Daniel S. Malawsky, Mahmoud Koko, Petr Danacek, Wei Huang, Olivia Wootton, Qinqin Huang, Emma E. Wade, Sarah J. Lindsay, Rosalind Arden, Matthew E. Hurles, Hilary C. Martin
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引用次数: 0
摘要
影响成人认知能力的常见和罕见基因变异也会导致儿童出现认知障碍的罕见神经发育疾病的风险。然而,人们对它们对生命早期认知能力的影响仍然知之甚少。在此,我们主要利用雅芳父母与子女纵向研究(Avon Longitudinal Study of Parents and Children,n=6,495 名无血缘关系的儿童)来研究常见的全基因组变异和罕见的外显子变异对儿童和青少年认知能力的影响。我们的研究表明,随着儿童年龄的增长,与教育程度和认知能力相关的常见变异的影响也在增加。相反,有害稀有变异体的负面影响会随着年龄的增长而减弱。通过三元分析,我们发现这些与年龄相关的趋势是由携带这些变异体的个体所受到的直接遗传效应驱动的。我们进一步发现,在表型分布的高端个体中,常见变异体的增加效应更强,而在低端个体中,罕见变异体的减弱效应更强。在千年队列研究(5,920 名儿童)和英国生物库(101,232 名成人)中观察到了一致的结果。常见和罕见基因变异对儿童认知能力的影响在程度上与父母教育程度、母亲疾病和早产等其他因素的影响大致相当。孕产妇疾病和早产对儿童认知能力的影响也会随着年龄的增长而减弱,而父母受教育程度的影响则不会。此外,我们还发现,这些不同因素的相对作用也不尽相同,这取决于我们考虑的是它们对整个人群表型变异的作用,还是对不良后果风险的作用。我们的发现可能有助于解释与神经发育状况相关的罕见损伤性变异的明显不完全渗透性。更广泛地说,这些发现还表明了研究整个生命过程中的动态遗传影响及其对表型分布的不同影响的重要性。
The differential effects of common and rare genetic variants on cognitive performance across development
Common and rare genetic variants that impact adult cognitive performance also contribute to risk of rare neurodevelopmental conditions involving cognitive deficits in children. However, their influence on cognitive performance across early life remains poorly understood. Here, we investigate the contribution of common genome-wide and rare exonic variation to cognitive performance across childhood and adolescence primarily using the Avon Longitudinal Study of Parents and Children (n=6,495 unrelated children). We show that the effect of common variants associated with educational attainment and cognitive performance increases as children age. Conversely, the negative effect of deleterious rare variants attenuates with age. Using trio analyses, we show that these age-related trends are driven by direct genetic effects on the individual who carries these variants. We further find that the increasing effects of common variants are stronger in individuals at the upper end of the phenotype distribution, whereas the attenuating effects of rare variants are stronger in those at the lower end. Concordant results were observed in the Millenium Cohort Study (5,920 children) and UK Biobank (101,232 adults). The effects of common and rare genetic variation on childhood cognitive performance are broadly comparable in magnitude to those of other factors such as parental educational attainment, maternal illness and preterm birth. The effects of maternal illness and preterm birth on childhood cognitive performance also attenuate with age, whereas the effect of parental educational attainment does not. Furthermore, we show that the relative contribution of these various factors differ depending on whether one considers their contribution to phenotypic variance across the entire population or to the risk of poor outcomes. Our findings may help explain the apparent incomplete penetrance of rare damaging variants associated with neurodevelopmental conditions. More generally, they also show the importance of studying dynamic genetic influences across the life course and their differential effects across the phenotype distribution.
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