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A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism

Most genome linkage scans for autism spectrum disorders (ASDs) have failed to be replicated. Recently, a new ASD phenotypic sub-classification method was developed which employed cluster analyses of severity scores from the Autism Diagnostic Interview-Revised (ADI-R). Here, we performed linkage anal...

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Autores principales: Talebizadeh, Zohreh, Arking, Dan E., Hu, Valerie W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3694043/
https://www.ncbi.nlm.nih.gov/pubmed/23840741
http://dx.doi.org/10.1371/journal.pone.0067569
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author Talebizadeh, Zohreh
Arking, Dan E.
Hu, Valerie W.
author_facet Talebizadeh, Zohreh
Arking, Dan E.
Hu, Valerie W.
author_sort Talebizadeh, Zohreh
collection PubMed
description Most genome linkage scans for autism spectrum disorders (ASDs) have failed to be replicated. Recently, a new ASD phenotypic sub-classification method was developed which employed cluster analyses of severity scores from the Autism Diagnostic Interview-Revised (ADI-R). Here, we performed linkage analysis for each of the four identified ADI-R stratified subgroups. Additional stratification was also applied to reduce intra-family heterogeneity and to investigate the impact of gender. For the purpose of replication, two independent sets of single nucleotide polymorphism markers for 392 families were used in our study. This deep subject stratification protocol resulted in 16 distinct group-specific datasets for linkage analysis. No locus reached significance for the combined non-stratified cohort. However, study-wide significant (P = 0.02) linkage scores were reached for chromosomes 22q11 (LOD = 4.43) and 13q21 (LOD = 4.37) for two subsets representing the most severely language impaired individuals with ASD. Notably, 13q21 has been previously linked to autism with language impairment, and 22q11 has been separately associated with either autism or language disorders. Linkage analysis on chromosome 5p15 for a combination of two stratified female-containing subgroups demonstrated suggestive linkage (LOD = 3.5), which replicates previous linkage result for female-containing pedigrees. A trend was also found for the association of previously reported 5p14-p15 SNPs in the same female-containing cohort. This study demonstrates a novel and effective method to address the heterogeneity in genetic studies of ASD. Moreover, the linkage results for the stratified subgroups provide evidence at the gene scan level for both inter- and intra-family heterogeneity as well as for gender-specific loci.
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spelling pubmed-36940432013-07-09 A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism Talebizadeh, Zohreh Arking, Dan E. Hu, Valerie W. PLoS One Research Article Most genome linkage scans for autism spectrum disorders (ASDs) have failed to be replicated. Recently, a new ASD phenotypic sub-classification method was developed which employed cluster analyses of severity scores from the Autism Diagnostic Interview-Revised (ADI-R). Here, we performed linkage analysis for each of the four identified ADI-R stratified subgroups. Additional stratification was also applied to reduce intra-family heterogeneity and to investigate the impact of gender. For the purpose of replication, two independent sets of single nucleotide polymorphism markers for 392 families were used in our study. This deep subject stratification protocol resulted in 16 distinct group-specific datasets for linkage analysis. No locus reached significance for the combined non-stratified cohort. However, study-wide significant (P = 0.02) linkage scores were reached for chromosomes 22q11 (LOD = 4.43) and 13q21 (LOD = 4.37) for two subsets representing the most severely language impaired individuals with ASD. Notably, 13q21 has been previously linked to autism with language impairment, and 22q11 has been separately associated with either autism or language disorders. Linkage analysis on chromosome 5p15 for a combination of two stratified female-containing subgroups demonstrated suggestive linkage (LOD = 3.5), which replicates previous linkage result for female-containing pedigrees. A trend was also found for the association of previously reported 5p14-p15 SNPs in the same female-containing cohort. This study demonstrates a novel and effective method to address the heterogeneity in genetic studies of ASD. Moreover, the linkage results for the stratified subgroups provide evidence at the gene scan level for both inter- and intra-family heterogeneity as well as for gender-specific loci. Public Library of Science 2013-06-26 /pmc/articles/PMC3694043/ /pubmed/23840741 http://dx.doi.org/10.1371/journal.pone.0067569 Text en © 2013 Talebizadeh et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Talebizadeh, Zohreh
Arking, Dan E.
Hu, Valerie W.
A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title_full A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title_fullStr A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title_full_unstemmed A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title_short A Novel Stratification Method in Linkage Studies to Address Inter- and Intra-Family Heterogeneity in Autism
title_sort novel stratification method in linkage studies to address inter- and intra-family heterogeneity in autism
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3694043/
https://www.ncbi.nlm.nih.gov/pubmed/23840741
http://dx.doi.org/10.1371/journal.pone.0067569
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