95%置信区间为1.07 - 4.01)。青春期的神经质水平介导了青春期的1a期与青年期的1b期之间18%的关联。

结论与意义

在这项队列研究中,符合早期临床阶段标准的有心理健康问题的年轻人发展为后续阶段的风险增加,且独立于早期生活风险因素。本研究支持精神障碍临床分期模型所基于的进展假设。