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   Thrombin Cleavage of Osteopontin Modulates Its Activities in Human Cells in Vitro and Mouse Experimental Autoimmune Encephalomyelitis in Vivo  
   
نویسنده boggio e. ,dianzani c. ,gigliotti c.l. ,soluri m.f. ,clemente n. ,cappellano g. ,toth e. ,raineri d. ,ferrara b. ,comi c. ,dianzani u. ,chiocchetti a.
منبع journal of immunology research - 2016 - دوره : 2016 - شماره : 0
چکیده    Osteopontin is a proinflammatory cytokine and plays a pathogenetic role in multiple sclerosis and its animal model,experimental autoimmune encephalomyelitis (eae),by recruiting autoreactive t cells into the central nervous system. osteopontin functions are modulated by thrombin cleavage generating n- and c-terminal fragment,whose individual roles are only partly known. published data are difficult to compare since they have been obtained with heterogeneous approaches. interestingly,thrombin cleavage of osteopontin unmasks a cryptic domain of interaction with α 4 β 1 integrin that is the main adhesion molecule involved in lymphocyte transmigration to the brain and is the target for natalizumab,the most potent drug preventing relapses. we produced recombinant osteopontin and its n- and c-terminal fragments in an eukaryotic system in order to allow their posttranslational modifications. we investigated,in vitro,their effect on human cells and in vivo in eae. we found that the osteopontin cleavage plays a key role in the function of this cytokine and that the two fragments exert distinct effects both in vitro and in vivo. these findings suggest that drugs targeting each fragment may be used to fine-tune the pathological effects of osteopontin in several diseases. © 2016 elena boggio et al.
آدرس department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of drug science and technology,university of torino,torino, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, biocenter,division for experimental pathophysiology and immunology,laboratory of autoimmunity,medical university of innsbruck,innsbruck, Austria, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of drug science and technology,university of torino,torino, Italy, department of translational medicine,neurology unit,a. avogadro upo,novara, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy, department of health sciences,interdisciplinary research center of autoimmune diseases (ircad),a. avogadro university of piemonte orientale (upo),novara, Italy
 
     
   
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