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   DNA methylation and gene expression changes in monozygotic twins discordant for psoriasis: Identification of epigenetically dysregulated genes  
   
نویسنده gervin k. ,vigeland m.d. ,mattingsdal m. ,hammerø m. ,nygård h. ,olsen a.o. ,brandt i. ,harris j.r. ,undlien d.e. ,lyle r.
منبع plos genetics - 2012 - دوره : 8 - شماره : 1
چکیده    Monozygotic (mz) twins do not show complete concordance for many complex diseases; for example,discordance rates for autoimmune diseases are 20%-80%. mz discordance indicates a role for epigenetic or environmental factors in disease. we used mz twins discordant for psoriasis to search for genome-wide differences in dna methylation and gene expression in cd4 + and cd8 + cells using illumina's humanmethylation27 and ht-12 expression assays,respectively. analysis of these data revealed no differentially methylated or expressed genes between co-twins when analyzed separately,although we observed a substantial amount of small differences. however,combined analysis of dna methylation and gene expression identified genes where differences in dna methylation between unaffected and affected twins were correlated with differences in gene expression. several of the top-ranked genes according to significance of the correlation in cd4 + cells are known to be associated with psoriasis. further,gene ontology (go) analysis revealed enrichment of biological processes associated with the immune response and clustering of genes in a biological pathway comprising cytokines and chemokines. these data suggest that dna methylation is involved in an epigenetic dysregulation of biological pathways involved in the pathogenesis of psoriasis. this is the first study based on data from mz twins discordant for psoriasis to detect epigenetic alterations that potentially contribute to development of the disease. © 2012 gervin et al.
آدرس department of medical genetics,oslo university hospital and university of oslo,oslo, Norway, department of medical genetics,oslo university hospital and university of oslo,oslo, Norway, research unit,sorlandet hospital,kristiansand,norway,institute of psychiatry,university of oslo,oslo, Norway, department of medical genetics,oslo university hospital and university of oslo,oslo, Norway, department of medical genetics,oslo university hospital and university of oslo,oslo, Norway, department of dermatology,oslo university hospital and university of oslo,oslo, Norway, division of epidemiology,norwegian institute of public health,oslo, Norway, division of epidemiology,norwegian institute of public health,oslo, Norway, department of medical genetics,oslo university hospital and university of oslo,oslo, Norway, department of medical genetics,oslo university hospital and university of oslo,oslo, Norway
 
     
   
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