Understanding the impact of 1q21.1 copy number variant

BACKGROUND: 1q21.1 Copy Number Variant (CNV) is associated with a highly variable phenotype ranging from congenital anomalies, learning deficits/intellectual disability (ID), to a normal phenotype. Hence, the clinical significance of this CNV can be difficult to evaluate. Here we described the conse...

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Autores principales: Harvard, Chansonette, Strong, Emma, Mercier, Eloi, Colnaghi, Rita, Alcantara, Diana, Chow, Eva, Martell, Sally, Tyson, Christine, Hrynchak, Monica, McGillivray, Barbara, Hamilton, Sara, Marles, Sandra, Mhanni, Aziz, Dawson, Angelika J, Pavlidis, Paul, Qiao, Ying, Holden, Jeanette J, Lewis, Suzanne ME, O'Driscoll, Mark, Rajcan-Separovic, Evica
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3180300/
https://www.ncbi.nlm.nih.gov/pubmed/21824431
http://dx.doi.org/10.1186/1750-1172-6-54
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author Harvard, Chansonette
Strong, Emma
Mercier, Eloi
Colnaghi, Rita
Alcantara, Diana
Chow, Eva
Martell, Sally
Tyson, Christine
Hrynchak, Monica
McGillivray, Barbara
Hamilton, Sara
Marles, Sandra
Mhanni, Aziz
Dawson, Angelika J
Pavlidis, Paul
Qiao, Ying
Holden, Jeanette J
Lewis, Suzanne ME
O'Driscoll, Mark
Rajcan-Separovic, Evica
author_facet Harvard, Chansonette
Strong, Emma
Mercier, Eloi
Colnaghi, Rita
Alcantara, Diana
Chow, Eva
Martell, Sally
Tyson, Christine
Hrynchak, Monica
McGillivray, Barbara
Hamilton, Sara
Marles, Sandra
Mhanni, Aziz
Dawson, Angelika J
Pavlidis, Paul
Qiao, Ying
Holden, Jeanette J
Lewis, Suzanne ME
O'Driscoll, Mark
Rajcan-Separovic, Evica
author_sort Harvard, Chansonette
collection PubMed
description BACKGROUND: 1q21.1 Copy Number Variant (CNV) is associated with a highly variable phenotype ranging from congenital anomalies, learning deficits/intellectual disability (ID), to a normal phenotype. Hence, the clinical significance of this CNV can be difficult to evaluate. Here we described the consequences of the 1q21.1 CNV on genome-wide gene expression and function of selected candidate genes within 1q21.1 using cell lines from clinically well described subjects. METHODS AND RESULTS: Eight subjects from 3 families were included in the study: six with a 1q21.1 deletion and two with a 1q21.1 duplication. High resolution Affymetrix 2.7M array was used to refine the 1q21.1 CNV breakpoints and exclude the presence of secondary CNVs of pathogenic relevance. Whole genome expression profiling, studied in lymphoblast cell lines (LBCs) from 5 subjects, showed enrichment of genes from 1q21.1 in the top 100 genes ranked based on correlation of expression with 1q21.1 copy number. The function of two top genes from 1q21.1, CHD1L/ALC1 and PRKAB2, was studied in detail in LBCs from a deletion and a duplication carrier. CHD1L/ALC1 is an enzyme with a role in chromatin modification and DNA damage response while PRKAB2 is a member of the AMP kinase complex, which senses and maintains systemic and cellular energy balance. The protein levels for CHD1L/ALC1 and PRKAB2 were changed in concordance with their copy number in both LBCs. A defect in chromatin remodeling was documented based on impaired decatenation (chromatid untangling) checkpoint (DCC) in both LBCs. This defect, reproduced by CHD1L/ALC1 siRNA, identifies a new role of CHD1L/ALC1 in DCC. Both LBCs also showed elevated levels of micronuclei following treatment with a Topoisomerase II inhibitor suggesting increased DNA breaks. AMP kinase function, specifically in the deletion containing LBCs, was attenuated. CONCLUSION: Our studies are unique as they show for the first time that the 1q21.1 CNV not only causes changes in the expression of its key integral genes, associated with changes at the protein level, but also results in changes in their known function, in the case of AMPK, and newly identified function such as DCC activation in the case of CHD1L/ALC1. Our results support the use of patient lymphoblasts for dissecting the functional sequelae of genes integral to CNVs in carrier cell lines, ultimately enhancing understanding of biological processes which may contribute to the clinical phenotype.
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spelling pubmed-31803002011-09-27 Understanding the impact of 1q21.1 copy number variant Harvard, Chansonette Strong, Emma Mercier, Eloi Colnaghi, Rita Alcantara, Diana Chow, Eva Martell, Sally Tyson, Christine Hrynchak, Monica McGillivray, Barbara Hamilton, Sara Marles, Sandra Mhanni, Aziz Dawson, Angelika J Pavlidis, Paul Qiao, Ying Holden, Jeanette J Lewis, Suzanne ME O'Driscoll, Mark Rajcan-Separovic, Evica Orphanet J Rare Dis Research BACKGROUND: 1q21.1 Copy Number Variant (CNV) is associated with a highly variable phenotype ranging from congenital anomalies, learning deficits/intellectual disability (ID), to a normal phenotype. Hence, the clinical significance of this CNV can be difficult to evaluate. Here we described the consequences of the 1q21.1 CNV on genome-wide gene expression and function of selected candidate genes within 1q21.1 using cell lines from clinically well described subjects. METHODS AND RESULTS: Eight subjects from 3 families were included in the study: six with a 1q21.1 deletion and two with a 1q21.1 duplication. High resolution Affymetrix 2.7M array was used to refine the 1q21.1 CNV breakpoints and exclude the presence of secondary CNVs of pathogenic relevance. Whole genome expression profiling, studied in lymphoblast cell lines (LBCs) from 5 subjects, showed enrichment of genes from 1q21.1 in the top 100 genes ranked based on correlation of expression with 1q21.1 copy number. The function of two top genes from 1q21.1, CHD1L/ALC1 and PRKAB2, was studied in detail in LBCs from a deletion and a duplication carrier. CHD1L/ALC1 is an enzyme with a role in chromatin modification and DNA damage response while PRKAB2 is a member of the AMP kinase complex, which senses and maintains systemic and cellular energy balance. The protein levels for CHD1L/ALC1 and PRKAB2 were changed in concordance with their copy number in both LBCs. A defect in chromatin remodeling was documented based on impaired decatenation (chromatid untangling) checkpoint (DCC) in both LBCs. This defect, reproduced by CHD1L/ALC1 siRNA, identifies a new role of CHD1L/ALC1 in DCC. Both LBCs also showed elevated levels of micronuclei following treatment with a Topoisomerase II inhibitor suggesting increased DNA breaks. AMP kinase function, specifically in the deletion containing LBCs, was attenuated. CONCLUSION: Our studies are unique as they show for the first time that the 1q21.1 CNV not only causes changes in the expression of its key integral genes, associated with changes at the protein level, but also results in changes in their known function, in the case of AMPK, and newly identified function such as DCC activation in the case of CHD1L/ALC1. Our results support the use of patient lymphoblasts for dissecting the functional sequelae of genes integral to CNVs in carrier cell lines, ultimately enhancing understanding of biological processes which may contribute to the clinical phenotype. BioMed Central 2011-08-08 /pmc/articles/PMC3180300/ /pubmed/21824431 http://dx.doi.org/10.1186/1750-1172-6-54 Text en Copyright ©2011 Harvard 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 cited.
spellingShingle Research
Harvard, Chansonette
Strong, Emma
Mercier, Eloi
Colnaghi, Rita
Alcantara, Diana
Chow, Eva
Martell, Sally
Tyson, Christine
Hrynchak, Monica
McGillivray, Barbara
Hamilton, Sara
Marles, Sandra
Mhanni, Aziz
Dawson, Angelika J
Pavlidis, Paul
Qiao, Ying
Holden, Jeanette J
Lewis, Suzanne ME
O'Driscoll, Mark
Rajcan-Separovic, Evica
Understanding the impact of 1q21.1 copy number variant
title Understanding the impact of 1q21.1 copy number variant
title_full Understanding the impact of 1q21.1 copy number variant
title_fullStr Understanding the impact of 1q21.1 copy number variant
title_full_unstemmed Understanding the impact of 1q21.1 copy number variant
title_short Understanding the impact of 1q21.1 copy number variant
title_sort understanding the impact of 1q21.1 copy number variant
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3180300/
https://www.ncbi.nlm.nih.gov/pubmed/21824431
http://dx.doi.org/10.1186/1750-1172-6-54
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