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Meta-Analysis of Genome-Wide Scans for Human Adult Stature Identifies Novel Loci and Associations with Measures of Skeletal Frame Size

Author

Listed:
  • Nicole Soranzo
  • Fernando Rivadeneira
  • Usha Chinappen-Horsley
  • Ida Malkina
  • J Brent Richards
  • Naomi Hammond
  • Lisette Stolk
  • Alexandra Nica
  • Michael Inouye
  • Albert Hofman
  • Jonathan Stephens
  • Eleanor Wheeler
  • Pascal Arp
  • Rhian Gwilliam
  • P Mila Jhamai
  • Simon Potter
  • Amy Chaney
  • Mohammed J R Ghori
  • Radhi Ravindrarajah
  • Sergey Ermakov
  • Karol Estrada
  • Huibert A P Pols
  • Frances M Williams
  • Wendy L McArdle
  • Joyce B van Meurs
  • Ruth J F Loos
  • Emmanouil T Dermitzakis
  • Kourosh R Ahmadi
  • Deborah J Hart
  • Willem H Ouwehand
  • Nicholas J Wareham
  • Inês Barroso
  • Manjinder S Sandhu
  • David P Strachan
  • Gregory Livshits
  • Timothy D Spector
  • André G Uitterlinden
  • Panos Deloukas

Abstract

Recent genome-wide (GW) scans have identified several independent loci affecting human stature, but their contribution through the different skeletal components of height is still poorly understood. We carried out a genome-wide scan in 12,611 participants, followed by replication in an additional 7,187 individuals, and identified 17 genomic regions with GW-significant association with height. Of these, two are entirely novel (rs11809207 in CATSPER4, combined P-value = 6.1×10−8 and rs910316 in TMED10, P-value = 1.4×10−7) and two had previously been described with weak statistical support (rs10472828 in NPR3, P-value = 3×10−7 and rs849141 in JAZF1, P-value = 3.2×10−11). One locus (rs1182188 at GNA12) identifies the first height eQTL. We also assessed the contribution of height loci to the upper- (trunk) and lower-body (hip axis and femur) skeletal components of height. We find evidence for several loci associated with trunk length (including rs6570507 in GPR126, P-value = 4×10−5 and rs6817306 in LCORL, P-value = 4×10−4), hip axis length (including rs6830062 at LCORL, P-value = 4.8×10−4 and rs4911494 at UQCC, P-value = 1.9×10−4), and femur length (including rs710841 at PRKG2, P-value = 2.4×10−5 and rs10946808 at HIST1H1D, P-value = 6.4×10−6). Finally, we used conditional analyses to explore a possible differential contribution of the height loci to these different skeletal size measurements. In addition to validating four novel loci controlling adult stature, our study represents the first effort to assess the contribution of genetic loci to three skeletal components of height. Further statistical tests in larger numbers of individuals will be required to verify if the height loci affect height preferentially through these subcomponents of height.Author Summary: The first genetic association studies of adult height have confirmed a role of many common variants in influencing human height, but to date, the genetic basis of differences between different skeletal components of height have not been addressed. Here, we take advantage of recent technical and methodological advances to examine the role of common genetic variants on both height and skeletal components of height. By examining nearly 20,000 individuals from the UK and the Netherlands, we provide statistically significant evidence that 17 genomic regions are associated with height, including four novel regions. We also examine, for the first time, the association of these 17 regions with skeletal size measurements of spine, femur, and hip axis length, a measurement of hip geometry known to influence the risk of osteoporotic fractures. We find that some height loci are also associated with these skeletal components, although further statistical tests will be required to verify if these genetic variants act differentially on the individual skeletal measurements. The knowledge generated by this and other studies will not only inform the genetics of human quantitative variation, but will also lead to the potential discovery of many medically important polymorphisms.

Suggested Citation

  • Nicole Soranzo & Fernando Rivadeneira & Usha Chinappen-Horsley & Ida Malkina & J Brent Richards & Naomi Hammond & Lisette Stolk & Alexandra Nica & Michael Inouye & Albert Hofman & Jonathan Stephens & , 2009. "Meta-Analysis of Genome-Wide Scans for Human Adult Stature Identifies Novel Loci and Associations with Measures of Skeletal Frame Size," PLOS Genetics, Public Library of Science, vol. 5(4), pages 1-13, April.
    • Handle: RePEc:plo:pgen00:1000445
    DOI: 10.1371/journal.pgen.1000445
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    Cited by:

    1. Akachi, Yoko & Canning, David, 2015. "Inferring the economic standard of living and health from cohort height: Evidence from modern populations in developing countries," Economics & Human Biology, Elsevier, vol. 19(C), pages 114-128.
    2. Josine L Min & Jennifer M Taylor & J Brent Richards & Tim Watts & Fredrik H Pettersson & John Broxholme & Kourosh R Ahmadi & Gabriela L Surdulescu & Ernesto Lowy & Christian Gieger & Chris Newton-Cheh, 2011. "The Use of Genome-Wide eQTL Associations in Lymphoblastoid Cell Lines to Identify Novel Genetic Pathways Involved in Complex Traits," PLOS ONE, Public Library of Science, vol. 6(7), pages 1-14, July.
    3. McEvoy, Brian P. & Visscher, Peter M., 2009. "Genetics of human height," Economics & Human Biology, Elsevier, vol. 7(3), pages 294-306, December.
    4. Alexander P Reiner & Guillaume Lettre & Michael A Nalls & Santhi K Ganesh & Rasika Mathias & Melissa A Austin & Eric Dean & Sampath Arepalli & Angela Britton & Zhao Chen & David Couper & J David Curb , 2011. "Genome-Wide Association Study of White Blood Cell Count in 16,388 African Americans: the Continental Origins and Genetic Epidemiology Network (COGENT)," PLOS Genetics, Public Library of Science, vol. 7(6), pages 1-14, June.

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