Institute of Biological Psychiatry, Mental Health Services, Copenhagen University Hospital, Copenhagen, Denmark.
The Lundbeck Foundation Initiative for Integrative Psychiatric Research, Copenhagen and Aarhus, Denmark.
JAMA Psychiatry. 2022 Jan 1;79(1):59-69. doi: 10.1001/jamapsychiatry.2021.3392.
Although the association between several recurrent genomic copy number variants (CNVs) and mental disorders has been studied for more than a decade, unbiased, population-based estimates of the prevalence, disease risks and trajectories, fertility, and mortality to contrast chromosomal abnormalities and advance precision health care are lacking.
To generate unbiased, population-based estimates of prevalence, disease risks and trajectories, fertility, and mortality of CNVs implicated in neuropsychiatric disorders.
DESIGN, SETTING, AND PARTICIPANTS: In a population-based case-cohort study, using the Lundbeck Foundation Initiative for Integrative Psychiatric Research (iPSYCH) 2012 database, individuals born between May 1, 1981, and December 31, 2005, and followed up until December 31, 2012, were analyzed. All individuals (n = 57 377) with attention-deficit/hyperactivity disorder (ADHD), major depressive disorder (MDD), schizophrenia (SCZ), autism spectrum disorder (ASD), or bipolar disorder (BPD) were included, as well as 30 000 individuals randomly drawn from the database. Data analysis was conducted from July 1, 2017, to September 7, 2021.
Copy number variants at 6 genomic loci (1q21.1, 15q11.2, 15q13.3, 16p11.2, 17p12, and 17q12).
Population-unbiased hazard ratio (HR) and survival estimates of CNV associations with the 5 ascertained psychiatric disorders, epilepsy, intellectual disability, selected somatic disorders, fertility, and mortality.
Participants' age ranged from 1 to 32 years (mean, 12.0 [IQR, 6.9] years) during follow-up, and 38 662 were male (52.3%). Copy number variants broadly associated with an increased risk of autism spectrum disorder and ADHD, whereas risk estimates of SCZ for most CNVs were lower than previously reported. Comparison with previous studies suggests that the lower risk estimates are associated with a higher CNV prevalence in the general population than in control samples of most case-control studies. Significant risk of major depressive disorder (HR, 5.8; 95% CI, 1.5-22.2) and sex-specific risk of bipolar disorder (HR, 17; 95% CI, 1.5-189.3, in men only) were noted for the 1q21.1 deletion. Although CNVs at 1q21.1 and 15q13.3 were associated with increased risk across most diagnoses, the 17p12 deletion consistently conferred less risk of psychiatric disorders (HR 0.4-0.8), although none of the estimates differed significantly from the general population. Trajectory analyses noted that, although diagnostic risk profiles differed across loci, they were similar for deletions and duplications within each locus. Sex-stratified analyses suggest that pathogenicity of many CNVs may be modulated by sex.
The findings of this study suggest that the iPSYCH population case cohort reveals broad disease risk for some of the studied CNVs and narrower risk for others, in addition to sex differential liability. This finding on genomic risk variants at the level of a population may be important for health care planning and clinical decision making, and thus the advancement of precision health care.
尽管已有十余年的时间研究了几种复发性基因组拷贝数变异(CNV)与精神障碍之间的关联,但缺乏无偏倚的、基于人群的患病率、疾病风险和轨迹、生育能力和死亡率估计值,以对比染色体异常并推进精准医疗保健。
生成与神经精神障碍相关的 CNV 的无偏倚、基于人群的患病率、疾病风险和轨迹、生育能力和死亡率的估计值。
设计、地点和参与者:在一项基于人群的病例-队列研究中,利用 Lundbeck 基金会综合精神医学研究倡议(iPSYCH)2012 数据库,分析了 1981 年 5 月 1 日至 2005 年 12 月 31 日出生并随访至 2012 年 12 月 31 日的个体。所有患有注意力缺陷/多动障碍(ADHD)、重度抑郁症(MDD)、精神分裂症(SCZ)、自闭症谱系障碍(ASD)或双相情感障碍(BPD)的个体(n=57377)以及从数据库中随机抽取的 30000 名个体均被纳入研究。数据分析于 2017 年 7 月 1 日至 2021 年 9 月 7 日进行。
6 个基因组位置(1q21.1、15q11.2、15q13.3、16p11.2、17p12 和 17q12)的拷贝数变异。
CNV 与 5 种已确定的精神障碍、癫痫、智力障碍、某些躯体疾病、生育能力和死亡率相关的无偏风险比(HR)和生存估计值。
参与者在随访期间的年龄范围为 1 至 32 岁(平均 12.0[IQR,6.9]岁),其中 38662 人为男性(52.3%)。拷贝数变异广泛与自闭症谱系障碍和 ADHD 的风险增加相关,而大多数 CNV 与 SCZ 的风险估计值低于之前的报道。与之前的研究相比,这表明较低的风险估计值与一般人群中 CNV 的患病率高于大多数病例对照研究的对照样本中的患病率有关。1q21.1 缺失与重度抑郁症的显著风险(HR,5.8;95%CI,1.5-22.2)和男性特有的双相情感障碍风险(HR,17;95%CI,1.5-189.3)有关。尽管 1q21.1 和 15q13.3 的 CNVs 与大多数诊断相关的风险增加有关,但 17p12 缺失一致地降低了精神障碍的风险(HR 0.4-0.8),尽管这些估计值与一般人群没有显著差异。轨迹分析指出,尽管各位置的诊断风险特征不同,但在每个位置的缺失和重复中,风险特征相似。性别分层分析表明,许多 CNVs 的致病性可能受到性别的调节。
这项研究的结果表明,iPSYCH 人群病例队列揭示了一些研究 CNV 的广泛疾病风险,而另一些则风险较低,此外还存在性别差异。这一发现可能对医疗保健规划和临床决策以及精准医疗保健的推进具有重要意义。
