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   Citrullination of Histone H3 Interferes with HP1-Mediated Transcriptional Repression  
   
نویسنده sharma p. ,azebi s. ,england p. ,christensen t. ,møller-larsen a. ,petersen t. ,batsché e. ,muchardt c.
منبع plos genetics - 2012 - دوره : 8 - شماره : 9
چکیده    Multiple sclerosis (ms) is an autoimmune disease associated with abnormal expression of a subset of cytokines,resulting in inappropriate t-lymphocyte activation and uncontrolled immune response. a key issue in the field is the need to understand why these cytokines are transcriptionally activated in the patients. here,we have examined several transcription units subject to pathological reactivation in ms,including the tnfα and il8 cytokine genes and also several human endogenous retroviruses (hervs). we find that both the immune genes and the hervs require the heterochromatin protein hp1α for their transcriptional repression. we further show that the peptidylarginine deiminase 4 (padi4),an enzyme with a suspected role in ms,weakens the binding of hp1α to tri-methylated histone h3 lysine 9 by citrullinating histone h3 arginine 8. the resulting de-repression of both cytokines and hervs can be reversed with the padi-inhibitor cl-amidine. finally,we show that in peripheral blood mononuclear cells (pbmcs) from ms patients,the promoters of tnfα,and several hervs share a deficit in hp1α recruitment and an augmented accumulation of histone h3 with a double citrulline 8 tri-methyl lysine 9 modifications. thus,our study provides compelling evidence that hp1α and padi4 are regulators of both immune genes and hervs,and that multiple events of transcriptional reactivation in ms patients can be explained by the deficiency of a single mechanism of gene silencing. © 2012 sharma et al.
آدرس institut pasteur,département de biologie du développement,cnrs ura2578,unité de régulation epigénétique,paris, France, institut pasteur,département de biologie du développement,cnrs ura2578,unité de régulation epigénétique,paris, France, institut pasteur,département de biologie structurale et chimie,cnrs umr3528,plate-forme de biophysique des macromolécules et de leurs interactions,paris, France, department of biomedicine,aarhus university,aarhus, Denmark, department of biomedicine,aarhus university,aarhus, Denmark, department of neurology,aarhus university hospital,aarhus, Denmark, institut pasteur,département de biologie du développement,cnrs ura2578,unité de régulation epigénétique,paris, France, institut pasteur,département de biologie du développement,cnrs ura2578,unité de régulation epigénétique,paris, France
 
     
   
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