Rosacea is a common, chronic skin disease of variable severity with limited treatment options. The cause of rosacea is unknown, but it is believed to be due to a combination of hereditary and environm Show more
Rosacea is a common, chronic skin disease of variable severity with limited treatment options. The cause of rosacea is unknown, but it is believed to be due to a combination of hereditary and environmental factors. Little is known about the genetics of the disease. We performed a genome-wide association study (GWAS) of rosacea symptom severity with data from 73โ265 research participants of European ancestry from the 23andMe customer base. Seven loci had variants associated with rosacea at the genome-wide significance level (Pโ<โ5โรโ10-8). Further analyses highlighted likely gene regions or effector genes including IRF4 (Pโ=โ1.5โรโ10-17), a human leukocyte antigen (HLA) region flanked by PSMB9 and HLA-DMB (Pโ=โ2.2โรโ10-15), HERC2-OCA2 (Pโ=โ4.2โรโ10-12), SLC45A2 (Pโ=โ1.7โรโ10-10), IL13 (Pโ=โ2.8โรโ10-9), a region flanked by NRXN3 and DIO2 (Pโ=โ4.1โรโ10-9), and a region flanked by OVOL1and SNX32 (Pโ=โ1.2โรโ10-8). All associations with rosacea were novel except for the HLA locus. Two of these loci (HERC-OCA2 and SLC45A2) and another precedented variant (rs1805007 in melanocortin 1 receptor) with an association P value just below the significance threshold (Pโ=โ1.3โรโ10-7) have been previously associated with skin phenotypes and pigmentation, two of these loci are linked to immuno-inflammation phenotypes (IL13 and PSMB9-HLA-DMA) and one has been associated with both categories (IRF4). Genes within three loci (PSMB9-HLA-DMA, HERC-OCA2 and NRX3-DIO2) were differentially expressed in a previously published clinical rosacea transcriptomics study that compared lesional to non-lesional samples. The identified loci provide specificity of inflammatory mechanisms in rosacea, and identify potential pathways for therapeutic intervention. Show less