Publikation

Defining the role of common variation in the genomic and biological architecture of adult human height

Wissenschaftlicher Artikel/Review - 05.10.2014

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PubMed
DOI

Zitation
Jousilahti P, Lakka T, Langenberg C, Le Marchand L, Lehtimäki T, Lupoli S, Madden P, Männistö S, Manunta P, Marette A, Matise T, McKnight B, Kuusisto J, Kumari M, Kraja A, Jula A, Kaprio J, Kastelein J, Kayser M, Kee F, Keinanen-Kiukaanniemi S, Kiemeney L, Kooner J, Kooperberg C, Koskinen S, Kovacs P, Meitinger T, Moll F, Montgomery G, Rankinen T, Rao D, Rice T, Ritchie M, Rudan I, Salomaa V, Samani N, Saramies J, Sarzynski M, Schwarz P, Sebert S, Raitakari O, Qi L, Price J, Morris A, Morris A, Murray J, Nelis M, Ohlsson C, Oldehinkel A, Ong K, Ouwehand W, Pasterkamp G, Peters A, Pramstaller P, Sever P, Jarvelin M, Wright A, Caulfield M, Chakravarti A, Collins R, Collins F, Crawford D, Cupples L, Danesh J, de Faire U, den Ruijter H, Erbel R, Erdmann J, Campbell H, Brown M, Brambilla P, Zhang Q, Arveiler D, Bakker S, Beilby J, Bergman R, Bergmann S, Biffar R, Blangero J, Boomsma D, Bornstein S, Bovet P, Eriksson J, Farrall M, Ferrannini E, Hattersley A, Heath A, Hengstenberg C, Hicks A, Hindorff L, Hingorani A, Hofman A, Hovingh G, Humphries S, Hunt S, Hyppönen E, Harris T, Hall A, Haas D, Ferrieres J, Ford I, Forouhi N, Forrester T, Gansevoort R, Gejman P, Gieger C, Golay A, Gottesman O, Gudnason V, Gyllensten U, Jacobs K, Shuldiner A, Reinmaa E, Völzke H, Walker M, Wareham N, Watkins H, Wichmann H, Wilson J, Zanen P, Deloukas P, Heid I, Lindgren C, Mohlke K, van der Harst P, Uusitupa M, Tuomilehto J, Ridker P, Rivadeneira F, Rotter J, Saaristo T, Saleheen D, Schlessinger D, Slagboom P, Snieder H, Spector T, Strauch K, Stumvoll M, Speliotes E, Thorsteinsdottir U, Barroso I, Price A, Lettre G, Loos R, Weedon M, Ingelsson E, O'Connell J, Abecasis G, Chasman D, Goddard M, Visscher P, Hirschhorn J, Willer C, Franke L, van Duijn C, Fox C, North K, Strachan D, Beckmann J, Berndt S, Boehnke M, Borecki I, McCarthy M, Metspalu A, Stefansson K, Uitterlinden A, Frayling T, Rauramaa R, Sinisalo J, Boerwinkle E, Bottinger E, Bouchard C, Cauchi S, Chambers J, Chanock S, Cooper R, de Bakker P, Dedoussis G, Ferrucci L, Franks P, Boehm B, Bochud M, Assimes T, Steinthorsdottir V, Stolk R, Tardif J, Tönjes A, Tremblay A, Tremoli E, Virtamo J, Vohl M, Amouyel P, Asselbergs F, Froguel P, Groop L, Haiman C, Moebus S, Munroe P, Njølstad I, Oostra B, Palmer C, Pedersen N, Perola M, Pérusse L, Peters U, Powell J, Power C, Melbye M, März W, Martin N, Hamsten A, Hayes M, Hui J, Hunter D, Hveem K, Jukema J, Kaplan R, Kivimäki M, Kuh D, Laakso M, Liu Y, Quertermous T, Nyholt D, van Setten J, van Vliet-Ostaptchouk J, Wang Z, Yengo L, Zhang W, Afzal U, Arnlöv J, Arscott G, Bandinelli S, Barrett A, Bellis C, van der Laan S, Trompet S, Teumer A, Palmer C, Pasko D, Pechlivanis S, Prokopenko I, Ried J, Ripke S, Shungin D, Stančáková A, Strawbridge R, Sung Y, Tanaka T, Bennett A, Berne C, Blüher M, Delgado G, Denny J, Dhonukshe-Rutten R, Dimitriou M, Doney A, Dörr M, Eklund N, Eury E, Folkersen L, Garcia M, Geller F, Deelen J, De Jong P, Daw E, Bolton J, Böttcher Y, Boyd H, Bruinenberg M, Buckley B, Buyske S, Caspersen I, Chines P, Clarke R, Claudi-Boehm S, Cooper M, Giedraitis V, Nalls M, Wood A, Fall T, Fehrmann R, Ferreira T, Jackson A, Karjalainen J, Lo K, Locke A, Mägi R, Mihailov E, Porcu E, Randall J, Duan Y, Day F, Croteau-Chonka D, Esko T, Yang J, Vedantam S, Pers T, Gustafsson S, Chu A, Estrada K, Luan J, Kutalik Z, Amin N, Buchkovich M, Scherag A, Vinkhuyzen A, Westra H, Goel A, Gong J, Justice A, Kanoni S, Kleber M, Kristiansson K, Lim U, Lotay V, Lui J, Mangino M, Mateo Leach I, Fraser R, Fischer K, Feitosa M, Winkler T, Workalemahu T, Zhao J, Absher D, Albrecht E, Anderson D, Baron J, Beekman M, Demirkan A, Ehret G, Feenstra B, Medina-Gomez C, Go A, Monda K, Roussel R, Sanna S, Scharnagl H, Scholtens S, Schumacher F, Schunkert H, Scott R, Sehmi J, Seufferlein T, Shi J, Silventoinen K, Rose L, Robertson N, Renström F, Morken M, Müller G, Müller-Nurasyid M, Musk A, Narisu N, Nauck M, Nolte I, Nöthen M, Oozageer L, Pilz S, Rayner N, Smit J, Smith A, Smolonska J, van Oort F, Vermeulen S, Verweij N, Vonk J, Waite L, Waldenberger M, Wennauer R, Wilkens L, Willenborg C, Wilsgaard T, Wojczynski M, van Heemst D, van der Velde N, van Schoor N, Stanton A, Stirrups K, Stott D, Stringham H, Sundstrom J, Swertz M, Syvänen A, Tayo B, Thorleifsson G, Tyrer J, van Dijk S, Wong A, Moayyeri A, Grallert H, Helmer Q, Hemani G, Henders A, Hillege H, Hlatky M, Hoffmann W, Hoffmann P, Holmen O, Houwing-Duistermaat J, Illig T, Isaacs A, Heard-Costa N, Hayward C, Hassinen M, Grammer T, Gräßler J, Grönberg H, de Groot L, Groves C, Haessler J, Hall P, Haller T, Hallmans G, Hannemann A, Hartman C, James A, Jeff J, Johansen B, Lu Y, Lyssenko V, Magnusson P, Mahajan A, Maillard M, McArdle W, McKenzie C, McLachlan S, McLaren P, Menni C, Merger S, Lorentzon M, Lobbens S, Lindström J, Johansson Å, Jolley J, Juliusdottir T, Junttila J, Kho A, Kinnunen L, Klopp N, Kocher T, Kratzer W, Lichtner P, Lind L, Milani L. Defining the role of common variation in the genomic and biological architecture of adult human height. Nat Genet 2014; 46:1173-86.
Art
Wissenschaftlicher Artikel/Review (Englisch)
Zeitschrift
Nat Genet 2014; 46
Veröffentlichungsdatum
05.10.2014
eISSN (Online)
1546-1718
Seiten
1173-86
Kurzbeschreibung/Zielsetzung

Using genome-wide data from 253,288 individuals, we identified 697 variants at genome-wide significance that together explained one-fifth of the heritability for adult height. By testing different numbers of variants in independent studies, we show that the most strongly associated ∼2,000, ∼3,700 and ∼9,500 SNPs explained ∼21%, ∼24% and ∼29% of phenotypic variance. Furthermore, all common variants together captured 60% of heritability. The 697 variants clustered in 423 loci were enriched for genes, pathways and tissue types known to be involved in growth and together implicated genes and pathways not highlighted in earlier efforts, such as signaling by fibroblast growth factors, WNT/β-catenin and chondroitin sulfate-related genes. We identified several genes and pathways not previously connected with human skeletal growth, including mTOR, osteoglycin and binding of hyaluronic acid. Our results indicate a genetic architecture for human height that is characterized by a very large but finite number (thousands) of causal variants.