Mediational pathways between aggregate genetic liability and nonfatal suicide attempt: A Swedish population-based cohort

IF 1.6 3区医学 Q3 GENETICS & HEREDITY

American Journal of Medical Genetics Part B: Neuropsychiatric Genetics Pub Date : 2024-02-17 DOI:10.1002/ajmg.b.32974

Séverine Lannoy, Henrik Ohlsson, Mallory Stephenson, Jan Sundquist, Kristina Sundquist, Alexis C. Edwards

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Abstract

Despite recent progress in the genetics of suicidal behavior, the pathway by which genetic liability increases suicide attempt risk is unclear. We investigated the mediational pathways from family/genetic risk for suicide attempt (FGRS_SA) to suicide attempt by considering the roles of psychiatric illnesses. In a Swedish cohort, we evaluated time to suicide attempt as a function of FGRS_SA and the mediational effects of alcohol use disorder, drug use disorder, attention-deficit/hyperactivity disorder, major depression, anxiety disorder, bipolar disorder, and non-affective psychosis. Analyses were conducted by sex in three age periods: 15–25 years (N_females = 850,278 and N_males = 899,366), 26–35 years (N_females = 800,189 and N_males = 861,774), and 36–45 years (N_females = 498,285 and N_males = 535,831). The association between FGRS_SA and suicide attempt was mediated via psychiatric disorders. The highest mediation effects were observed for alcohol use disorder in males (15–25 years, HR_total = 1.60 [1.59; 1.62], mediation = 14.4%), drug use disorder in females (25–36 years, HR_total = 1.46 [1.44; 1.49], mediation = 11.2%), and major depression (25–36 years) in females (HR_total = 1.46 [1.44; 1.49], mediation = 7%) and males (HR_total = 1.50 [1.47;1.52], mediation = 4.7%). While the direct effect of FGRS_SA was higher at ages of 15–25, the mediation via psychiatric disorders was more prominent in later adulthood. Our study informs about the psychiatric illnesses via which genetic liability operates to impact suicide attempt risk, with distinct contributions according to age and sex.

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总体遗传责任与非致命自杀企图之间的中介途径：瑞典人群队列

尽管最近在自杀行为遗传学方面取得了进展，但遗传因素增加自杀未遂风险的途径尚不清楚。通过考虑精神疾病的作用，我们研究了从自杀未遂的家庭/遗传风险（FGRSSA）到自杀未遂的中介途径。在瑞典的一个队列中，我们评估了自杀未遂时间与 FGRSSA 的函数关系，以及酒精使用障碍、药物使用障碍、注意力缺陷/多动障碍、重度抑郁症、焦虑症、双相情感障碍和非情感性精神病的中介效应。按性别对三个年龄段进行了分析：15-25 岁（女性=850 278 人，男性=899 366 人）、26-35 岁（女性=800 189 人，男性=861 774 人）和 36-45 岁（女性=498 285 人，男性=535 831 人）。FGRSSA与自杀未遂之间的关联是通过精神障碍来调节的。男性酒精使用障碍（15-25 岁，HRtotal = 1.60 [1.59; 1.62]，中介 = 14.4%）、女性药物使用障碍（25-36 岁，HRtotal = 1.46[1.44；1.49]，调解 = 11.2%），以及女性（HRtotal = 1.46 [1.44；1.49]，调解 = 7%）和男性（HRtotal = 1.50 [1.47；1.52]，调解 = 4.7%）的重度抑郁症（25-36 岁）。在 15-25 岁年龄段，FGRSSA 的直接影响较高，而通过精神障碍产生的中介作用在成年后更为突出。我们的研究揭示了遗传因子对自杀未遂风险产生影响的精神疾病，不同年龄和性别的遗传因子对自杀未遂风险的影响各不相同。

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来源期刊

American Journal of Medical Genetics Part B: Neuropsychiatric Genetics 医学-精神病学

CiteScore

5.90

自引率

7.10%

发文量

审稿时长

4-8 weeks

期刊介绍： Neuropsychiatric Genetics, Part B of the American Journal of Medical Genetics (AJMG) , provides a forum for experimental and clinical investigations of the genetic mechanisms underlying neurologic and psychiatric disorders. It is a resource for novel genetics studies of the heritable nature of psychiatric and other nervous system disorders, characterized at the molecular, cellular or behavior levels. Neuropsychiatric Genetics publishes eight times per year.