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Association of psoriasis to PGLYRP and SPRR genes at PSORS4 locus on 1q shows heterogeneity between Finnish, Swedish and Irish families. | LitMetric

AI Article Synopsis

  • - The PSORS4 susceptibility locus for psoriasis is located on chromosome 1q21, centered around the loricrin (LOR) gene, but no direct link between LOR gene polymorphisms and psoriasis has been found.
  • - Researchers focused on three gene clusters (S100, SPRR, and PGLYRP) in the region, as they contain genes previously implicated in psoriasis, with some showing altered expression and associations in past studies.
  • - A significant association was found with a specific five-SNP haplotype in PGLYRP among Finnish families, and findings were further supported by studies in Swedish and Irish families, indicating potential allelic diversity in the associations.

Article Abstract

A susceptibility locus for psoriasis, PSORS4, has been mapped to chromosome 1q21 in the region of the epidermal differentiation complex. The region has been refined to a 115 kb interval around the loricrin (LOR) gene. However, no evidence of association between polymorphisms in the LOR gene and psoriasis has been found. Therefore, we have analysed association to three candidate gene clusters of the region, the S100, small proline-rich protein (SPRR) and PGLYRP (peptidoglycan recognition protein) genes, which all contain functionally interesting psoriasis candidate genes. In previous studies, the SPRR and S100 genes have shown altered expression in psoriasis. Also polymorphisms in the PGLYRP genes have shown to be associated with psoriasis. We genotyped altogether 29 single nucleotide polymorphisms (SNPs) in 255 Finnish psoriasis families and analysed association with psoriasis using transmission disequilibrium test. A five-SNP haplotype of PGLYRP SNPs associated significantly with psoriasis. There was also suggestive evidence of association to SPRR gene locus in Finnish families. To confirm the putative associations, selected SNPs were genotyped also in a family collection of Swedish and Irish patients. The families supported association to the two gene regions, but there was also evidence of allelic heterogeneity.

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Source
http://dx.doi.org/10.1111/j.1600-0625.2008.00769.xDOI Listing

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