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Association between abnormal fetal head growth and autism spectrum disorder

INTRODUCTION: Despite evidence for the prenatal onset of abnormal head growth in ASD children, studies on fetal ultrasound data in ASD are limited and controversial. OBJECTIVES: To understand whether people with ASD have abnormal head growth during gestation METHODS: A longitudinal matched case-sibl...

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Autores principales: Regev, O., Cohen, G., Hadar, A., Meiri, G., Flusser, H., Michaelovski, A., Dinstein, I., Hershkovitz, R., Menashe, I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cambridge University Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9470422/
http://dx.doi.org/10.1192/j.eurpsy.2021.364
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author Regev, O.
Cohen, G.
Hadar, A.
Meiri, G.
Flusser, H.
Michaelovski, A.
Dinstein, I.
Hershkovitz, R.
Menashe, I.
author_facet Regev, O.
Cohen, G.
Hadar, A.
Meiri, G.
Flusser, H.
Michaelovski, A.
Dinstein, I.
Hershkovitz, R.
Menashe, I.
author_sort Regev, O.
collection PubMed
description INTRODUCTION: Despite evidence for the prenatal onset of abnormal head growth in ASD children, studies on fetal ultrasound data in ASD are limited and controversial. OBJECTIVES: To understand whether people with ASD have abnormal head growth during gestation METHODS: A longitudinal matched case-sibling-control study on prenatal ultrasound biometric measures of ASD children was conducted. Children with ASD were matched to two control groups: (1) typically developed sibling (TDS) and (2) typically developed population (TDP). The cohort comprised 528 children (72.7% males): 174 ASD, 178 TDS, and 176 TDP. RESULTS: Second-trimester ASD and TDS fetuses had significantly smaller biparietal diameter (BPD) than TDP fetuses (aOR(zBPD)=0.685, 95%CI=0.527-0.890 and aOR(zBPD)=0.587, 95%CI=0.459-0.751, respectively). However, these differences became statistically indistinguishable in the third trimester. Head biometric measures were associated with the sex of the fetus, with males having larger heads than females within and across groups. A linear mixed-effect model assessing the effects of sex and group assignment on fetal longitudinal head growth indicated faster BPD growth in TDS vs both ASD and TDP in males (β=0.084 and β=0.100 respectively; p<0.001) but not in females, suggesting an ASD–sex interaction in head growth during gestation. Fetal head shape showed sex-specific characteristics, and head growth was inversely correlated with ASD severity in males and females, thus further supporting the sex effect on the association between fetal head growth and ASD. CONCLUSIONS: Our findings suggest that abnormal fetal head growth is a familial trait of ASD, which is modulated by sex and is associated with the severity of the disorder. DISCLOSURE: No significant relationships.
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spelling pubmed-94704222022-09-29 Association between abnormal fetal head growth and autism spectrum disorder Regev, O. Cohen, G. Hadar, A. Meiri, G. Flusser, H. Michaelovski, A. Dinstein, I. Hershkovitz, R. Menashe, I. Eur Psychiatry Abstract INTRODUCTION: Despite evidence for the prenatal onset of abnormal head growth in ASD children, studies on fetal ultrasound data in ASD are limited and controversial. OBJECTIVES: To understand whether people with ASD have abnormal head growth during gestation METHODS: A longitudinal matched case-sibling-control study on prenatal ultrasound biometric measures of ASD children was conducted. Children with ASD were matched to two control groups: (1) typically developed sibling (TDS) and (2) typically developed population (TDP). The cohort comprised 528 children (72.7% males): 174 ASD, 178 TDS, and 176 TDP. RESULTS: Second-trimester ASD and TDS fetuses had significantly smaller biparietal diameter (BPD) than TDP fetuses (aOR(zBPD)=0.685, 95%CI=0.527-0.890 and aOR(zBPD)=0.587, 95%CI=0.459-0.751, respectively). However, these differences became statistically indistinguishable in the third trimester. Head biometric measures were associated with the sex of the fetus, with males having larger heads than females within and across groups. A linear mixed-effect model assessing the effects of sex and group assignment on fetal longitudinal head growth indicated faster BPD growth in TDS vs both ASD and TDP in males (β=0.084 and β=0.100 respectively; p<0.001) but not in females, suggesting an ASD–sex interaction in head growth during gestation. Fetal head shape showed sex-specific characteristics, and head growth was inversely correlated with ASD severity in males and females, thus further supporting the sex effect on the association between fetal head growth and ASD. CONCLUSIONS: Our findings suggest that abnormal fetal head growth is a familial trait of ASD, which is modulated by sex and is associated with the severity of the disorder. DISCLOSURE: No significant relationships. Cambridge University Press 2021-08-13 /pmc/articles/PMC9470422/ http://dx.doi.org/10.1192/j.eurpsy.2021.364 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Abstract
Regev, O.
Cohen, G.
Hadar, A.
Meiri, G.
Flusser, H.
Michaelovski, A.
Dinstein, I.
Hershkovitz, R.
Menashe, I.
Association between abnormal fetal head growth and autism spectrum disorder
title Association between abnormal fetal head growth and autism spectrum disorder
title_full Association between abnormal fetal head growth and autism spectrum disorder
title_fullStr Association between abnormal fetal head growth and autism spectrum disorder
title_full_unstemmed Association between abnormal fetal head growth and autism spectrum disorder
title_short Association between abnormal fetal head growth and autism spectrum disorder
title_sort association between abnormal fetal head growth and autism spectrum disorder
topic Abstract
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9470422/
http://dx.doi.org/10.1192/j.eurpsy.2021.364
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