Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes

Kirk E Lohmueller; Thomas Hempel Sparsø; Qibin Li; Ehm Andersson; Thorfinn Sand Korneliussen; Anders Albrechtsen; Karina Banasik; Niels Grarup; Ingileif Hallgrimsdottir; Kristoffer Kiil; Tuomas Kilpeläinen; Nikolaj Thure Krarup; Tune H Pers; Gaston Sanchez; Youna Hu; Michael Degiorgio; Torben Jørgensen; Annelli Sandbæk; Torsten Lauritzen; Søren Brunak; Karsten Kristiansen; Yingrui Li; Torben Hansen; Jun Wang; Rasmus Byrdal Nielsen; Oluf Borbye Pedersen

doi:10.1016/j.ajhg.2013.11.005

Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes

Kirk E Lohmueller, Thomas Hempel Sparsø, Qibin Li, Ehm Andersson, Thorfinn Sand Korneliussen, Anders Albrechtsen, Karina Banasik, Niels Grarup, Ingileif Hallgrimsdottir, Kristoffer Kiil, Tuomas Kilpeläinen, Nikolaj Thure Krarup, Tune H Pers, Gaston Sanchez, Youna Hu, Michael Degiorgio, Torben Jørgensen, Annelli Sandbæk, Torsten Lauritzen, Søren BrunakKarsten Kristiansen, Yingrui Li, Torben Hansen, Jun Wang, Rasmus Byrdal Nielsen, Oluf Borbye Pedersen

111 Citations (Scopus)

Abstract

It has been hypothesized that, in aggregate, rare variants in coding regions of genes explain a substantial fraction of the heritability of common diseases. We sequenced the exomes of 1,000 Danish cases with common forms of type 2 diabetes (including body mass index > 27.5 kg/m(2) and hypertension) and 1,000 healthy controls to an average depth of 56×. Our simulations suggest that our study had the statistical power to detect at least one causal gene (a gene containing causal mutations) if the heritability of these common diseases was explained by rare variants in the coding regions of a limited number of genes. We applied a series of gene-based tests to detect such susceptibility genes. However, no gene showed a significant association with disease risk after we corrected for the number of genes analyzed. Thus, we could reject a model for the genetic architecture of type 2 diabetes where rare nonsynonymous variants clustered in a modest number of genes (fewer than 20) are responsible for the majority of disease risk.

Original language	English
Journal	American Journal of Human Genetics
Volume	93
Issue number	6
Pages (from-to)	1072-86
DOIs	https://doi.org/10.1016/j.ajhg.2013.11.005
Publication status	Published - 26 Nov 2013

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Lohmueller, K. E., Sparsø, T. H., Li, Q., Andersson, E., Korneliussen, T. S., Albrechtsen, A., Banasik, K., Grarup, N., Hallgrimsdottir, I., Kiil, K., Kilpeläinen, T., Krarup, N. T., Pers, T. H., Sanchez, G., Hu, Y., Degiorgio, M., Jørgensen, T., Sandbæk, A., Lauritzen, T., ... Pedersen, O. B. (2013). Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes. American Journal of Human Genetics, 93(6), 1072-86. https://doi.org/10.1016/j.ajhg.2013.11.005

Lohmueller, KE, Sparsø, TH, Li, Q, Andersson, E, Korneliussen, TS, Albrechtsen, A, Banasik, K, Grarup, N, Hallgrimsdottir, I, Kiil, K, Kilpeläinen, T, Krarup, NT, Pers, TH, Sanchez, G, Hu, Y, Degiorgio, M, Jørgensen, T, Sandbæk, A, Lauritzen, T, Brunak, S, Kristiansen, K, Li, Y, Hansen, T, Wang, J, Nielsen, RB & Pedersen, OB 2013, 'Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes', American Journal of Human Genetics, vol. 93, no. 6, pp. 1072-86. https://doi.org/10.1016/j.ajhg.2013.11.005

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title = "Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes",

abstract = "It has been hypothesized that, in aggregate, rare variants in coding regions of genes explain a substantial fraction of the heritability of common diseases. We sequenced the exomes of 1,000 Danish cases with common forms of type 2 diabetes (including body mass index > 27.5 kg/m(2) and hypertension) and 1,000 healthy controls to an average depth of 56×. Our simulations suggest that our study had the statistical power to detect at least one causal gene (a gene containing causal mutations) if the heritability of these common diseases was explained by rare variants in the coding regions of a limited number of genes. We applied a series of gene-based tests to detect such susceptibility genes. However, no gene showed a significant association with disease risk after we corrected for the number of genes analyzed. Thus, we could reject a model for the genetic architecture of type 2 diabetes where rare nonsynonymous variants clustered in a modest number of genes (fewer than 20) are responsible for the majority of disease risk.",

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AU - Andersson, Ehm

AU - Korneliussen, Thorfinn Sand

AU - Albrechtsen, Anders

AU - Banasik, Karina

AU - Grarup, Niels

AU - Hallgrimsdottir, Ingileif

AU - Kiil, Kristoffer

AU - Kilpeläinen, Tuomas

AU - Krarup, Nikolaj Thure

AU - Pers, Tune H

AU - Sanchez, Gaston

AU - Hu, Youna

AU - Degiorgio, Michael

AU - Jørgensen, Torben

AU - Sandbæk, Annelli

AU - Lauritzen, Torsten

AU - Brunak, Søren

AU - Kristiansen, Karsten

AU - Li, Yingrui

AU - Hansen, Torben

AU - Wang, Jun

AU - Nielsen, Rasmus Byrdal

AU - Pedersen, Oluf Borbye

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N2 - It has been hypothesized that, in aggregate, rare variants in coding regions of genes explain a substantial fraction of the heritability of common diseases. We sequenced the exomes of 1,000 Danish cases with common forms of type 2 diabetes (including body mass index > 27.5 kg/m(2) and hypertension) and 1,000 healthy controls to an average depth of 56×. Our simulations suggest that our study had the statistical power to detect at least one causal gene (a gene containing causal mutations) if the heritability of these common diseases was explained by rare variants in the coding regions of a limited number of genes. We applied a series of gene-based tests to detect such susceptibility genes. However, no gene showed a significant association with disease risk after we corrected for the number of genes analyzed. Thus, we could reject a model for the genetic architecture of type 2 diabetes where rare nonsynonymous variants clustered in a modest number of genes (fewer than 20) are responsible for the majority of disease risk.

AB - It has been hypothesized that, in aggregate, rare variants in coding regions of genes explain a substantial fraction of the heritability of common diseases. We sequenced the exomes of 1,000 Danish cases with common forms of type 2 diabetes (including body mass index > 27.5 kg/m(2) and hypertension) and 1,000 healthy controls to an average depth of 56×. Our simulations suggest that our study had the statistical power to detect at least one causal gene (a gene containing causal mutations) if the heritability of these common diseases was explained by rare variants in the coding regions of a limited number of genes. We applied a series of gene-based tests to detect such susceptibility genes. However, no gene showed a significant association with disease risk after we corrected for the number of genes analyzed. Thus, we could reject a model for the genetic architecture of type 2 diabetes where rare nonsynonymous variants clustered in a modest number of genes (fewer than 20) are responsible for the majority of disease risk.

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JO - American Journal of Human Genetics

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ER -

Whole-Exome Sequencing of 2,000 Danish Individuals and the Role of Rare Coding Variants in Type 2 Diabetes

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