King's College London, United Kingdom.
Columbia Mailman School of Public Health, New York, New York.
J Am Acad Child Adolesc Psychiatry. 2021 Sep;60(9):1147-1156. doi: 10.1016/j.jaac.2020.12.033. Epub 2021 Jan 10.
To understand whether genetic risk for attention-deficit/hyperactivity disorder (ADHD) is associated with the course of the disorder across childhood and into young adulthood.
Participants were from the Environmental Risk (E-Risk) Longitudinal Twin Study, a population-based birth cohort of 2,232 twins. ADHD was assessed at ages 5, 7, 10, and 12 with mother- and teacher-reports and at age 18 with self-report. Polygenic risk scores (PRSs) were created using a genome-wide association study of ADHD case status. Associations with PRS were examined at multiple points in childhood and longitudinally from early childhood to adolescence. We investigated ADHD PRS and course to young adulthood, as reflected by ADHD remission, persistence, and late onset.
Participants with higher ADHD PRSs had increased risk for meeting ADHD diagnostic criteria (odds ratios ranging from 1.17 at age 10 to 1.54 at age 12) and for elevated symptoms at ages 5, 7, 10, and 12. Higher PRS was longitudinally associated with more hyperactivity/impulsivity (incidence rate ratio = 1.18) and inattention (incidence rate ratio = 1.14) from age 5 to age 12. In young adulthood, participants with persistent ADHD exhibited the highest PRS (mean PRS = 0.37), followed by participants with remission (mean PRS = 0.21); both groups had higher PRS than controls (mean PRS = -0.03), but did not significantly differ from one another. Participants with late-onset ADHD did not show elevated PRS for ADHD, depression, alcohol dependence, or marijuana use disorder.
Genetic risk scores derived from case-control genome-wide association studies may have relevance not only for incidence of mental health disorders, but also for understanding the longitudinal course of mental health disorders.
了解注意力缺陷多动障碍(ADHD)的遗传风险是否与该障碍在儿童期及进入青年期的病程有关。
参与者来自环境风险(E-Risk)纵向双胞胎研究,这是一项基于人群的 2232 对双胞胎出生队列研究。ADHD 采用母亲和教师报告的方式在 5、7、10 和 12 岁进行评估,并采用自我报告的方式在 18 岁进行评估。使用 ADHD 病例状态的全基因组关联研究创建多基因风险评分(PRS)。在儿童期的多个时间点以及从儿童早期到青春期的纵向进行 PRS 与 ADHD 的关联研究。我们研究了 ADHD PRS 与进入青年期的病程的关系,反映在 ADHD 的缓解、持续存在和晚发上。
具有较高 ADHD PRS 的参与者患 ADHD 诊断标准的风险增加(10 岁时的优势比范围为 1.17 至 12 岁时的 1.54),且在 5、7、10 和 12 岁时出现症状升高。较高的 PRS 与从 5 岁到 12 岁的多动/冲动(发病率比为 1.18)和注意力不集中(发病率比为 1.14)的纵向关联。在青年期,持续存在 ADHD 的参与者表现出最高的 PRS(平均 PRS 为 0.37),其次是缓解的参与者(平均 PRS 为 0.21);与对照组相比(平均 PRS 为-0.03),两组的 PRS 均较高,但彼此之间没有显著差异。晚发 ADHD 参与者的 ADHD、抑郁、酒精依赖或大麻使用障碍的 PRS 没有升高。
源自病例对照全基因组关联研究的遗传风险评分不仅与精神疾病的发病率有关,而且与精神疾病的纵向病程有关。
