[No authors listed]
Psoriasis vulgaris (PsV) is a common, chronic skin disease with a complex genetic and environmental etiology. We investigated, in 461 psoriatic patients and 454 healthy controls, the associations with psoriasis of four single-nucleotide polymorphisms (SNPs) from the psoriasis susceptibility 1 (PSORS1) interval: rs1062470 (PSORS1C1/CDSN), rs887466 (PSORS1C3), rs2894207 and rs10484554 (LOC105375015). The minor alleles of three SNPs (rs1062470A, rs2894207C and rs10484554T) strongly increased the disease risk (ORâ=â2.17, pâ<â0.0001; ORâ=â2.33, pâ<â0.0001 and ORâ=â2.68, pâ<â0.0001, respectively), whereas the minor A allele of rs887466 exerted a protective effect (ORâ=â0.73, pâ=â0.001). The strength of association for SNPs was the highest in patients with very early onset psoriasis (â¤â20 years), while in late onset psoriasis (>â40 years) the association was the weakest. The haplotype rs1062470A/rs887466G/rs2894207C/rs10484554T highly significantly increased the disease risk (ORâ=â3.58, pâ=â8.0e-027), while the haplotypes rs1062470G/rs887466A/rs2894207T/rs10484554C and rs1062470G/rs887466G/rs2894207T/rs10484554C were strongly protective (ORâ=â0.65, pâ=â0.002 and ORâ=â0.55, pâ=â2.4e-009, respectively). Additionally, we showed a HLA-C*06:02-independent gender-related effect of the rs887466A allele which was protective against psoriasis in males (ORâ=â0.61, pâ=â9.2e-005), but not in females (pâ=â0.66). We also demonstrated a correlation of PASI score value with rs1062470 genotype, and again only in male patients (pâ=â0.006) and HLA-C*06:02-independent. Our results show, for the first time, the male-only associations of the PSORS1C3 gene with psoriasis risk and of the PSORS1C1/CDSN gene with severity of disease. However, the age dependent associations need to be validated in larger sample sizes as well as in other populations.
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