Authors: Zhu, Gu¹; Evans, David M.¹; Duffy, David L.¹; Montgomery, Grant W.¹; Medland, Sarah E.¹; Gillespie, Nathan A.¹; Ewen, Kelly R.²; Jewell, Mary³; Liew, Yew Wah⁴; Hayward, Nicholas K.¹; Sturm, Richard A.⁵; Trent, Jeffrey M.⁶; Martin, Nicholas G.¹

Source: Twin Research, Volume 7, Number 2, 1 April 2004 , pp. 197-210(14)

Publisher: Australian Academic Press

Abstract:

We have rated eye color on a 3-point scale (1 = blue/grey, 2 = hazel/green, 3 = brown) in 502 twin families and carried out a 5-10 cM genome scan (400-757 markers). We analyzed eye color as a threshold trait and performed multipoint sib pair linkage analysis using variance components analysis in Mx. A lod of 19.2 was found at the marker D15S1002, less than 1 cM from OCA2, which has been previously implicated in eye color variation. We estimate that 74% of variance in eye color liability is due to this QTL and a further 18% due to polygenic effects. However, a large shoulder on this peak suggests that other loci affecting eye color may be telomeric of OCA2 and inflating the QTL estimate. No other peaks reached genome-wide significance, although lods > 2 were seen on 5p and 14q and lods >1 were additionally seen on chromosomes 2, 3, 6, 7, 8, 9, 17 and 18. Most of these secondary peaks were reduced or eliminated when we repeated the scan as a two locus analysis with the 15q linkage included, although this does not necessarily exclude them as false positives. We also estimated the interaction between the 15q QTL and the other marker locus but there was only minor evidence for additive × additive epistasis. Elaborating the analysis to the full two-locus model including non-additive main effects and interactions did not strengthen the evidence for epistasis. We conclude that most variation in eye color in Europeans is due to polymorphism in OCA2 but that there may be modifiers at several other loci.

Document Type: Research article

DOI: 10.1375/136905204323016186

Affiliations: 1: Queensland Institute of Medical Research, Brisbane 2: Australian Genome Research Facility, Melbourne 3: Center for Inherited Disease Research, Baltimore 4: Australian Red Cross Blood Service, Brisbane 5: Institute for Molecular Bioscience, University of Queensland, Brisbane 6: National Cancer Institute, Bethesda, and Translational Genomics Research Institute, Phoenix

Share this item with others: These icons link to social bookmarking sites where readers can share and discover new web pages.

• Website © 2009 Ingenta. Article copyright remains with the publisher, society or author(s) as specified within the article.
• Terms and Conditions
• Privacy Policy
• Information for advertisers

Click here for Page Help

Browse

Search

Electronic content Journal or book title

 

• Search history

Shopping cart

Tools

• Print
• Article access options
• Export
  • EndNote
  • BibT_EX
• Linking
  • IngentaConnect
  • OpenURL
  • DOI
• Alerting Options
  • Receive New Issue Alert
  • Latest TOC RSS Feed
  • Recent Issues RSS Feed
• Bookmark
  • Marked List
  • Add to Marked List
  • Social Bookmarking Links

Sign in

Text size: A | A | A | A