Genetic neurodevelopmental clustering and dyslexia
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Published:2024-07-15
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ISSN:1359-4184
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Container-title:Molecular Psychiatry
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language:en
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Short-container-title:Mol Psychiatry
Author:
Ciulkinyte AustejaORCID, Mountford Hayley S.ORCID, Fontanillas PierreORCID, , Aslibekyan Stella, Auton Adam, Babalola Elizabeth, Bell Robert K., Bielenberg Jessica, Bowes Jonathan, Bryc Katarzyna, Chaudhary Ninad S., Coker Daniella, Das Sayantan, DelloRusso Emily, Elson Sarah L., Eriksson Nicholas, Filshtein Teresa, Freyman Will, Fuller Zach, German Chris, Granka Julie M., Heilbron Karl, Hernandez Alejandro, Hicks Barry, Hinds David A., Jewett Ethan M., Jiang Yunxuan, Kukar Katelyn, Kwong Alan, Liang Yanyu, Lin Keng-Han, Llamas Bianca A., McIntyre Matthew H., Micheletti Steven J., Moreno Meghan E., Nandakumar Priyanka, Nguyen Dominique T., O’Connell Jared, Petrakovitz Aaron A., Poznik G. David, Reynoso Alexandra, Saini Shubham, Schumacher Morgan, Selcer Leah, Shastri Anjali J., Shelton Janie F., Shi Jingchunzi, Shringarpure Suyash, Su Qiaojuan Jane, Tat Susana A., Tran Vinh, Tung Joyce Y., Wang Xin, Wang Wei, Weldon Catherine H., Wilton Peter, Wong Corinna D., Bates Timothy C.ORCID, Martin Nicholas G.ORCID, Fisher Simon E.ORCID, Luciano MichelleORCID
Abstract
AbstractDyslexia is a learning difficulty with neurodevelopmental origins, manifesting as reduced accuracy and speed in reading and spelling. It is substantially heritable and frequently co-occurs with other neurodevelopmental conditions, particularly attention deficit-hyperactivity disorder (ADHD). Here, we investigate the genetic structure underlying dyslexia and a range of psychiatric traits using results from genome-wide association studies of dyslexia, ADHD, autism, anorexia nervosa, anxiety, bipolar disorder, major depressive disorder, obsessive compulsive disorder, schizophrenia, and Tourette syndrome. Genomic Structural Equation Modelling (GenomicSEM) showed heightened support for a model consisting of five correlated latent genomic factors described as: F1) compulsive disorders (including obsessive-compulsive disorder, anorexia nervosa, Tourette syndrome), F2) psychotic disorders (including bipolar disorder, schizophrenia), F3) internalising disorders (including anxiety disorder, major depressive disorder), F4) neurodevelopmental traits (including autism, ADHD), and F5) attention and learning difficulties (including ADHD, dyslexia). ADHD loaded more strongly on the attention and learning difficulties latent factor (F5) than on the neurodevelopmental traits latent factor (F4). The attention and learning difficulties latent factor (F5) was positively correlated with internalising disorders (.40), neurodevelopmental traits (.25) and psychotic disorders (.17) latent factors, and negatively correlated with the compulsive disorders (–.16) latent factor. These factor correlations are mirrored in genetic correlations observed between the attention and learning difficulties latent factor and other cognitive, psychological and wellbeing traits. We further investigated genetic variants underlying both dyslexia and ADHD, which implicated 49 loci (40 not previously found in GWAS of the individual traits) mapping to 174 genes (121 not found in GWAS of individual traits) as potential pleiotropic variants. Our study confirms the increased genetic relation between dyslexia and ADHD versus other psychiatric traits and uncovers novel pleiotropic variants affecting both traits. In future, analyses including additional co-occurring traits such as dyscalculia and dyspraxia will allow a clearer definition of the attention and learning difficulties latent factor, yielding further insights into factor structure and pleiotropic effects.
Funder
Wellcome Trust RCUK | Biotechnology and Biological Sciences Research Council Max-Planck-Gesellschaft
Publisher
Springer Science and Business Media LLC
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