Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence

BACKGROUND: Social-communication abilities are heritable traits, and their impairments overlap with the autism continuum. To characterise the genetic architecture of social-communication difficulties developmentally and identify genetic links with the autistic dimension, we conducted a genome-wide s...

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Autores principales: St Pourcain, Beate, Skuse, David H, Mandy, William P, Wang, Kai, Hakonarson, Hakon, Timpson, Nicholas J, Evans, David M, Kemp, John P, Ring, Susan M, McArdle, Wendy L, Golding, Jean, Smith, George Davey
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3940728/
https://www.ncbi.nlm.nih.gov/pubmed/24564958
http://dx.doi.org/10.1186/2040-2392-5-18
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author St Pourcain, Beate
Skuse, David H
Mandy, William P
Wang, Kai
Hakonarson, Hakon
Timpson, Nicholas J
Evans, David M
Kemp, John P
Ring, Susan M
McArdle, Wendy L
Golding, Jean
Smith, George Davey
author_facet St Pourcain, Beate
Skuse, David H
Mandy, William P
Wang, Kai
Hakonarson, Hakon
Timpson, Nicholas J
Evans, David M
Kemp, John P
Ring, Susan M
McArdle, Wendy L
Golding, Jean
Smith, George Davey
author_sort St Pourcain, Beate
collection PubMed
description BACKGROUND: Social-communication abilities are heritable traits, and their impairments overlap with the autism continuum. To characterise the genetic architecture of social-communication difficulties developmentally and identify genetic links with the autistic dimension, we conducted a genome-wide screen of social-communication problems at multiple time-points during childhood and adolescence. METHODS: Social-communication difficulties were ascertained at ages 8, 11, 14 and 17 years in a UK population-based birth cohort (Avon Longitudinal Study of Parents and Children; N ≤ 5,628) using mother-reported Social Communication Disorder Checklist scores. Genome-wide Complex Trait Analysis (GCTA) was conducted for all phenotypes. The time-points with the highest GCTA heritability were subsequently analysed for single SNP association genome-wide. Type I error in the presence of measurement relatedness and the likelihood of observing SNP signals near known autism susceptibility loci (co-location) were assessed via large-scale, genome-wide permutations. Association signals (P ≤ 10(−5)) were also followed up in Autism Genetic Resource Exchange pedigrees (N = 793) and the Autism Case Control cohort (N(cases)/N(controls) = 1,204/6,491). RESULTS: GCTA heritability was strongest in childhood (h(2)((8 years)) = 0.24) and especially in later adolescence (h(2)((17 years)) = 0.45), with a marked drop during early to middle adolescence (h(2)((11 years)) = 0.16 and h(2)((14 years)) = 0.08). Genome-wide screens at ages 8 and 17 years identified for the latter time-point evidence for association at 3p22.2 near SCN11A (rs4453791, P = 9.3 × 10(−9); genome-wide empirical P = 0.011) and suggestive evidence at 20p12.3 at PLCB1 (rs3761168, P = 7.9 × 10(−8); genome-wide empirical P = 0.085). None of these signals contributed to risk for autism. However, the co-location of population-based signals and autism susceptibility loci harbouring rare mutations, such as PLCB1, is unlikely to be due to chance (genome-wide empirical P(co-location) = 0.007). CONCLUSIONS: Our findings suggest that measurable common genetic effects for social-communication difficulties vary developmentally and that these changes may affect detectable overlaps with the autism spectrum.
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spelling pubmed-39407282014-03-05 Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence St Pourcain, Beate Skuse, David H Mandy, William P Wang, Kai Hakonarson, Hakon Timpson, Nicholas J Evans, David M Kemp, John P Ring, Susan M McArdle, Wendy L Golding, Jean Smith, George Davey Mol Autism Research BACKGROUND: Social-communication abilities are heritable traits, and their impairments overlap with the autism continuum. To characterise the genetic architecture of social-communication difficulties developmentally and identify genetic links with the autistic dimension, we conducted a genome-wide screen of social-communication problems at multiple time-points during childhood and adolescence. METHODS: Social-communication difficulties were ascertained at ages 8, 11, 14 and 17 years in a UK population-based birth cohort (Avon Longitudinal Study of Parents and Children; N ≤ 5,628) using mother-reported Social Communication Disorder Checklist scores. Genome-wide Complex Trait Analysis (GCTA) was conducted for all phenotypes. The time-points with the highest GCTA heritability were subsequently analysed for single SNP association genome-wide. Type I error in the presence of measurement relatedness and the likelihood of observing SNP signals near known autism susceptibility loci (co-location) were assessed via large-scale, genome-wide permutations. Association signals (P ≤ 10(−5)) were also followed up in Autism Genetic Resource Exchange pedigrees (N = 793) and the Autism Case Control cohort (N(cases)/N(controls) = 1,204/6,491). RESULTS: GCTA heritability was strongest in childhood (h(2)((8 years)) = 0.24) and especially in later adolescence (h(2)((17 years)) = 0.45), with a marked drop during early to middle adolescence (h(2)((11 years)) = 0.16 and h(2)((14 years)) = 0.08). Genome-wide screens at ages 8 and 17 years identified for the latter time-point evidence for association at 3p22.2 near SCN11A (rs4453791, P = 9.3 × 10(−9); genome-wide empirical P = 0.011) and suggestive evidence at 20p12.3 at PLCB1 (rs3761168, P = 7.9 × 10(−8); genome-wide empirical P = 0.085). None of these signals contributed to risk for autism. However, the co-location of population-based signals and autism susceptibility loci harbouring rare mutations, such as PLCB1, is unlikely to be due to chance (genome-wide empirical P(co-location) = 0.007). CONCLUSIONS: Our findings suggest that measurable common genetic effects for social-communication difficulties vary developmentally and that these changes may affect detectable overlaps with the autism spectrum. BioMed Central 2014-02-24 /pmc/articles/PMC3940728/ /pubmed/24564958 http://dx.doi.org/10.1186/2040-2392-5-18 Text en Copyright © 2014 St Pourcain et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
St Pourcain, Beate
Skuse, David H
Mandy, William P
Wang, Kai
Hakonarson, Hakon
Timpson, Nicholas J
Evans, David M
Kemp, John P
Ring, Susan M
McArdle, Wendy L
Golding, Jean
Smith, George Davey
Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title_full Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title_fullStr Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title_full_unstemmed Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title_short Variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
title_sort variability in the common genetic architecture of social-communication spectrum phenotypes during childhood and adolescence
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3940728/
https://www.ncbi.nlm.nih.gov/pubmed/24564958
http://dx.doi.org/10.1186/2040-2392-5-18
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