Genome-wide search for nevus density shows linkage to two melanoma loci on chromosome 9 and identifies a new QTL on 5q31 in an adult twin cohort

doi:10.1093/hmg/ddl227

Human Molecular Genetics Advance Access originally published online on August 23, 2006
Human Molecular Genetics 2006 15(20):2975-2979; doi:10.1093/hmg/ddl227

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Genome-wide search for nevus density shows linkage to two melanoma loci on chromosome 9 and identifies a new QTL on 5q31 in an adult twin cohort

Mario Falchi¹, Tim D. Spector¹, Ursula Perks¹, Bernet S. Kato¹ and Veronique Bataille¹^,2^,*

¹ Twin Research and Genetic Epidemiology Unit, St Thomas' Campus, Kings College London, London SE1 7EH, UK and ² Dermatology Department, West Herts NHS Trust, Hemel Hempstead General Hospital, Hillfield Road, Herts HP2 4AD, UK

^* To whom correspondence should be addressed at: Twin Research and Genetic Epidemiology Unit, St Thomas' Campus, Kings College London, Lambeth Palace Road, London SE1 7EH, UK. Tel: +44 2071886765; Fax: +44 2071886718; Email: bataille{at}doctors.org.uk

Received July 12, 2006; Accepted August 8, 2006

The density of acquired melanocytic nevi represents an importantrisk factor for malignant melanoma. Total body nevus countswere collected in a cross-sectional study of 1730 healthy femalesfrom the UK Adult twin registry comprising 709 dizygous and156 monozygous pairs. Nevus density (ND) increased up to theage of 35 years and then gradually declined. Quantitative geneticanalysis showed a smaller genetic influence (36%) on ND up to35 years, compared with after 35 years where it rose to 59%.Using a sub-sample of 1238 genotyped individuals, we performeddistinct genome-wide scans for individuals above and below 35separately. In the younger sub-sample, we confirmed a quantitativetrait locus (QTL) for ND on chromosomes 9p21 (LOD=2.54), a regionalready linked to both familial melanoma and ND. We also observeda linkage signal on 9q21 (LOD=2.55) overlapping a recently reportedsusceptibility locus for ocular and cutaneous melanoma in Danishfamilies. The strongest evidence of linkage identified a novelQTL on chromosome 5q31–32 (LOD=3.47). None of these linkageswas observed in the group aged 35 years and over, which showedsuggestive linkage on chromosome 2p24 (LOD=2.75). To the bestof our knowledge, this is the first genome-wide search for NDin a large sample of healthy adults. The results suggest thatdifferent sets of genes are likely to influence the processesleading to the appearance of nevi and their involution. Theyprovide both novel and replicated QTLs for nevus development,some of which might overlap with those for melanoma and warrantdetailed investigation.

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