Meta-analysis of Dense Genecentric Association Studies Reveals Common and Uncommon Variants Associated with Height

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• 作者：Matthew B. Lanktree¹ ; ¹¹⁵ ; Yiran Guo² ; ³ ; ¹¹⁵ ; Muhammed Murtaza⁴ ; ⁶⁶ ; Joseph T. Glessner² ; Swneke D. Bailey⁶ ; N. Charlotte Onland-Moret²¹ ; Guillaume Lettre⁵ ; Halit Ongen⁸ ; Ramakrishnan Rajagopalan¹⁰ ; Toby Johnson⁹ ; Haiqing Shen¹¹ ; Christopher P. Nelson¹⁵ ; ⁸⁶ ; Norman Klopp¹² ; Jens Baumert¹² ; Sandosh Padmanabhan⁵⁴ ; Nathan Pankratz²⁴ ; ⁸³ ; James S. Pankow⁸³ ; Sonia Shah⁸⁷ ; Kira Taylor¹³ ; John Barnard¹⁴ ; Bas J. Peters¹⁰⁸ ; Cliona M. Maloney³⁰ ; Maximilian T. Lobmeyer¹⁶ ; Alice Stanton⁵⁸ ; M. Hadi Zafarmand¹⁸ ; ¹⁰⁹ ; Simon P.R. Romaine²³ ; Amar Mehta²⁵ ; Erik P.A. van Iperen²² ; ⁸² ; Yan Gong¹⁶ ; Tom S. Price²⁰ ; Erin N. Smith³¹ ; Cecilia E. Kim² ; Yun R. Li² ; Folkert W. Asselbergs¹⁸ ; ²¹ ; ¹⁰⁹ ; Larry D. Atwood³⁵ ; Kristian M. Bailey²³ ; Deepak Bhatt⁹⁹ ; Florianne Bauer²¹ ; Elijah R. Behr⁴⁵ ; Tushar Bhangale⁴³ ; Jolanda M.A. Boer²⁸ ; Bernhard O. Boehm⁹² ; Jonathan P. Bradfield² ; Morris Brown⁹⁵ ; Peter S. Braund¹⁵ ; ⁸⁶ ; Paul R. Burton³² ; Cara Carty¹⁹ ; Hareesh R. Chandrupatla²⁹ ; Wei Chen¹⁰⁵ ; John Connell³⁸ ; Chrysoula Dalgeorgou⁴⁶ ; Anthonius de Boer¹⁰⁸ ; Fotios Drenos²⁷ ; Clara C. Elbers²¹ ; James C. Fang⁵¹ ; Caroline S. Fox³⁵ ; Edward C. Frackelton² ; Barry Fuchs³⁶ ; Clement E. Furlong¹⁰ ; Quince Gibson¹¹ ; Christian Gieger¹² ; Anuj Goel⁸ ; ⁷² ; Diederik E. Grobbee¹⁰⁴ ; Claire Hastie⁵⁴ ; Philip J. Howard⁹ ; Guan-Hua Huang⁵² ; W. Craig Johnson³⁴ ; Qing Li¹¹¹ ; Marcus E. Kleber⁸⁸ ; Barbara E.K. Klein¹⁷ ; Ronald Klein¹⁷ ; Charles Kooperberg¹⁹ ; Bonnie Ky⁵⁰ ; Andrea LaCroix¹⁹ ; Paul Lanken³⁶ ; Mark Lathrop⁹⁶ ; Mingyao Li²⁹ ; Vanessa Marshall⁹⁴ ; Olle Melander⁵⁵ ; Frank D. Mentch² ; Nuala J. Meyer³⁶ ; Keri L. Monda⁴⁰ ; Alexandre Montpetit⁴² ; Gurunathan Murugesan³³ ; Karen Nakayama¹⁰ ; Dave Nondahl¹⁷ ; Abiodun Onipinla⁹ ; Suzanne Rafelt¹⁵ ; ⁸⁶ ; Stephen J. Newhouse⁹ ; F. George Otieno² ; Sanjey R. Patel⁴¹ ; Mary E. Putt¹⁰² ; Santiago Rodriguez⁵³ ; Radwan N. Safa⁴⁹ ; Douglas B. Sawyer⁴⁸ ; Pamela J. Schreiner³⁹ ; Claire Simpson¹¹¹ ; Suthesh Sivapalaratnam²⁶ ; Sathanur R. Srinivasan¹⁰⁵ ; Christine Suver³⁰ ; Gary Swergold¹¹² ; Nancy K. Sweitzer⁴⁷ ; Kelly A. Thomas² ; Barbara Thorand¹² ; Nicholas J. Timpson⁵³ ; Sam Tischfield⁴⁴ ; Martin Tobin³² ; Maciej Tomaszweski¹⁵ ; ⁸⁶ ; W.M. Monique Verschuren²⁸ ; Chris Wallace⁹⁷ ; Bernhard Winkelmann⁹³ ; Haitao Zhang² ; Dongling Zheng⁴⁶ ; Li Zhang¹⁴ ; Joseph M. Zmuda³⁷ ; Robert Clarke¹⁰⁷ ; Anthony J. Balmforth²³ ; John Danesh⁶⁵ ; Ian N. Day⁵³ ; Nicholas J. Schork³¹ ; Paul I.W. de Bakker⁶² ; ⁴⁴ ; ²¹ ; Christian Delles⁵⁴ ; David Duggan⁵⁹ ; Aroon D. Hingorani⁷ ; ⁷¹ ; Joel N. Hirschhorn⁴⁴ ; ⁷⁷ ; ⁷⁸ ; Marten H. Hofker⁶³ ; Steve E. Humphries²⁷ ; Mika Kivimaki⁷ ; Debbie A. Lawlor⁵³ ; Kandice Kottke-Marchant¹⁰⁰ ; Jessica L. Mega⁶⁰ ; Braxton D. Mitchell¹¹ ; David A. Morrow⁶⁰ ; Jutta Palmen²⁷ ; Susan Redline⁴¹ ; Denis C. Shields⁵⁷ ; Alan R. Shuldiner¹¹ ; ⁸⁰ ; Patrick M. Sleiman² ; George Davey Smith⁵³ ; Martin Farrall⁸ ; ⁷² ; Yalda Jamshidi⁴⁶ ; David C. Christiani²⁵ ; ⁸¹ ; Juan P. Casas¹¹⁰ ; Alistair S. Hall²³ ; Pieter A. Doevendans¹⁸ ; Jason D. Christie³⁶ ; Gerald S. Berenson¹⁰⁵ ; Sarah S. Murray³¹ ; Thomas Illig¹² ; Gerald W. Dorn II⁸⁵ ; Thomas P. Cappola⁵⁰ ; Eric Boerwinkle⁶⁸ ; Peter Sever¹⁰¹ ; Daniel J. Rader²⁹ ; ⁷⁴ ; Muredach P. Reilly²⁹ ; ⁷⁴ ; Mark Caulfield⁹ ; Philippa J. Talmud²⁷ ; Eric Topol⁹⁸ ; James C. Engert⁶⁷ ; Kai Wang² ; Anna Dominiczak⁵⁶ ; Anders Hamsten¹⁰⁶ ; Sean P. Curtis¹¹³ ; Roy L. Silverstein⁶¹ ; Leslie A. Lange⁴⁰ ; Marc S. Sabatine⁶⁰ ; Mieke Trip²⁶ ; Danish Saleheen⁶⁵ ; ⁶⁶ ; John F. Peden⁸ ; ⁷² ; Karen J. Cruickshanks¹⁷ ; ⁷⁹ ; Winfried Mä ; rz⁸⁹ ; ⁹⁰ ; ⁹¹ ; Jeffrey R. O'Connell¹¹ ; Olaf H. Klungel¹⁰⁸ ; Cisca Wijmenga⁶⁹ ; Anke Hilse Maitland-van der Zee¹⁰⁸ ; Eric E. Schadt⁸⁴ ; Julie A. Johnson⁶⁴ ; Gail P. Jarvik¹⁰ ; George J. Papanicolaou⁷⁰ ; Hugh Watkins on behalf of PROCARDIS⁷² ; Struan F.A. Grant² ; ⁷⁵ ; Patricia B. Munroe⁹ ; Kari E. North¹³ ; ⁷⁶ ; Nilesh J. Samani¹⁵ ; ⁸⁶ ; Wolfgang Koenig¹⁰³ ; Tom R. Gaunt⁵³ ; Sonia S. Anand⁷³ ; Yvonne T. van der Schouw¹⁰⁴ ; Meena Kumari on behalf of the Whitehall II Study ; the WHII 50K Group⁷ ; Nicole Soranzo⁴ ; Garret A. FitzGerald⁷⁴ ; Alex Reiner¹⁹ ; Robert A. Hegele¹ ; Hakon Hakonarson² ; ⁷⁵ ; ^{hakonarson@chop.edu} ; Brendan J. Keating²⁹ ; ⁷⁴ ; ¹¹⁴ ; ^{bkeating@chop.edu}
• 刊名：The American Journal of Human Genetics
• 出版年：2011
• 出版时间：7 January 2011
• 年：2011
• 卷：88
• 期：1
• 页码：6-18
• 全文大小：319 K

文摘

Height is a classic complex trait with common variants in a growing list of genes known to contribute to the phenotype. Using a genecentric genotyping array targeted toward cardiovascular-related loci, comprising 49,320 SNPs across approximately 2000 loci, we evaluated the association of common and uncommon SNPs with adult height in 114,223 individuals from 47 studies and six ethnicities. A total of 64 loci contained a SNP associated with height at array-wide significance (p < 2.4 × 10⁻⁶), with 42 loci surpassing the conventional genome-wide significance threshold (p < 5 × 10⁻⁸). Common variants with minor allele frequencies greater than 5 % were observed to be associated with height in 37 previously reported loci. In individuals of European ancestry, uncommon SNPs in IL11 and SMAD3, which would not be genotyped with the use of standard genome-wide genotyping arrays, were strongly associated with height (p < 3 × 10⁻¹¹). Conditional analysis within associated regions revealed five additional variants associated with height independent of lead SNPs within the locus, suggesting allelic heterogeneity. Although underpowered to replicate findings from individuals of European ancestry, the direction of effect of associated variants was largely consistent in African American, South Asian, and Hispanic populations. Overall, we show that dense coverage of genes for uncommon SNPs, coupled with large-scale meta-analysis, can successfully identify additional variants associated with a common complex trait.