Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees

Goo Jun; Alisa Manning; Marcio Almeida; Matthew Zawistowski; Andrew R. Wood; Tanya M. Teslovich; Christian Fuchsberger; Shuang Feng; Pablo Cingolani; Kyle J. Gaulton; Thomas Dyer; Thomas W. Blackwell; Han Chen; Peter S. Chines; Sungkyoung Choi; Claire Churchhouse; Pierre Fontanillas; Ryan King; Sung Young Lee; Stephen E. Lincoln; Vasily Trubetskoy; Mark DePristo; Tasha Fingerlin; Robert Grossman; Jason Grundstad; Alison Heath; Jayoun Kim; Young Jin Kim; Jason Laramie; Jaehoon Lee; Heng Li; Xuanyao Liu; Oren Livne; Adam Locke; Julian Maller; Alexander Mazur; Andrew P. Morris; Toni I. Pollin; Derek Ragona; David Reich; Manuel A. Rivas; Laura J. Scott; Xueling Sim; Rick G. Tearle; Yik Ying Teo; Amy L. Williams; Sebastian Zöllner; Joanne E. Curran; Juan Peralta; Beena Akolkar; Graeme I. Bell; Noël P. Burtt; Nancy J. Cox; Jose C. Florez; Craig L. Hanis; Catherine McKeon; Karen L. Mohlke; Mark Seielstad; James G. Wilson; Gil Atzmon; Jennifer E. Below; Josée Dupuis; Dan L. Nicolae; Donna Lehman; Taesung Park; Sungho Won; Robert Sladek; David Altshuler; Mark I. McCarthy; Ravindranath Duggirala; Michael Boehnke; Timothy M. Frayling; Gonçalo R. Abecasis; John Blangero

doi:10.1073/pnas.1705859115

Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees

Goo Jun, Alisa Manning, Marcio Almeida, Matthew Zawistowski, Andrew R. Wood, Tanya M. Teslovich, Christian Fuchsberger, Shuang Feng, Pablo Cingolani, Kyle J. Gaulton, Thomas Dyer, Thomas W. Blackwell, Han Chen, Peter S. Chines, Sungkyoung Choi, Claire Churchhouse, Pierre Fontanillas, Ryan King, Sung Young Lee, Stephen E. LincolnVasily Trubetskoy, Mark DePristo, Tasha Fingerlin, Robert Grossman, Jason Grundstad, Alison Heath, Jayoun Kim, Young Jin Kim, Jason Laramie, Jaehoon Lee, Heng Li, Xuanyao Liu, Oren Livne, Adam Locke, Julian Maller, Alexander Mazur, Andrew P. Morris, Toni I. Pollin, Derek Ragona, David Reich, Manuel A. Rivas, Laura J. Scott, Xueling Sim, Rick G. Tearle, Yik Ying Teo, Amy L. Williams, Sebastian Zöllner, Joanne E. Curran, Juan Peralta, Beena Akolkar, Graeme I. Bell, Noël P. Burtt, Nancy J. Cox, Jose C. Florez, Craig L. Hanis, Catherine McKeon, Karen L. Mohlke, Mark Seielstad, James G. Wilson, Gil Atzmon, Jennifer E. Below, Josée Dupuis, Dan L. Nicolae, Donna Lehman, Taesung Park, Sungho Won, Robert Sladek, David Altshuler, Mark I. McCarthy, Ravindranath Duggirala, Michael Boehnke, Timothy M. Frayling, Gonçalo R. Abecasis, John Blangero

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27 Scopus citations

Abstract

A major challenge in evaluating the contribution of rare variants to complex disease is identifying enough copies of the rare alleles to permit informative statistical analysis. To investigate the contribution of rare variants to the risk of type 2 diabetes (T2D) and related traits, we performed deep whole-genome analysis of 1,034 members of 20 large Mexican-American families with high prevalence of T2D. If rare variants of large effect accounted for much of the diabetes risk in these families, our experiment was powered to detect association. Using gene expression data on 21,677 transcripts for 643 pedigree members, we identified evidence for large-effect rare-variant cis-expression quantitative trait loci that could not be detected in population studies, validating our approach. However, we did not identify any rare variants of large effect associated with T2D, or the related traits of fasting glucose and insulin, suggesting that large-effect rare variants account for only a modest fraction of the genetic risk of these traits in this sample of families. Reliable identification of large-effect rare variants will require larger samples of extended pedigrees or different study designs that further enrich for such variants.

Original language	English
Pages (from-to)	379-384
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	115
Issue number	2
DOIs	https://doi.org/10.1073/pnas.1705859115
State	Published - Jan 9 2017

Keywords

EQTL
Genetics
Rare variants
Sequencing
Type 2 diabetes

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10.1073/pnas.1705859115

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Jun, G., Manning, A., Almeida, M., Zawistowski, M., Wood, A. R., Teslovich, T. M., Fuchsberger, C., Feng, S., Cingolani, P., Gaulton, K. J., Dyer, T., Blackwell, T. W., Chen, H., Chines, P. S., Choi, S., Churchhouse, C., Fontanillas, P., King, R., Lee, S. Y., ... Blangero, J. (2017). Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees. Proceedings of the National Academy of Sciences of the United States of America, 115(2), 379-384. https://doi.org/10.1073/pnas.1705859115

@article{8e68bbfca15a4273bc2eefb3b2f53124,

title = "Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees",

abstract = "A major challenge in evaluating the contribution of rare variants to complex disease is identifying enough copies of the rare alleles to permit informative statistical analysis. To investigate the contribution of rare variants to the risk of type 2 diabetes (T2D) and related traits, we performed deep whole-genome analysis of 1,034 members of 20 large Mexican-American families with high prevalence of T2D. If rare variants of large effect accounted for much of the diabetes risk in these families, our experiment was powered to detect association. Using gene expression data on 21,677 transcripts for 643 pedigree members, we identified evidence for large-effect rare-variant cis-expression quantitative trait loci that could not be detected in population studies, validating our approach. However, we did not identify any rare variants of large effect associated with T2D, or the related traits of fasting glucose and insulin, suggesting that large-effect rare variants account for only a modest fraction of the genetic risk of these traits in this sample of families. Reliable identification of large-effect rare variants will require larger samples of extended pedigrees or different study designs that further enrich for such variants.",

keywords = "EQTL, Genetics, Rare variants, Sequencing, Type 2 diabetes",

author = "Goo Jun and Alisa Manning and Marcio Almeida and Matthew Zawistowski and Wood, {Andrew R.} and Teslovich, {Tanya M.} and Christian Fuchsberger and Shuang Feng and Pablo Cingolani and Gaulton, {Kyle J.} and Thomas Dyer and Blackwell, {Thomas W.} and Han Chen and Chines, {Peter S.} and Sungkyoung Choi and Claire Churchhouse and Pierre Fontanillas and Ryan King and Lee, {Sung Young} and Lincoln, {Stephen E.} and Vasily Trubetskoy and Mark DePristo and Tasha Fingerlin and Robert Grossman and Jason Grundstad and Alison Heath and Jayoun Kim and Kim, {Young Jin} and Jason Laramie and Jaehoon Lee and Heng Li and Xuanyao Liu and Oren Livne and Adam Locke and Julian Maller and Alexander Mazur and Morris, {Andrew P.} and Pollin, {Toni I.} and Derek Ragona and David Reich and Rivas, {Manuel A.} and Scott, {Laura J.} and Xueling Sim and Tearle, {Rick G.} and Teo, {Yik Ying} and Williams, {Amy L.} and Sebastian Z{\"o}llner and Curran, {Joanne E.} and Juan Peralta and Beena Akolkar and Bell, {Graeme I.} and Burtt, {No{\"e}l P.} and Cox, {Nancy J.} and Florez, {Jose C.} and Hanis, {Craig L.} and Catherine McKeon and Mohlke, {Karen L.} and Mark Seielstad and Wilson, {James G.} and Gil Atzmon and Below, {Jennifer E.} and Jos{\'e}e Dupuis and Nicolae, {Dan L.} and Donna Lehman and Taesung Park and Sungho Won and Robert Sladek and David Altshuler and McCarthy, {Mark I.} and Ravindranath Duggirala and Michael Boehnke and Frayling, {Timothy M.} and Abecasis, {Gon{\c c}alo R.} and John Blangero",

note = "Funding Information: We warmly thank the participants of the SAFHS and SAFDGS for their contribution, enthusiasm, and cooperation. This study is part of the Type 2 Diabetes Genetic Exploration by Next-generation sequencing in multi-Ethnic Samples (T2D-GENES) Consortium, funded by the European Commission (HEALTH-F4-2007-201413), Wellcome Trust (090367, 090532, 098381), Medical Research Council (G0601261), and NIH/NIDDK (RC2-DK08839, DK105535, DK085524, DK085545, DK085584, DK085501, DK098032, DK078616, DK085526). The whole-genome sequencing was done commercially by Complete Genomics, Inc. Additional genetic and phenotypic data were provided by the San Antonio Family Heart Study and San Antonio Family Diabetes/Gallbladder Study, which are supported by NIH Grants R01 HL0113323, P01 HL045222, R01 DK047482, and R01 DK053889. SAFHS gene expression data were generated through a donation from the Azar and Shepperd families. J.G.W. was supported by U54GM115428 from the National Institute of General Medical Sciences. S.C., S.L., J.K., J. Lee, and T.P. were supported by the Bio-Synergy Research Project (2013M3A9C4078158) of the Ministry of Science, ICT and Future Planning through the National Research Foundation of Korea, and Korea Health Technology R&D Project through the Korea Health Industry Development Institute, funded by the Ministry of Health and Welfare (HI15C2165, HI16C2037). A.K.M. was supported by American Diabetes Association Mentor-Based Postdoctoral Fellowship #7-12-MN-02. M.I.M. is a Wellcome Trust Senior Investigator. The research was supported by the National Institute for Health Research (NIHR), Oxford Biomedical Research Centre. The views expressed are those of the authors and not necessarily those of the National Health Service, NIHR, or Department of Health, United Kingdom. Funding Information: and R01 DK053889. SAFHS gene expression data were generated through a donation from the Azar and Shepperd families. J.G.W. was supported by U54GM115428 from the National Institute of General Medical Sciences. S.C., S.L., J.K., J. Lee, and T.P. were supported by the Bio-Synergy Research Project (2013M3A9C4078158) of the Ministry of Science, ICT and Future Planning through the National Research Foundation of Korea, and Korea Health Technology R&D Project through the Korea Health Industry Development Institute, funded by the Ministry of Health and Welfare (HI15C2165, HI16C2037). A.K.M. was supported by American Diabetes Association Mentor-Based Postdoctoral Fellowship #7-12-MN-02. M.I.M. is a Wellcome Trust Senior Investigator. The research was supported by the National Institute for Health Research (NIHR), Oxford Biomedical Research Centre. The views expressed are those of the authors and not necessarily those of the National Health Service, NIHR, or Department of Health, United Kingdom. Funding Information: ACKNOWLEDGMENTS. We warmly thank the participants of the SAFHS and SAFDGS for their contribution, enthusiasm, and cooperation. This study is part of the Type 2 Diabetes Genetic Exploration by Next-generation sequencing in multi-Ethnic Samples (T2D-GENES) Consortium, funded by the European Commission (HEALTH-F4-2007-201413), Wellcome Trust (090367, 090532, 098381), Medical Research Council (G0601261), and NIH/NIDDK (RC2-DK08839, DK105535, DK085524, DK085545, DK085584, DK085501, DK098032, DK078616, DK085526). The whole-genome sequencing was done commercially by Complete Genomics, Inc. Additional genetic and phenotypic data were provided by the San Antonio Family Heart Study and San Antonio Family Diabetes/Gallbladder Study, which are supported by NIH Grants R01 HL0113323, P01 HL045222, R01 DK047482,",

year = "2017",

month = jan,

day = "9",

doi = "10.1073/pnas.1705859115",

language = "English",

volume = "115",

pages = "379--384",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

number = "2",

}

Jun, G, Manning, A, Almeida, M, Zawistowski, M, Wood, AR, Teslovich, TM, Fuchsberger, C, Feng, S, Cingolani, P, Gaulton, KJ, Dyer, T, Blackwell, TW, Chen, H, Chines, PS, Choi, S, Churchhouse, C, Fontanillas, P, King, R, Lee, SY, Lincoln, SE, Trubetskoy, V, DePristo, M, Fingerlin, T, Grossman, R, Grundstad, J, Heath, A, Kim, J, Kim, YJ, Laramie, J, Lee, J, Li, H, Liu, X, Livne, O, Locke, A, Maller, J, Mazur, A, Morris, AP, Pollin, TI, Ragona, D, Reich, D, Rivas, MA, Scott, LJ, Sim, X, Tearle, RG, Teo, YY, Williams, AL, Zöllner, S, Curran, JE, Peralta, J, Akolkar, B, Bell, GI, Burtt, NP, Cox, NJ, Florez, JC, Hanis, CL, McKeon, C, Mohlke, KL, Seielstad, M, Wilson, JG, Atzmon, G, Below, JE, Dupuis, J, Nicolae, DL, Lehman, D, Park, T, Won, S, Sladek, R, Altshuler, D, McCarthy, MI, Duggirala, R, Boehnke, M, Frayling, TM, Abecasis, GR & Blangero, J 2017, 'Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees', Proceedings of the National Academy of Sciences of the United States of America, vol. 115, no. 2, pp. 379-384. https://doi.org/10.1073/pnas.1705859115

TY - JOUR

T1 - Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees

AU - Jun, Goo

AU - Manning, Alisa

AU - Almeida, Marcio

AU - Zawistowski, Matthew

AU - Wood, Andrew R.

AU - Teslovich, Tanya M.

AU - Fuchsberger, Christian

AU - Feng, Shuang

AU - Cingolani, Pablo

AU - Gaulton, Kyle J.

AU - Dyer, Thomas

AU - Blackwell, Thomas W.

AU - Chen, Han

AU - Chines, Peter S.

AU - Choi, Sungkyoung

AU - Churchhouse, Claire

AU - Fontanillas, Pierre

AU - King, Ryan

AU - Lee, Sung Young

AU - Lincoln, Stephen E.

AU - Trubetskoy, Vasily

AU - DePristo, Mark

AU - Fingerlin, Tasha

AU - Grossman, Robert

AU - Grundstad, Jason

AU - Heath, Alison

AU - Kim, Jayoun

AU - Kim, Young Jin

AU - Laramie, Jason

AU - Lee, Jaehoon

AU - Li, Heng

AU - Liu, Xuanyao

AU - Livne, Oren

AU - Locke, Adam

AU - Maller, Julian

AU - Mazur, Alexander

AU - Morris, Andrew P.

AU - Pollin, Toni I.

AU - Ragona, Derek

AU - Reich, David

AU - Rivas, Manuel A.

AU - Scott, Laura J.

AU - Sim, Xueling

AU - Tearle, Rick G.

AU - Teo, Yik Ying

AU - Williams, Amy L.

AU - Zöllner, Sebastian

AU - Curran, Joanne E.

AU - Peralta, Juan

AU - Akolkar, Beena

AU - Bell, Graeme I.

AU - Burtt, Noël P.

AU - Cox, Nancy J.

AU - Florez, Jose C.

AU - Hanis, Craig L.

AU - McKeon, Catherine

AU - Mohlke, Karen L.

AU - Seielstad, Mark

AU - Wilson, James G.

AU - Atzmon, Gil

AU - Below, Jennifer E.

AU - Dupuis, Josée

AU - Nicolae, Dan L.

AU - Lehman, Donna

AU - Park, Taesung

AU - Won, Sungho

AU - Sladek, Robert

AU - Altshuler, David

AU - McCarthy, Mark I.

AU - Duggirala, Ravindranath

AU - Boehnke, Michael

AU - Frayling, Timothy M.

AU - Abecasis, Gonçalo R.

AU - Blangero, John

N1 - Funding Information: We warmly thank the participants of the SAFHS and SAFDGS for their contribution, enthusiasm, and cooperation. This study is part of the Type 2 Diabetes Genetic Exploration by Next-generation sequencing in multi-Ethnic Samples (T2D-GENES) Consortium, funded by the European Commission (HEALTH-F4-2007-201413), Wellcome Trust (090367, 090532, 098381), Medical Research Council (G0601261), and NIH/NIDDK (RC2-DK08839, DK105535, DK085524, DK085545, DK085584, DK085501, DK098032, DK078616, DK085526). The whole-genome sequencing was done commercially by Complete Genomics, Inc. Additional genetic and phenotypic data were provided by the San Antonio Family Heart Study and San Antonio Family Diabetes/Gallbladder Study, which are supported by NIH Grants R01 HL0113323, P01 HL045222, R01 DK047482, and R01 DK053889. SAFHS gene expression data were generated through a donation from the Azar and Shepperd families. J.G.W. was supported by U54GM115428 from the National Institute of General Medical Sciences. S.C., S.L., J.K., J. Lee, and T.P. were supported by the Bio-Synergy Research Project (2013M3A9C4078158) of the Ministry of Science, ICT and Future Planning through the National Research Foundation of Korea, and Korea Health Technology R&D Project through the Korea Health Industry Development Institute, funded by the Ministry of Health and Welfare (HI15C2165, HI16C2037). A.K.M. was supported by American Diabetes Association Mentor-Based Postdoctoral Fellowship #7-12-MN-02. M.I.M. is a Wellcome Trust Senior Investigator. The research was supported by the National Institute for Health Research (NIHR), Oxford Biomedical Research Centre. The views expressed are those of the authors and not necessarily those of the National Health Service, NIHR, or Department of Health, United Kingdom. Funding Information: and R01 DK053889. SAFHS gene expression data were generated through a donation from the Azar and Shepperd families. J.G.W. was supported by U54GM115428 from the National Institute of General Medical Sciences. S.C., S.L., J.K., J. Lee, and T.P. were supported by the Bio-Synergy Research Project (2013M3A9C4078158) of the Ministry of Science, ICT and Future Planning through the National Research Foundation of Korea, and Korea Health Technology R&D Project through the Korea Health Industry Development Institute, funded by the Ministry of Health and Welfare (HI15C2165, HI16C2037). A.K.M. was supported by American Diabetes Association Mentor-Based Postdoctoral Fellowship #7-12-MN-02. M.I.M. is a Wellcome Trust Senior Investigator. The research was supported by the National Institute for Health Research (NIHR), Oxford Biomedical Research Centre. The views expressed are those of the authors and not necessarily those of the National Health Service, NIHR, or Department of Health, United Kingdom. Funding Information: ACKNOWLEDGMENTS. We warmly thank the participants of the SAFHS and SAFDGS for their contribution, enthusiasm, and cooperation. This study is part of the Type 2 Diabetes Genetic Exploration by Next-generation sequencing in multi-Ethnic Samples (T2D-GENES) Consortium, funded by the European Commission (HEALTH-F4-2007-201413), Wellcome Trust (090367, 090532, 098381), Medical Research Council (G0601261), and NIH/NIDDK (RC2-DK08839, DK105535, DK085524, DK085545, DK085584, DK085501, DK098032, DK078616, DK085526). The whole-genome sequencing was done commercially by Complete Genomics, Inc. Additional genetic and phenotypic data were provided by the San Antonio Family Heart Study and San Antonio Family Diabetes/Gallbladder Study, which are supported by NIH Grants R01 HL0113323, P01 HL045222, R01 DK047482,

PY - 2017/1/9

Y1 - 2017/1/9

N2 - A major challenge in evaluating the contribution of rare variants to complex disease is identifying enough copies of the rare alleles to permit informative statistical analysis. To investigate the contribution of rare variants to the risk of type 2 diabetes (T2D) and related traits, we performed deep whole-genome analysis of 1,034 members of 20 large Mexican-American families with high prevalence of T2D. If rare variants of large effect accounted for much of the diabetes risk in these families, our experiment was powered to detect association. Using gene expression data on 21,677 transcripts for 643 pedigree members, we identified evidence for large-effect rare-variant cis-expression quantitative trait loci that could not be detected in population studies, validating our approach. However, we did not identify any rare variants of large effect associated with T2D, or the related traits of fasting glucose and insulin, suggesting that large-effect rare variants account for only a modest fraction of the genetic risk of these traits in this sample of families. Reliable identification of large-effect rare variants will require larger samples of extended pedigrees or different study designs that further enrich for such variants.

AB - A major challenge in evaluating the contribution of rare variants to complex disease is identifying enough copies of the rare alleles to permit informative statistical analysis. To investigate the contribution of rare variants to the risk of type 2 diabetes (T2D) and related traits, we performed deep whole-genome analysis of 1,034 members of 20 large Mexican-American families with high prevalence of T2D. If rare variants of large effect accounted for much of the diabetes risk in these families, our experiment was powered to detect association. Using gene expression data on 21,677 transcripts for 643 pedigree members, we identified evidence for large-effect rare-variant cis-expression quantitative trait loci that could not be detected in population studies, validating our approach. However, we did not identify any rare variants of large effect associated with T2D, or the related traits of fasting glucose and insulin, suggesting that large-effect rare variants account for only a modest fraction of the genetic risk of these traits in this sample of families. Reliable identification of large-effect rare variants will require larger samples of extended pedigrees or different study designs that further enrich for such variants.

KW - EQTL

KW - Genetics

KW - Rare variants

KW - Sequencing

KW - Type 2 diabetes

UR - http://www.scopus.com/inward/record.url?scp=85040252130&partnerID=8YFLogxK

U2 - 10.1073/pnas.1705859115

DO - 10.1073/pnas.1705859115

M3 - Article

C2 - 29279374

AN - SCOPUS:85040252130

SN - 0027-8424

VL - 115

SP - 379

EP - 384

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 2

ER -

Evaluating the contribution of rare variants to type 2 diabetes and related traits using pedigrees

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