Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)

BACKGROUND: DNA copy number variants (CNVs) are found in 15% of subjects with ID but their association with phenotypic abnormalities has been predominantly studied in smaller cohorts of subjects with detailed yet non-systematically categorized phenotypes, or larger cohorts (thousands of cases) with...

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Autores principales: Qiao, Ying, Mercier, Eloi, Dastan, Jila, Hurlburt, Jane, McGillivray, Barbara, Chudley, Albert E, Farrell, Sandra, Bernier, Francois P, Lewis, ME Suzanne, Pavlidis, Paul, Rajcan-Separovic, Evica
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4107469/
https://www.ncbi.nlm.nih.gov/pubmed/25030379
http://dx.doi.org/10.1186/1471-2350-15-82
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author Qiao, Ying
Mercier, Eloi
Dastan, Jila
Hurlburt, Jane
McGillivray, Barbara
Chudley, Albert E
Farrell, Sandra
Bernier, Francois P
Lewis, ME Suzanne
Pavlidis, Paul
Rajcan-Separovic, Evica
author_facet Qiao, Ying
Mercier, Eloi
Dastan, Jila
Hurlburt, Jane
McGillivray, Barbara
Chudley, Albert E
Farrell, Sandra
Bernier, Francois P
Lewis, ME Suzanne
Pavlidis, Paul
Rajcan-Separovic, Evica
author_sort Qiao, Ying
collection PubMed
description BACKGROUND: DNA copy number variants (CNVs) are found in 15% of subjects with ID but their association with phenotypic abnormalities has been predominantly studied in smaller cohorts of subjects with detailed yet non-systematically categorized phenotypes, or larger cohorts (thousands of cases) with smaller number of generalized phenotypes. METHODS: We evaluated the association of de novo, familial and common CNVs detected in 78 ID subjects with phenotypic abnormalities classified using the Winter-Baraitser Dysmorphology Database (WBDD) (formerly the London Dysmorphology Database). Terminology for 34 primary (coarse) and 169 secondary (fine) phenotype features were used to categorize the abnormal phenotypes and determine the prevalence of each phenotype in patients grouped by the type of CNV they had. RESULTS: In our cohort more than 50% of cases had abnormalities in primary categories related to head (cranium, forehead, ears, eye globes, eye associated structures, nose) as well as hands and feet. The median number of primary and secondary abnormalities was 12 and 18 per subject, respectively, indicating that the cohort consisted of subjects with a high number of phenotypic abnormalities (median De Vries score for the cohort was 5). The prevalence of each phenotypic abnormality was comparable in patients with de novo or familial CNVs in comparison to those with only common CNVs, although a trend for increased frequency of cranial and forehead abnormalities was noted in subjects with rare de novo and familial CNVs. Two clusters of subjects were identified based on the prevalence of each fine phenotypic feature, with an average of 28.3 and 13.5 abnormal phenotypes/subject in the two clusters respectively (P < 0.05). CONCLUSIONS: Our study is a rare example of using standardized, deep morphologic phenotype clustering with phenotype/CNV correlation in a cohort of subjects with ID. The composition of the cohort inevitably influences the phenotype/genotype association, and our studies show that the influence of the de novo CNVs on the phenotype is less obvious in cohorts consisting of subjects with a high number of phenotypic abnormalities. The outcome of phenotype/genotype analysis also depends on the choice of phenotypes assessed and standardized phenotyping is required to minimize variability.
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spelling pubmed-41074692014-07-24 Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID) Qiao, Ying Mercier, Eloi Dastan, Jila Hurlburt, Jane McGillivray, Barbara Chudley, Albert E Farrell, Sandra Bernier, Francois P Lewis, ME Suzanne Pavlidis, Paul Rajcan-Separovic, Evica BMC Med Genet Research Article BACKGROUND: DNA copy number variants (CNVs) are found in 15% of subjects with ID but their association with phenotypic abnormalities has been predominantly studied in smaller cohorts of subjects with detailed yet non-systematically categorized phenotypes, or larger cohorts (thousands of cases) with smaller number of generalized phenotypes. METHODS: We evaluated the association of de novo, familial and common CNVs detected in 78 ID subjects with phenotypic abnormalities classified using the Winter-Baraitser Dysmorphology Database (WBDD) (formerly the London Dysmorphology Database). Terminology for 34 primary (coarse) and 169 secondary (fine) phenotype features were used to categorize the abnormal phenotypes and determine the prevalence of each phenotype in patients grouped by the type of CNV they had. RESULTS: In our cohort more than 50% of cases had abnormalities in primary categories related to head (cranium, forehead, ears, eye globes, eye associated structures, nose) as well as hands and feet. The median number of primary and secondary abnormalities was 12 and 18 per subject, respectively, indicating that the cohort consisted of subjects with a high number of phenotypic abnormalities (median De Vries score for the cohort was 5). The prevalence of each phenotypic abnormality was comparable in patients with de novo or familial CNVs in comparison to those with only common CNVs, although a trend for increased frequency of cranial and forehead abnormalities was noted in subjects with rare de novo and familial CNVs. Two clusters of subjects were identified based on the prevalence of each fine phenotypic feature, with an average of 28.3 and 13.5 abnormal phenotypes/subject in the two clusters respectively (P < 0.05). CONCLUSIONS: Our study is a rare example of using standardized, deep morphologic phenotype clustering with phenotype/CNV correlation in a cohort of subjects with ID. The composition of the cohort inevitably influences the phenotype/genotype association, and our studies show that the influence of the de novo CNVs on the phenotype is less obvious in cohorts consisting of subjects with a high number of phenotypic abnormalities. The outcome of phenotype/genotype analysis also depends on the choice of phenotypes assessed and standardized phenotyping is required to minimize variability. BioMed Central 2014-07-16 /pmc/articles/PMC4107469/ /pubmed/25030379 http://dx.doi.org/10.1186/1471-2350-15-82 Text en Copyright © 2014 Qiao et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/4.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), 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 Article
Qiao, Ying
Mercier, Eloi
Dastan, Jila
Hurlburt, Jane
McGillivray, Barbara
Chudley, Albert E
Farrell, Sandra
Bernier, Francois P
Lewis, ME Suzanne
Pavlidis, Paul
Rajcan-Separovic, Evica
Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title_full Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title_fullStr Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title_full_unstemmed Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title_short Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID)
title_sort copy number variants (cnvs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (id)
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4107469/
https://www.ncbi.nlm.nih.gov/pubmed/25030379
http://dx.doi.org/10.1186/1471-2350-15-82
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