% pubman genre = article @article{item_3477250, title = {{A genome-wide association study identifies novel gene associations with facial skin wrinkling and mole count in Latin Americans}}, author = {Chen, Y. and Andr{\'e}, M. and Adhikari, K. and Blin, M. and Bonfante, B. and Mendoza-Revilla, J. and Fuentes-Guajardo, M. and Palmal, S. and Chac{\'o}n-Duque, J.C. and Hurtado, M. and Villegas, V. and Granja, V. and Jaramillo, C. and Arias, W. and Barquera Lozano, Rodrigo Jos{\'e} and Everardo-Mart{\'\i}nez, P. and G{\'o}mez-Vald{\'e}s, J. and Villamil-Ram{\'\i}rez, H. and de Cerqueira, C.C.S. and H{\"u}nemeier, T. and Ramallo, V. and Gonzalez-Jos{\'e}, R. and Sch{\"u}ler-Faccini, L. and Bortolini, M.-C. and Acu{\~n}a-Alonzo, V. and Canizales-Quinteros, S. and Gallo, C. and Poletti, G. and Bedoya, G. and Rothhammer, F. and Balding, D. and Tobin, D.J. and Wang, S. and Faux, P. and Ruiz-Linares, A.}, language = {eng}, issn = {0007-0963}, doi = {10.1111/bjd.20436}, publisher = {Published for the British Association of Dermatologists by Blackwell Scientific Publications [etc.]}, address = {Oxford [etc.]}, year = {2021}, date = {2021-11}, abstract = {{Background: Genome-wide association studies (GWASs) have identified genes influencing skin ageing and mole count in Europeans, but little is known about the relevance of these (or other genes) in non-Europeans. - {\textless}br{\textgreater}Objectives: To conduct a GWAS for facial skin ageing and mole count in adults {\textless} 40 years old, of mixed European, Native American and African ancestry, recruited in Latin America. - {\textless}br{\textgreater}Methods: Skin ageing and mole count scores were obtained from facial photographs of over 6000 individuals. After quality control checks, three wrinkling traits and mole count were retained for genetic analyses. DNA samples were genotyped with Illumina{\textquoteright}s HumanOmniExpress chip. Association testing was performed on around 8 703 729 single-nucleotide polymorphisms (SNPs) across the autosomal genome. -{\textless}br{\textgreater}Results: Genome-wide significant association was observed at four genome regions: two were associated with wrinkling (in 1p13{\mbox{$\cdot$}}3 and 21q21{\mbox{$\cdot$}}2), one with mole count (in 1q32{\mbox{$\cdot$}}3) and one with both wrinkling and mole count (in 5p13{\mbox{$\cdot$}}2). Associated SNPs in 5p13{\mbox{$\cdot$}}2 and in 1p13{\mbox{$\cdot$}}3 are intronic within SLC45A2 and VAV3, respectively, while SNPs in 1q32{\mbox{$\cdot$}}3 are near the SLC30A1 gene, and those in 21q21{\mbox{$\cdot$}}2 occur in a gene desert. Analyses of SNPs in IRF4 and MC1R are consistent with a role of these genes in skin ageing. - {\textless}br{\textgreater}Conclusions: We replicate the association of wrinkling with variants in SLC45A2, IRF4 and MC1R reported in Europeans. We identify VAV3 and SLC30A1 as two novel candidate genes impacting on wrinkling and mole count, respectively. We provide the first evidence that SLC45A2 influences mole count, in addition to variants in this gene affecting melanoma risk in Europeans.{\textless}br{\textgreater}}}, contents = {Patients and methods - Study participants - Phenotyping - DNA genotyping - Statistical genetics analyses Results - Traits examined - Genome-wide association analyses - Evaluation of MC1R and IRF4 variants associated with skin ageing in Europeans Discussion}, journal = {{British Journal of Dermatology}}, volume = {185}, number = {5}, pages = {988--998}, eid = {20436}, }