Polygenic and developmental profiles of autism differ by age at diagnosis

Xinhe Zhang; Jakob Grove; Yuanjun Gu; Cornelia K. Buus; Lea K. Nielsen; Sharon A. S. Neufeld; Mahmoud Koko; Daniel S. Malawsky; Emma M. Wade; Ellen Verhoef; Anna Gui; Laura Hegemann; Carrie Allison; Alex Tsompanidis; Deep Adhya; Rosemary Holt; Omar Al-Rubaie; Ramin Ali Marandi Ghoddousi; Alexander E. P. Heazell; Jonathan Mill; Alice Franklin; Rosie Bamford; Matthew E. Hurles; Mahmoud Mousa; David H. Rowitch; Kathy K. Niakan; Graham J. Burton; Tereza Cindrova-Davies; Deepak P. Srivastava; Lucia Dutan-Polit; Adam Pavlinek; Laura Sichlinger; Roland Nagy; Madeline A. Lancaster; Jose Gonzalez-Martinez; Tal Biron-Shental; Lidia V. Gabis; Dorothea Floris; Richard Bethlehem; Michael V. Lombardo; Marcin Radecki; Meng-Chuan Lai; Yeshaya David Greenberg; Elizabeth Weir; Florina Uzefovsky; Yumnah T. Khan; Juan Pablo Del Rio; Jonas Bybjerg-Grauholm; David M. Hougaard; Et al.; Bart P. F. Rutten

doi:10.1038/s41586-025-09542-6

Polygenic and developmental profiles of autism differ by age at diagnosis

Xinhe Zhang^*, Jakob Grove, Yuanjun Gu, Cornelia K. Buus, Lea K. Nielsen, Sharon A. S. Neufeld, Mahmoud Koko, Daniel S. Malawsky, Emma M. Wade, Ellen Verhoef, Anna Gui, Laura Hegemann, Carrie Allison, Alex Tsompanidis, Deep Adhya, Rosemary Holt, Omar Al-Rubaie, Ramin Ali Marandi Ghoddousi, Alexander E. P. Heazell, Jonathan MillAlice Franklin, Rosie Bamford, Matthew E. Hurles, Mahmoud Mousa, David H. Rowitch, Kathy K. Niakan, Graham J. Burton, Tereza Cindrova-Davies, Deepak P. Srivastava, Lucia Dutan-Polit, Adam Pavlinek, Laura Sichlinger, Roland Nagy, Madeline A. Lancaster, Jose Gonzalez-Martinez, Tal Biron-Shental, Lidia V. Gabis, Dorothea Floris, Richard Bethlehem, Michael V. Lombardo, Marcin Radecki, Meng-Chuan Lai, Yeshaya David Greenberg, Elizabeth Weir, Florina Uzefovsky, Yumnah T. Khan, Juan Pablo Del Rio, Jonas Bybjerg-Grauholm, David M. Hougaard, Et al., Bart P. F. Rutten

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Although autism has historically been conceptualized as a condition that emerges in early childhood1,2, many autistic people are diagnosed later in life3, 4-5. It is unknown whether earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Using longitudinal data from four independent birth cohorts, we demonstrate that two different socioemotional and behavioural trajectories are associated with age at diagnosis. In independent cohorts of autistic individuals, common genetic variants account for approximately 11% of the variance in age at autism diagnosis, similar to the contribution of individual sociodemographic and clinical factors, which typically explain less than 15% of this variance. We further demonstrate that the polygenic architecture of autism can be broken down into two modestly genetically correlated (rg = 0.38, s.e. = 0.07) autism polygenic factors. One of these factors is associated with earlier autism diagnosis and lower social and communication abilities in early childhood, but is only moderately genetically correlated with attention deficit-hyperactivity disorder (ADHD) and mental-health conditions. Conversely, the second factor is associated with later autism diagnosis and increased socioemotional and behavioural difficulties in adolescence, and has moderate to high positive genetic correlations with ADHD and mental-health conditions. These findings indicate that earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Our findings have important implications for how we conceptualize autism and provide a model to explain some of the diversity found in autism.

Original language	English
Number of pages	28
Journal	Nature
DOIs	https://doi.org/10.1038/s41586-025-09542-6
Publication status	E-pub ahead of print - 1 Oct 2025

Keywords

GENOME-WIDE ASSOCIATION
DIFFICULTIES QUESTIONNAIRE
SPECTRUM DISORDER
GENOTYPE IMPUTATION
R PACKAGE
POPULATION
CHILDREN
MULTIVARIATE
CHILDHOOD
STRENGTHS

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Zhang, X., Grove, J., Gu, Y., Buus, C. K., Nielsen, L. K., Neufeld, S. A. S., Koko, M., Malawsky, D. S., Wade, E. M., Verhoef, E., Gui, A., Hegemann, L., Allison, C., Tsompanidis, A., Adhya, D., Holt, R., Al-Rubaie, O., Ghoddousi, R. A. M., Heazell, A. E. P., ... Rutten, B. P. F. (2025). Polygenic and developmental profiles of autism differ by age at diagnosis. Nature. Advance online publication. https://doi.org/10.1038/s41586-025-09542-6

@article{e0799215d11741bd99d8fe7365d82e45,

title = "Polygenic and developmental profiles of autism differ by age at diagnosis",

abstract = "Although autism has historically been conceptualized as a condition that emerges in early childhood1,2, many autistic people are diagnosed later in life3, 4-5. It is unknown whether earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Using longitudinal data from four independent birth cohorts, we demonstrate that two different socioemotional and behavioural trajectories are associated with age at diagnosis. In independent cohorts of autistic individuals, common genetic variants account for approximately 11\% of the variance in age at autism diagnosis, similar to the contribution of individual sociodemographic and clinical factors, which typically explain less than 15\% of this variance. We further demonstrate that the polygenic architecture of autism can be broken down into two modestly genetically correlated (rg = 0.38, s.e. = 0.07) autism polygenic factors. One of these factors is associated with earlier autism diagnosis and lower social and communication abilities in early childhood, but is only moderately genetically correlated with attention deficit-hyperactivity disorder (ADHD) and mental-health conditions. Conversely, the second factor is associated with later autism diagnosis and increased socioemotional and behavioural difficulties in adolescence, and has moderate to high positive genetic correlations with ADHD and mental-health conditions. These findings indicate that earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Our findings have important implications for how we conceptualize autism and provide a model to explain some of the diversity found in autism.",

keywords = "GENOME-WIDE ASSOCIATION, DIFFICULTIES QUESTIONNAIRE, SPECTRUM DISORDER, GENOTYPE IMPUTATION, R PACKAGE, POPULATION, CHILDREN, MULTIVARIATE, CHILDHOOD, STRENGTHS",

author = "Xinhe Zhang and Jakob Grove and Yuanjun Gu and Buus, \{Cornelia K.\} and Nielsen, \{Lea K.\} and Neufeld, \{Sharon A. S.\} and Mahmoud Koko and Malawsky, \{Daniel S.\} and Wade, \{Emma M.\} and Ellen Verhoef and Anna Gui and Laura Hegemann and Carrie Allison and Alex Tsompanidis and Deep Adhya and Rosemary Holt and Omar Al-Rubaie and Ghoddousi, \{Ramin Ali Marandi\} and Heazell, \{Alexander E. P.\} and Jonathan Mill and Alice Franklin and Rosie Bamford and Hurles, \{Matthew E.\} and Mahmoud Mousa and Rowitch, \{David H.\} and Niakan, \{Kathy K.\} and Burton, \{Graham J.\} and Tereza Cindrova-Davies and Srivastava, \{Deepak P.\} and Lucia Dutan-Polit and Adam Pavlinek and Laura Sichlinger and Roland Nagy and Lancaster, \{Madeline A.\} and Jose Gonzalez-Martinez and Tal Biron-Shental and Gabis, \{Lidia V.\} and Dorothea Floris and Richard Bethlehem and Lombardo, \{Michael V.\} and Marcin Radecki and Meng-Chuan Lai and Greenberg, \{Yeshaya David\} and Elizabeth Weir and Florina Uzefovsky and Khan, \{Yumnah T.\} and \{Del Rio\}, \{Juan Pablo\} and Jonas Bybjerg-Grauholm and Hougaard, \{David M.\} and \{Et al.\} and Rutten, \{Bart P. F.\}",

year = "2025",

month = oct,

day = "1",

doi = "10.1038/s41586-025-09542-6",

language = "English",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Research",

}

Zhang, X, Grove, J, Gu, Y, Buus, CK, Nielsen, LK, Neufeld, SAS, Koko, M, Malawsky, DS, Wade, EM, Verhoef, E, Gui, A, Hegemann, L, Allison, C, Tsompanidis, A, Adhya, D, Holt, R, Al-Rubaie, O, Ghoddousi, RAM, Heazell, AEP, Mill, J, Franklin, A, Bamford, R, Hurles, ME, Mousa, M, Rowitch, DH, Niakan, KK, Burton, GJ, Cindrova-Davies, T, Srivastava, DP, Dutan-Polit, L, Pavlinek, A, Sichlinger, L, Nagy, R, Lancaster, MA, Gonzalez-Martinez, J, Biron-Shental, T, Gabis, LV, Floris, D, Bethlehem, R, Lombardo, MV, Radecki, M, Lai, M-C, Greenberg, YD, Weir, E, Uzefovsky, F, Khan, YT, Del Rio, JP, Bybjerg-Grauholm, J, Hougaard, DM, Et al. & Rutten, BPF 2025, 'Polygenic and developmental profiles of autism differ by age at diagnosis', Nature. https://doi.org/10.1038/s41586-025-09542-6

TY - JOUR

T1 - Polygenic and developmental profiles of autism differ by age at diagnosis

AU - Zhang, Xinhe

AU - Grove, Jakob

AU - Gu, Yuanjun

AU - Buus, Cornelia K.

AU - Nielsen, Lea K.

AU - Neufeld, Sharon A. S.

AU - Koko, Mahmoud

AU - Malawsky, Daniel S.

AU - Wade, Emma M.

AU - Verhoef, Ellen

AU - Gui, Anna

AU - Hegemann, Laura

AU - Allison, Carrie

AU - Tsompanidis, Alex

AU - Adhya, Deep

AU - Holt, Rosemary

AU - Al-Rubaie, Omar

AU - Ghoddousi, Ramin Ali Marandi

AU - Heazell, Alexander E. P.

AU - Mill, Jonathan

AU - Franklin, Alice

AU - Bamford, Rosie

AU - Hurles, Matthew E.

AU - Mousa, Mahmoud

AU - Rowitch, David H.

AU - Niakan, Kathy K.

AU - Burton, Graham J.

AU - Cindrova-Davies, Tereza

AU - Srivastava, Deepak P.

AU - Dutan-Polit, Lucia

AU - Pavlinek, Adam

AU - Sichlinger, Laura

AU - Nagy, Roland

AU - Lancaster, Madeline A.

AU - Gonzalez-Martinez, Jose

AU - Biron-Shental, Tal

AU - Gabis, Lidia V.

AU - Floris, Dorothea

AU - Bethlehem, Richard

AU - Lombardo, Michael V.

AU - Radecki, Marcin

AU - Lai, Meng-Chuan

AU - Greenberg, Yeshaya David

AU - Weir, Elizabeth

AU - Uzefovsky, Florina

AU - Khan, Yumnah T.

AU - Del Rio, Juan Pablo

AU - Bybjerg-Grauholm, Jonas

AU - Hougaard, David M.

AU - Et al.

AU - Rutten, Bart P. F.

PY - 2025/10/1

Y1 - 2025/10/1

N2 - Although autism has historically been conceptualized as a condition that emerges in early childhood1,2, many autistic people are diagnosed later in life3, 4-5. It is unknown whether earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Using longitudinal data from four independent birth cohorts, we demonstrate that two different socioemotional and behavioural trajectories are associated with age at diagnosis. In independent cohorts of autistic individuals, common genetic variants account for approximately 11% of the variance in age at autism diagnosis, similar to the contribution of individual sociodemographic and clinical factors, which typically explain less than 15% of this variance. We further demonstrate that the polygenic architecture of autism can be broken down into two modestly genetically correlated (rg = 0.38, s.e. = 0.07) autism polygenic factors. One of these factors is associated with earlier autism diagnosis and lower social and communication abilities in early childhood, but is only moderately genetically correlated with attention deficit-hyperactivity disorder (ADHD) and mental-health conditions. Conversely, the second factor is associated with later autism diagnosis and increased socioemotional and behavioural difficulties in adolescence, and has moderate to high positive genetic correlations with ADHD and mental-health conditions. These findings indicate that earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Our findings have important implications for how we conceptualize autism and provide a model to explain some of the diversity found in autism.

AB - Although autism has historically been conceptualized as a condition that emerges in early childhood1,2, many autistic people are diagnosed later in life3, 4-5. It is unknown whether earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Using longitudinal data from four independent birth cohorts, we demonstrate that two different socioemotional and behavioural trajectories are associated with age at diagnosis. In independent cohorts of autistic individuals, common genetic variants account for approximately 11% of the variance in age at autism diagnosis, similar to the contribution of individual sociodemographic and clinical factors, which typically explain less than 15% of this variance. We further demonstrate that the polygenic architecture of autism can be broken down into two modestly genetically correlated (rg = 0.38, s.e. = 0.07) autism polygenic factors. One of these factors is associated with earlier autism diagnosis and lower social and communication abilities in early childhood, but is only moderately genetically correlated with attention deficit-hyperactivity disorder (ADHD) and mental-health conditions. Conversely, the second factor is associated with later autism diagnosis and increased socioemotional and behavioural difficulties in adolescence, and has moderate to high positive genetic correlations with ADHD and mental-health conditions. These findings indicate that earlier- and later-diagnosed autism have different developmental trajectories and genetic profiles. Our findings have important implications for how we conceptualize autism and provide a model to explain some of the diversity found in autism.

KW - GENOME-WIDE ASSOCIATION

KW - DIFFICULTIES QUESTIONNAIRE

KW - SPECTRUM DISORDER

KW - GENOTYPE IMPUTATION

KW - R PACKAGE

KW - POPULATION

KW - CHILDREN

KW - MULTIVARIATE

KW - CHILDHOOD

KW - STRENGTHS

U2 - 10.1038/s41586-025-09542-6

DO - 10.1038/s41586-025-09542-6

M3 - Article

SN - 0028-0836

JO - Nature

JF - Nature

ER -

Polygenic and developmental profiles of autism differ by age at diagnosis

Abstract

Keywords

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