Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome

BACKGROUND: Intellectual disability (ID) affects 2–3% of the population and may occur with or without multiple congenital anomalies (MCA) or other medical conditions. Established genetic syndromes and visible chromosome abnormalities account for a substantial percentage of ID diagnoses, although for...

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Autores principales: Pani, Ariel M., Hobart, Holly H., Morris, Colleen A., Mervis, Carolyn B., Bray-Ward, Patricia, Kimberley, Kendra W., Rios, Cecilia M., Clark, Robin C., Gulbronson, Maricela D., Gowans, Gordon C., Gregg, Ronald G.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2930846/
https://www.ncbi.nlm.nih.gov/pubmed/20824207
http://dx.doi.org/10.1371/journal.pone.0012349
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author Pani, Ariel M.
Hobart, Holly H.
Morris, Colleen A.
Mervis, Carolyn B.
Bray-Ward, Patricia
Kimberley, Kendra W.
Rios, Cecilia M.
Clark, Robin C.
Gulbronson, Maricela D.
Gowans, Gordon C.
Gregg, Ronald G.
author_facet Pani, Ariel M.
Hobart, Holly H.
Morris, Colleen A.
Mervis, Carolyn B.
Bray-Ward, Patricia
Kimberley, Kendra W.
Rios, Cecilia M.
Clark, Robin C.
Gulbronson, Maricela D.
Gowans, Gordon C.
Gregg, Ronald G.
author_sort Pani, Ariel M.
collection PubMed
description BACKGROUND: Intellectual disability (ID) affects 2–3% of the population and may occur with or without multiple congenital anomalies (MCA) or other medical conditions. Established genetic syndromes and visible chromosome abnormalities account for a substantial percentage of ID diagnoses, although for ∼50% the molecular etiology is unknown. Individuals with features suggestive of various syndromes but lacking their associated genetic anomalies pose a formidable clinical challenge. With the advent of microarray techniques, submicroscopic genome alterations not associated with known syndromes are emerging as a significant cause of ID and MCA. METHODOLOGY/PRINCIPAL FINDINGS: High-density SNP microarrays were used to determine genome wide copy number in 42 individuals: 7 with confirmed alterations in the WS region but atypical clinical phenotypes, 31 with ID and/or MCA, and 4 controls. One individual from the first group had the most telomeric gene in the WS critical region deleted along with 2 Mb of flanking sequence. A second person had the classic WS deletion and a rearrangement on chromosome 5p within the Cri du Chat syndrome (OMIM:123450) region. Six individuals from the ID/MCA group had large rearrangements (3 deletions, 3 duplications), one of whom had a large inversion associated with a deletion that was not detected by the SNP arrays. CONCLUSIONS/SIGNIFICANCE: Combining SNP microarray analyses and qPCR allowed us to clone and sequence 21 deletion breakpoints in individuals with atypical deletions in the WS region and/or ID or MCA. Comparison of these breakpoints to databases of genomic variation revealed that 52% occurred in regions harboring structural variants in the general population. For two probands the genomic alterations were flanked by segmental duplications, which frequently mediate recurrent genome rearrangements; these may represent new genomic disorders. While SNP arrays and related technologies can identify potentially pathogenic deletions and duplications, obtaining sequence information from the breakpoints frequently provides additional information.
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spelling pubmed-29308462010-09-03 Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome Pani, Ariel M. Hobart, Holly H. Morris, Colleen A. Mervis, Carolyn B. Bray-Ward, Patricia Kimberley, Kendra W. Rios, Cecilia M. Clark, Robin C. Gulbronson, Maricela D. Gowans, Gordon C. Gregg, Ronald G. PLoS One Research Article BACKGROUND: Intellectual disability (ID) affects 2–3% of the population and may occur with or without multiple congenital anomalies (MCA) or other medical conditions. Established genetic syndromes and visible chromosome abnormalities account for a substantial percentage of ID diagnoses, although for ∼50% the molecular etiology is unknown. Individuals with features suggestive of various syndromes but lacking their associated genetic anomalies pose a formidable clinical challenge. With the advent of microarray techniques, submicroscopic genome alterations not associated with known syndromes are emerging as a significant cause of ID and MCA. METHODOLOGY/PRINCIPAL FINDINGS: High-density SNP microarrays were used to determine genome wide copy number in 42 individuals: 7 with confirmed alterations in the WS region but atypical clinical phenotypes, 31 with ID and/or MCA, and 4 controls. One individual from the first group had the most telomeric gene in the WS critical region deleted along with 2 Mb of flanking sequence. A second person had the classic WS deletion and a rearrangement on chromosome 5p within the Cri du Chat syndrome (OMIM:123450) region. Six individuals from the ID/MCA group had large rearrangements (3 deletions, 3 duplications), one of whom had a large inversion associated with a deletion that was not detected by the SNP arrays. CONCLUSIONS/SIGNIFICANCE: Combining SNP microarray analyses and qPCR allowed us to clone and sequence 21 deletion breakpoints in individuals with atypical deletions in the WS region and/or ID or MCA. Comparison of these breakpoints to databases of genomic variation revealed that 52% occurred in regions harboring structural variants in the general population. For two probands the genomic alterations were flanked by segmental duplications, which frequently mediate recurrent genome rearrangements; these may represent new genomic disorders. While SNP arrays and related technologies can identify potentially pathogenic deletions and duplications, obtaining sequence information from the breakpoints frequently provides additional information. Public Library of Science 2010-08-31 /pmc/articles/PMC2930846/ /pubmed/20824207 http://dx.doi.org/10.1371/journal.pone.0012349 Text en Pani 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
Pani, Ariel M.
Hobart, Holly H.
Morris, Colleen A.
Mervis, Carolyn B.
Bray-Ward, Patricia
Kimberley, Kendra W.
Rios, Cecilia M.
Clark, Robin C.
Gulbronson, Maricela D.
Gowans, Gordon C.
Gregg, Ronald G.
Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title_full Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title_fullStr Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title_full_unstemmed Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title_short Genome Rearrangements Detected by SNP Microarrays in Individuals with Intellectual Disability Referred with Possible Williams Syndrome
title_sort genome rearrangements detected by snp microarrays in individuals with intellectual disability referred with possible williams syndrome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2930846/
https://www.ncbi.nlm.nih.gov/pubmed/20824207
http://dx.doi.org/10.1371/journal.pone.0012349
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