Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population

Yuanjun Gu; Eva Maria-Stauffer; Saashi A. Bedford; Rafael Romero-Garcia; Jakob Grove; Anders Borglum; Hilary Martin; Simon Baron-Cohen; Richard A. I. Bethlehem; Varun Warrier; Thomas Werge; Merete Nordentoft; APEX consortium; iPSYCH-autism consortium

doi:10.1038/s41380-025-02927-z

Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population

Yuanjun Gu^*, Eva Maria-Stauffer, Saashi A. Bedford, Rafael Romero-Garcia, Jakob Grove, Anders Borglum, Hilary Martin, Simon Baron-Cohen, Richard A. I. Bethlehem, Varun Warrier^*, Thomas Werge (Member of author collaboration), Merete Nordentoft (Member of author collaboration), APEX consortium, iPSYCH-autism consortium

^*Corresponding author for this work

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Abstract

Genetic variants linked to autism are thought to change cognition and behaviour by altering the structure and function of the brain. Although a substantial body of literature has identified structural brain differences in autism, it is unknown whether autism-associated common genetic variants are linked to changes in cortical macro- and micro-structure. We investigated this using neuroimaging and genetic data from adults (UK Biobank, N = 31,748) and children (ABCD, N = 4928). Using polygenic scores and genetic correlations we observe a robust negative association between common variants for autism and a magnetic resonance imaging derived phenotype for neurite density (intracellular volume fraction) in the general population. This result is consistent across both children and adults, in both the cortex and in white matter tracts, and confirmed using polygenic scores and genetic correlations. There were no sex differences in this association. Mendelian randomisation analyses provide no evidence for a causal relationship between autism and intracellular volume fraction, although this should be revisited using better powered instruments. Overall, this study provides evidence for shared common variant genetics between autism and cortical neurite density.

Original language	English
Journal	Molecular Psychiatry
Volume	30
Issue number	8
Pages (from-to)	3393-3403
Number of pages	11
ISSN	1359-4184
DOIs	https://doi.org/10.1038/s41380-025-02927-z
Publication status	Published - 2025

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Publisher Copyright:
© The Author(s) 2025.

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Gu, Y., Maria-Stauffer, E., Bedford, S. A., Romero-Garcia, R., Grove, J., Borglum, A., Martin, H., Baron-Cohen, S., Bethlehem, R. A. I., Warrier, V., Werge, T., Nordentoft, M., APEX consortium, & iPSYCH-autism consortium (2025). Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population. Molecular Psychiatry, 30(8), 3393-3403. https://doi.org/10.1038/s41380-025-02927-z

Gu, Y, Maria-Stauffer, E, Bedford, SA, Romero-Garcia, R, Grove, J, Borglum, A, Martin, H, Baron-Cohen, S, Bethlehem, RAI, Warrier, V, Werge, T , Nordentoft, M, APEX consortium & iPSYCH-autism consortium 2025, 'Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population', Molecular Psychiatry, vol. 30, no. 8, pp. 3393-3403. https://doi.org/10.1038/s41380-025-02927-z

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title = "Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population",

abstract = "Genetic variants linked to autism are thought to change cognition and behaviour by altering the structure and function of the brain. Although a substantial body of literature has identified structural brain differences in autism, it is unknown whether autism-associated common genetic variants are linked to changes in cortical macro- and micro-structure. We investigated this using neuroimaging and genetic data from adults (UK Biobank, N = 31,748) and children (ABCD, N = 4928). Using polygenic scores and genetic correlations we observe a robust negative association between common variants for autism and a magnetic resonance imaging derived phenotype for neurite density (intracellular volume fraction) in the general population. This result is consistent across both children and adults, in both the cortex and in white matter tracts, and confirmed using polygenic scores and genetic correlations. There were no sex differences in this association. Mendelian randomisation analyses provide no evidence for a causal relationship between autism and intracellular volume fraction, although this should be revisited using better powered instruments. Overall, this study provides evidence for shared common variant genetics between autism and cortical neurite density.",

author = "Yuanjun Gu and Eva Maria-Stauffer and Bedford, {Saashi A.} and Rafael Romero-Garcia and Jakob Grove and Anders Borglum and Hilary Martin and Simon Baron-Cohen and Bethlehem, {Richard A. I.} and Varun Warrier and Thomas Werge and Merete Nordentoft and {APEX consortium} and {iPSYCH-autism consortium}",

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doi = "10.1038/s41380-025-02927-z",

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T1 - Polygenic scores for autism are associated with reduced neurite density in adults and children from the general population

AU - Gu, Yuanjun

AU - Maria-Stauffer, Eva

AU - Bedford, Saashi A.

AU - Romero-Garcia, Rafael

AU - Grove, Jakob

AU - Borglum, Anders

AU - Martin, Hilary

AU - Baron-Cohen, Simon

AU - Bethlehem, Richard A. I.

AU - Warrier, Varun

AU - APEX consortium

AU - iPSYCH-autism consortium

A2 - Werge, Thomas

A2 - Nordentoft, Merete

PY - 2025

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N2 - Genetic variants linked to autism are thought to change cognition and behaviour by altering the structure and function of the brain. Although a substantial body of literature has identified structural brain differences in autism, it is unknown whether autism-associated common genetic variants are linked to changes in cortical macro- and micro-structure. We investigated this using neuroimaging and genetic data from adults (UK Biobank, N = 31,748) and children (ABCD, N = 4928). Using polygenic scores and genetic correlations we observe a robust negative association between common variants for autism and a magnetic resonance imaging derived phenotype for neurite density (intracellular volume fraction) in the general population. This result is consistent across both children and adults, in both the cortex and in white matter tracts, and confirmed using polygenic scores and genetic correlations. There were no sex differences in this association. Mendelian randomisation analyses provide no evidence for a causal relationship between autism and intracellular volume fraction, although this should be revisited using better powered instruments. Overall, this study provides evidence for shared common variant genetics between autism and cortical neurite density.

AB - Genetic variants linked to autism are thought to change cognition and behaviour by altering the structure and function of the brain. Although a substantial body of literature has identified structural brain differences in autism, it is unknown whether autism-associated common genetic variants are linked to changes in cortical macro- and micro-structure. We investigated this using neuroimaging and genetic data from adults (UK Biobank, N = 31,748) and children (ABCD, N = 4928). Using polygenic scores and genetic correlations we observe a robust negative association between common variants for autism and a magnetic resonance imaging derived phenotype for neurite density (intracellular volume fraction) in the general population. This result is consistent across both children and adults, in both the cortex and in white matter tracts, and confirmed using polygenic scores and genetic correlations. There were no sex differences in this association. Mendelian randomisation analyses provide no evidence for a causal relationship between autism and intracellular volume fraction, although this should be revisited using better powered instruments. Overall, this study provides evidence for shared common variant genetics between autism and cortical neurite density.

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DO - 10.1038/s41380-025-02927-z

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SN - 1359-4184

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JO - Molecular Psychiatry

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