[No authors listed]
Psoriasis is a chronic inflammatory skin disease. Keratinocytes (KCs), as skinâspecific cells, serve an important role in the immunopathogenesis of psoriasis. In the present study, transcriptome data derived from psoriasisâlike KCs were used together with the reported transcriptome data from the skin/epidermis of patient with psoriasis, excluding known psoriasisâassociated genes that have been well described in the previous studies according to GeneCards database, to screen for novel psoriasisâassociated genes. According to the human expressed sequence tag of UniGene dataset, six genes that are located near psoriasisâassociated loci were highly expressed in skin. Among these six genes, four genes (epiregulin, NIPA like domain containing 4, serpin family B member 7 and WAP fourâdisulfide core domain 12) were highly expressed in normal mouse epidermis (mainly KCs) and mouse psoriatic epidermis cells, but not in psoriatic dermis cells, which further emphasized the specificity of these genes. Furthermore, in systemic inflammatory response syndrome (SIRS), SERPINB7 showed no difference in expression in immuneâactivated tissues from SIRS and control mice. It was also found that the mRNA expression levels of SERPINB in lesional skin of patients with psoriasis were significantly higher than in nonâlesional psoriatic skin from the same patients. SERPINB7 may be a valuable candidate for further studies. In the present study, a method for identifying novel key pathogenic skinâspecific molecules is presented, which may be used for investigating and treating psoriasis.
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