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Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder

IMPORTANCE: What is inherited or acquired in neurodevelopmental conditions such as autism spectrum disorder (ASD) is not a fixed outcome, but instead is a vulnerability to a spectrum of traits, especially social difficulties. Identifying the biological mechanisms associated with vulnerability requir...

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Autores principales: Ciarrusta, Judit, O'Muircheartaigh, Jonathan, Dimitrova, Ralica, Batalle, Dafnis, Cordero-Grande, Lucilio, Price, Anthony, Hughes, Emer, Steinweg, Johannes Klaus, Kangas, Johanna, Perry, Emily, Javed, Ayesha, Stoencheva, Vladimira, Akolekar, Ranjit, Victor, Suresh, Hajnal, Joseph, Murphy, Declan, Edwards, David, Arichi, Tomoki, McAlonan, Grainne
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Medical Association 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6450332/
https://www.ncbi.nlm.nih.gov/pubmed/30951164
http://dx.doi.org/10.1001/jamanetworkopen.2019.1868
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author Ciarrusta, Judit
O'Muircheartaigh, Jonathan
Dimitrova, Ralica
Batalle, Dafnis
Cordero-Grande, Lucilio
Price, Anthony
Hughes, Emer
Steinweg, Johannes Klaus
Kangas, Johanna
Perry, Emily
Javed, Ayesha
Stoencheva, Vladimira
Akolekar, Ranjit
Victor, Suresh
Hajnal, Joseph
Murphy, Declan
Edwards, David
Arichi, Tomoki
McAlonan, Grainne
author_facet Ciarrusta, Judit
O'Muircheartaigh, Jonathan
Dimitrova, Ralica
Batalle, Dafnis
Cordero-Grande, Lucilio
Price, Anthony
Hughes, Emer
Steinweg, Johannes Klaus
Kangas, Johanna
Perry, Emily
Javed, Ayesha
Stoencheva, Vladimira
Akolekar, Ranjit
Victor, Suresh
Hajnal, Joseph
Murphy, Declan
Edwards, David
Arichi, Tomoki
McAlonan, Grainne
author_sort Ciarrusta, Judit
collection PubMed
description IMPORTANCE: What is inherited or acquired in neurodevelopmental conditions such as autism spectrum disorder (ASD) is not a fixed outcome, but instead is a vulnerability to a spectrum of traits, especially social difficulties. Identifying the biological mechanisms associated with vulnerability requires looking as early in life as possible, before the brain is shaped by postnatal mechanisms and/or the experiences of living with these traits. Animal studies suggest that susceptibility to neurodevelopmental disorders arises when genetic and/or environmental risks for these conditions alter patterns of synchronous brain activity in the perinatal period, but this has never been examined in human neonates. OBJECTIVE: To assess whether alternation of functional maturation of social brain circuits is associated with a family history of ASD in newborns. DESIGN, SETTING, AND PARTICIPANTS: In this cohort study of 36 neonates with and without a family history of ASD, neonates underwent magnetic resonance imaging at St Thomas Hospital in London, England, using a dedicated neonatal brain imaging system between June 23, 2015, and August 1, 2018. Neonates with a first-degree relative with ASD (R+) and therefore vulnerable to autistic traits and neonates without a family history (R−) were recruited for the study. Synchronous neural activity in brain regions linked to social function was compared. MAIN OUTCOMES AND MEASURES: Regions responsible for social function were selected with reference to a published meta-analysis and the level of synchronous activity within each region was used as a measure of local functional connectivity in a regional homogeneity analysis. Group differences, controlling for sex, age at birth, age at scan, and group × age interactions, were examined. RESULTS: The final data set consisted of 18 R+ infants (13 male; median [range] postmenstrual age at scan, 42.93 [40.00-44.86] weeks) and 18 R− infants (13 male; median [range] postmenstrual age at scan, 42.50 [39.29-44.58] weeks). Neonates who were R+ had significantly higher levels of synchronous activity in the right posterior fusiform (t = 2.48; P = .04) and left parietal cortices (t = 3.96; P = .04). In addition, there was a significant group × age interaction within the anterior segment of the left insula (t = 3.03; P = .04) and cingulate cortices (right anterior: t = 3.00; P = .03; left anterior: t = 2.81; P = .03; right posterior: t = 2.77; P = .03; left posterior: t = 2.55; P = .03). In R+ infants, levels of synchronous activity decreased over 39 to 45 weeks’ postmenstrual age, whereas synchronous activity levels increased in R− infants over the same period. CONCLUSIONS AND RELEVANCE: Synchronous activity is required during maturation of functionally connected networks. This study found that in newborn humans, having a first-degree relative with ASD was associated with higher levels of local functional connectivity and dysmaturation of interconnected regions responsible for processing higher-order social information.
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spelling pubmed-64503322019-04-24 Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder Ciarrusta, Judit O'Muircheartaigh, Jonathan Dimitrova, Ralica Batalle, Dafnis Cordero-Grande, Lucilio Price, Anthony Hughes, Emer Steinweg, Johannes Klaus Kangas, Johanna Perry, Emily Javed, Ayesha Stoencheva, Vladimira Akolekar, Ranjit Victor, Suresh Hajnal, Joseph Murphy, Declan Edwards, David Arichi, Tomoki McAlonan, Grainne JAMA Netw Open Original Investigation IMPORTANCE: What is inherited or acquired in neurodevelopmental conditions such as autism spectrum disorder (ASD) is not a fixed outcome, but instead is a vulnerability to a spectrum of traits, especially social difficulties. Identifying the biological mechanisms associated with vulnerability requires looking as early in life as possible, before the brain is shaped by postnatal mechanisms and/or the experiences of living with these traits. Animal studies suggest that susceptibility to neurodevelopmental disorders arises when genetic and/or environmental risks for these conditions alter patterns of synchronous brain activity in the perinatal period, but this has never been examined in human neonates. OBJECTIVE: To assess whether alternation of functional maturation of social brain circuits is associated with a family history of ASD in newborns. DESIGN, SETTING, AND PARTICIPANTS: In this cohort study of 36 neonates with and without a family history of ASD, neonates underwent magnetic resonance imaging at St Thomas Hospital in London, England, using a dedicated neonatal brain imaging system between June 23, 2015, and August 1, 2018. Neonates with a first-degree relative with ASD (R+) and therefore vulnerable to autistic traits and neonates without a family history (R−) were recruited for the study. Synchronous neural activity in brain regions linked to social function was compared. MAIN OUTCOMES AND MEASURES: Regions responsible for social function were selected with reference to a published meta-analysis and the level of synchronous activity within each region was used as a measure of local functional connectivity in a regional homogeneity analysis. Group differences, controlling for sex, age at birth, age at scan, and group × age interactions, were examined. RESULTS: The final data set consisted of 18 R+ infants (13 male; median [range] postmenstrual age at scan, 42.93 [40.00-44.86] weeks) and 18 R− infants (13 male; median [range] postmenstrual age at scan, 42.50 [39.29-44.58] weeks). Neonates who were R+ had significantly higher levels of synchronous activity in the right posterior fusiform (t = 2.48; P = .04) and left parietal cortices (t = 3.96; P = .04). In addition, there was a significant group × age interaction within the anterior segment of the left insula (t = 3.03; P = .04) and cingulate cortices (right anterior: t = 3.00; P = .03; left anterior: t = 2.81; P = .03; right posterior: t = 2.77; P = .03; left posterior: t = 2.55; P = .03). In R+ infants, levels of synchronous activity decreased over 39 to 45 weeks’ postmenstrual age, whereas synchronous activity levels increased in R− infants over the same period. CONCLUSIONS AND RELEVANCE: Synchronous activity is required during maturation of functionally connected networks. This study found that in newborn humans, having a first-degree relative with ASD was associated with higher levels of local functional connectivity and dysmaturation of interconnected regions responsible for processing higher-order social information. American Medical Association 2019-04-05 /pmc/articles/PMC6450332/ /pubmed/30951164 http://dx.doi.org/10.1001/jamanetworkopen.2019.1868 Text en Copyright 2019 Ciarrusta J et al. JAMA Network Open. http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the CC-BY License.
spellingShingle Original Investigation
Ciarrusta, Judit
O'Muircheartaigh, Jonathan
Dimitrova, Ralica
Batalle, Dafnis
Cordero-Grande, Lucilio
Price, Anthony
Hughes, Emer
Steinweg, Johannes Klaus
Kangas, Johanna
Perry, Emily
Javed, Ayesha
Stoencheva, Vladimira
Akolekar, Ranjit
Victor, Suresh
Hajnal, Joseph
Murphy, Declan
Edwards, David
Arichi, Tomoki
McAlonan, Grainne
Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title_full Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title_fullStr Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title_full_unstemmed Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title_short Social Brain Functional Maturation in Newborn Infants With and Without a Family History of Autism Spectrum Disorder
title_sort social brain functional maturation in newborn infants with and without a family history of autism spectrum disorder
topic Original Investigation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6450332/
https://www.ncbi.nlm.nih.gov/pubmed/30951164
http://dx.doi.org/10.1001/jamanetworkopen.2019.1868
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