The DNA methylation of MIR-203, AMD1 and bcap31 gene in psoriasis

Abstract

Psoriasis is a chronic inflammatory skin disease. Its characteristic features in the skin consist of inflammatory changes in both dermis and epidermis, with abnormal keratinocyte differentiation and proliferation. Dysfunctional apoptotic process occurs in psoriasis. There is a decrease apoptosis of lesional keratinocyte. DNA methylation is a major epigenetic modification, affects cell function by altering gene expression. DNA methylation of promoter region in CpG island, has shown to be associated with transcription silencing of the gene in normal development. Aberrant DNA methylation plays an important role in the development of autoimmune disease including psoriasis. Previous studies show that abnormal DNA methylation was found in many genes, such as SHP-1, P16INK4a, and p15 genes. This study aimed to analyze promoter methylation of mir-203, AMD1 and BCAP31 genes in patients with psoriasis compare to normal using combined bisulfite restriction analysis (COBRA), methylation specific PCR (MSP), and bisulfite sequencing, respectively. Then, the correlation between the promoter methylation and their expression level were investigated. We analyzed the methylation level of miR-203 in epidermis and AMD1 in epidermis and total leukocytes. There were no significant differences in methylation level of mir-203 and AMD1 in psoriasis, compared to normal controls. Our results suggest that, mir-203 and AMD1 mRNA expression in psoriasis is not controlled by mir-203 and AMD1 promoter methylation. Then, mRNA expression level and promoter methylation of BCAP31 genes in PBMCs were studied. Interestingly, The expression level of BCAP31 mRNA was significantly decrease and correlated with promoter hypermethylation in psoriasis group compared with healthy control. BCAP31, an ubiquitous ER membrane protein, has been implicated in the regulation of apoptosis in lymphocytes and epithelial cells. Thus, down-regulation of BCAP31 may increase potential to resist apoptosis of lymphocyte in psoriasis. This is the first report showed that hypermethylation of BCAP31 promoter contributes to down-regulation of mRNA expression in psoriasis.