Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations

Copy number variants (CNVs) are suggested to have a widespread impact on the human genome and phenotypes. To understand the role of CNVs across human diseases, we examine the CNV genomic landscape of 100,028 unrelated individuals of European ancestry, using SNP and CGH array datasets. We observe an...

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Autores principales: Li, Yun Rose, Glessner, Joseph T., Coe, Bradley P., Li, Jin, Mohebnasab, Maede, Chang, Xiao, Connolly, John, Kao, Charlly, Wei, Zhi, Bradfield, Jonathan, Kim, Cecilia, Hou, Cuiping, Khan, Munir, Mentch, Frank, Qiu, Haijun, Bakay, Marina, Cardinale, Christopher, Lemma, Maria, Abrams, Debra, Bridglall-Jhingoor, Andrew, Behr, Meckenzie, Harrison, Shanell, Otieno, George, Thomas, Alexandria, Wang, Fengxiang, Chiavacci, Rosetta, Wu, Lawrence, Hadley, Dexter, Goldmuntz, Elizabeth, Elia, Josephine, Maris, John, Grundmeier, Robert, Devoto, Marcella, Keating, Brendan, March, Michael, Pellagrino, Renata, Grant, Struan F. A., Sleiman, Patrick M. A., Li, Mingyao, Eichler, Evan E., Hakonarson, Hakon
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6959272/
https://www.ncbi.nlm.nih.gov/pubmed/31937769
http://dx.doi.org/10.1038/s41467-019-13624-1
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author Li, Yun Rose
Glessner, Joseph T.
Coe, Bradley P.
Li, Jin
Mohebnasab, Maede
Chang, Xiao
Connolly, John
Kao, Charlly
Wei, Zhi
Bradfield, Jonathan
Kim, Cecilia
Hou, Cuiping
Khan, Munir
Mentch, Frank
Qiu, Haijun
Bakay, Marina
Cardinale, Christopher
Lemma, Maria
Abrams, Debra
Bridglall-Jhingoor, Andrew
Behr, Meckenzie
Harrison, Shanell
Otieno, George
Thomas, Alexandria
Wang, Fengxiang
Chiavacci, Rosetta
Wu, Lawrence
Hadley, Dexter
Goldmuntz, Elizabeth
Elia, Josephine
Maris, John
Grundmeier, Robert
Devoto, Marcella
Keating, Brendan
March, Michael
Pellagrino, Renata
Grant, Struan F. A.
Sleiman, Patrick M. A.
Li, Mingyao
Eichler, Evan E.
Hakonarson, Hakon
author_facet Li, Yun Rose
Glessner, Joseph T.
Coe, Bradley P.
Li, Jin
Mohebnasab, Maede
Chang, Xiao
Connolly, John
Kao, Charlly
Wei, Zhi
Bradfield, Jonathan
Kim, Cecilia
Hou, Cuiping
Khan, Munir
Mentch, Frank
Qiu, Haijun
Bakay, Marina
Cardinale, Christopher
Lemma, Maria
Abrams, Debra
Bridglall-Jhingoor, Andrew
Behr, Meckenzie
Harrison, Shanell
Otieno, George
Thomas, Alexandria
Wang, Fengxiang
Chiavacci, Rosetta
Wu, Lawrence
Hadley, Dexter
Goldmuntz, Elizabeth
Elia, Josephine
Maris, John
Grundmeier, Robert
Devoto, Marcella
Keating, Brendan
March, Michael
Pellagrino, Renata
Grant, Struan F. A.
Sleiman, Patrick M. A.
Li, Mingyao
Eichler, Evan E.
Hakonarson, Hakon
author_sort Li, Yun Rose
collection PubMed
description Copy number variants (CNVs) are suggested to have a widespread impact on the human genome and phenotypes. To understand the role of CNVs across human diseases, we examine the CNV genomic landscape of 100,028 unrelated individuals of European ancestry, using SNP and CGH array datasets. We observe an average CNV burden of ~650 kb, identifying a total of 11,314 deletion, 5625 duplication, and 2746 homozygous deletion CNV regions (CNVRs). In all, 13.7% are unreported, 58.6% overlap with at least one gene, and 32.8% interrupt coding exons. These CNVRs are significantly more likely to overlap OMIM genes (2.94-fold), GWAS loci (1.52-fold), and non-coding RNAs (1.44-fold), compared with random distribution (P < 1 × 10(−3)). We uncover CNV associations with four major disease categories, including autoimmune, cardio-metabolic, oncologic, and neurological/psychiatric diseases, and identify several drug-repurposing opportunities. Our results demonstrate robust frequency definition for large-scale rare variant association studies, identify CNVs associated with major disease categories, and illustrate the pleiotropic impact of CNVs in human disease.
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spelling pubmed-69592722020-01-15 Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations Li, Yun Rose Glessner, Joseph T. Coe, Bradley P. Li, Jin Mohebnasab, Maede Chang, Xiao Connolly, John Kao, Charlly Wei, Zhi Bradfield, Jonathan Kim, Cecilia Hou, Cuiping Khan, Munir Mentch, Frank Qiu, Haijun Bakay, Marina Cardinale, Christopher Lemma, Maria Abrams, Debra Bridglall-Jhingoor, Andrew Behr, Meckenzie Harrison, Shanell Otieno, George Thomas, Alexandria Wang, Fengxiang Chiavacci, Rosetta Wu, Lawrence Hadley, Dexter Goldmuntz, Elizabeth Elia, Josephine Maris, John Grundmeier, Robert Devoto, Marcella Keating, Brendan March, Michael Pellagrino, Renata Grant, Struan F. A. Sleiman, Patrick M. A. Li, Mingyao Eichler, Evan E. Hakonarson, Hakon Nat Commun Article Copy number variants (CNVs) are suggested to have a widespread impact on the human genome and phenotypes. To understand the role of CNVs across human diseases, we examine the CNV genomic landscape of 100,028 unrelated individuals of European ancestry, using SNP and CGH array datasets. We observe an average CNV burden of ~650 kb, identifying a total of 11,314 deletion, 5625 duplication, and 2746 homozygous deletion CNV regions (CNVRs). In all, 13.7% are unreported, 58.6% overlap with at least one gene, and 32.8% interrupt coding exons. These CNVRs are significantly more likely to overlap OMIM genes (2.94-fold), GWAS loci (1.52-fold), and non-coding RNAs (1.44-fold), compared with random distribution (P < 1 × 10(−3)). We uncover CNV associations with four major disease categories, including autoimmune, cardio-metabolic, oncologic, and neurological/psychiatric diseases, and identify several drug-repurposing opportunities. Our results demonstrate robust frequency definition for large-scale rare variant association studies, identify CNVs associated with major disease categories, and illustrate the pleiotropic impact of CNVs in human disease. Nature Publishing Group UK 2020-01-14 /pmc/articles/PMC6959272/ /pubmed/31937769 http://dx.doi.org/10.1038/s41467-019-13624-1 Text en © The Author(s) 2020 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Li, Yun Rose
Glessner, Joseph T.
Coe, Bradley P.
Li, Jin
Mohebnasab, Maede
Chang, Xiao
Connolly, John
Kao, Charlly
Wei, Zhi
Bradfield, Jonathan
Kim, Cecilia
Hou, Cuiping
Khan, Munir
Mentch, Frank
Qiu, Haijun
Bakay, Marina
Cardinale, Christopher
Lemma, Maria
Abrams, Debra
Bridglall-Jhingoor, Andrew
Behr, Meckenzie
Harrison, Shanell
Otieno, George
Thomas, Alexandria
Wang, Fengxiang
Chiavacci, Rosetta
Wu, Lawrence
Hadley, Dexter
Goldmuntz, Elizabeth
Elia, Josephine
Maris, John
Grundmeier, Robert
Devoto, Marcella
Keating, Brendan
March, Michael
Pellagrino, Renata
Grant, Struan F. A.
Sleiman, Patrick M. A.
Li, Mingyao
Eichler, Evan E.
Hakonarson, Hakon
Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title_full Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title_fullStr Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title_full_unstemmed Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title_short Rare copy number variants in over 100,000 European ancestry subjects reveal multiple disease associations
title_sort rare copy number variants in over 100,000 european ancestry subjects reveal multiple disease associations
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6959272/
https://www.ncbi.nlm.nih.gov/pubmed/31937769
http://dx.doi.org/10.1038/s41467-019-13624-1
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