Shared and divergent mental health characteristics of ADNP-, CHD8- and DYRK1A-related neurodevelopmental conditions

IF 4.1 2区 医学 Q1 CLINICAL NEUROLOGY Journal of Neurodevelopmental Disorders Pub Date : 2024-04-15 DOI:10.1186/s11689-024-09532-1
Emily Neuhaus, Hannah Rea, Elizabeth Jones, Hannah Benavidez, Conor Miles, Alana Whiting, Margaret Johansson, Curtis Eayrs, Evangeline C. Kurtz-Nelson, Rachel Earl, Raphael A. Bernier, Evan E. Eichler
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Abstract

Neurodevelopmental conditions such as intellectual disability (ID) and autism spectrum disorder (ASD) can stem from a broad array of inherited and de novo genetic differences, with marked physiological and behavioral impacts. We currently know little about the psychiatric phenotypes of rare genetic variants associated with ASD, despite heightened risk of psychiatric concerns in ASD more broadly. Understanding behavioral features of these variants can identify shared versus specific phenotypes across gene groups, facilitate mechanistic models, and provide prognostic insights to inform clinical practice. In this paper, we evaluate behavioral features within three gene groups associated with ID and ASD – ADNP, CHD8, and DYRK1A – with two aims: (1) characterize phenotypes across behavioral domains of anxiety, depression, ADHD, and challenging behavior; and (2) understand whether age and early developmental milestones are associated with later mental health outcomes. Phenotypic data were obtained for youth with disruptive variants in ADNP, CHD8, or DYRK1A (N = 65, mean age = 8.7 years, 40% female) within a long-running, genetics-first study. Standardized caregiver-report measures of mental health features (anxiety, depression, attention-deficit/hyperactivity, oppositional behavior) and developmental history were extracted and analyzed for effects of gene group, age, and early developmental milestones on mental health features. Patterns of mental health features varied by group, with anxiety most prominent for CHD8, oppositional features overrepresented among ADNP, and attentional and depressive features most prominent for DYRK1A. For the full sample, age was positively associated with anxiety features, such that elevations in anxiety relative to same-age and same-sex peers may worsen with increasing age. Predictive utility of early developmental milestones was limited, with evidence of early language delays predicting greater difficulties across behavioral domains only for the CHD8 group. Despite shared associations with autism and intellectual disability, disruptive variants in ADNP, CHD8, and DYRK1A may yield variable psychiatric phenotypes among children and adolescents. With replication in larger samples over time, efforts such as these may contribute to improved clinical care for affected children and adolescents, allow for earlier identification of emerging mental health difficulties, and promote early intervention to alleviate concerns and improve quality of life.
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ADNP、CHD8 和 DYRK1A 相关神经发育疾病的共同和不同心理健康特征
智力障碍(ID)和自闭症谱系障碍(ASD)等神经发育疾病可能源于一系列遗传和新发基因差异,并对生理和行为产生明显影响。目前,我们对与 ASD 相关的罕见遗传变异的精神表型知之甚少,尽管 ASD 更广泛地存在精神问题的风险增加。了解这些变异体的行为特征可以识别不同基因组的共同表型和特殊表型,促进机理模型的建立,并为临床实践提供预后见解。在本文中,我们评估了与 ID 和 ASD 相关的三个基因组(ADNP、CHD8 和 DYRK1A)的行为特征,目的有两个:(1)描述焦虑、抑郁、ADHD 和挑战行为等行为领域的表型特征;(2)了解年龄和早期发育里程碑是否与日后的心理健康结果相关。在一项长期的遗传学先行研究中,我们获得了患有 ADNP、CHD8 或 DYRK1A 破坏性变异的青少年的表型数据(N = 65,平均年龄 = 8.7 岁,40% 为女性)。研究人员提取了护理人员报告的心理健康特征(焦虑、抑郁、注意力缺陷/多动、对抗行为)和发育史的标准化测量数据,并分析了基因组、年龄和早期发育里程碑对心理健康特征的影响。心理健康特征的模式因基因组而异,焦虑在 CHD8 中最为突出,对抗行为特征在 ADNP 中比例较高,而注意力和抑郁特征在 DYRK1A 中最为突出。在全部样本中,年龄与焦虑特征呈正相关,因此,与同龄和同性同伴相比,焦虑的增加可能会随着年龄的增加而加剧。早期发育里程碑的预测作用有限,只有 CHD8 组的早期语言发育迟缓能预测出行为领域的更大困难。尽管ADNP、CHD8和DYRK1A中的破坏性变异与自闭症和智障有共同的关联,但它们可能会在儿童和青少年中产生不同的精神表型。随着时间的推移,在更大的样本中进行复制,这样的努力可能有助于改善受影响儿童和青少年的临床治疗,允许更早地识别新出现的心理健康问题,并促进早期干预,以减轻忧虑和提高生活质量。
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来源期刊
CiteScore
7.60
自引率
4.10%
发文量
58
审稿时长
>12 weeks
期刊介绍: Journal of Neurodevelopmental Disorders is an open access journal that integrates current, cutting-edge research across a number of disciplines, including neurobiology, genetics, cognitive neuroscience, psychiatry and psychology. The journal’s primary focus is on the pathogenesis of neurodevelopmental disorders including autism, fragile X syndrome, tuberous sclerosis, Turner Syndrome, 22q Deletion Syndrome, Prader-Willi and Angelman Syndrome, Williams syndrome, lysosomal storage diseases, dyslexia, specific language impairment and fetal alcohol syndrome. With the discovery of specific genes underlying neurodevelopmental syndromes, the emergence of powerful tools for studying neural circuitry, and the development of new approaches for exploring molecular mechanisms, interdisciplinary research on the pathogenesis of neurodevelopmental disorders is now increasingly common. Journal of Neurodevelopmental Disorders provides a unique venue for researchers interested in comparing and contrasting mechanisms and characteristics related to the pathogenesis of the full range of neurodevelopmental disorders, sharpening our understanding of the etiology and relevant phenotypes of each condition.
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