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Crystal structure of the complex mAb 17.2 and the C-terminal region of Trypanosoma cruzi P2β protein: Implications in cross-reactivity
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نویسنده
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pizarro j.c. ,boulot g. ,bentley g.a. ,gómez k.a. ,hoebeke j. ,hontebeyrie m. ,levin m.j. ,smulski c.r.
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منبع
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plos neglected tropical diseases - 2011 - دوره : 5 - شماره : 11
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چکیده
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Patients with chronic chagas' heart disease possess high levels of antibodies against the carboxyl-terminal end of the ribosomal p2ß protein of trypanosoma cruzi (tcp2ß). these antibodies,as well as the murine monoclonal antibody (mab) 17.2,recognize the last 13 amino acids of tcp2ß (called the r13 epitope: eeedddmgfglfd) and are able to cross-react with,and stimulate,the ß1 adrenergic receptor (ß1-ar). indeed,the mab 17.2 was able to specifically detect human β1-ar,stably transfected into hek cells,by flow cytometry and to induce repolarisation abnormalities and first degree atrioventricular conduction block after passive transfer to naïve mice. to study the structural basis of this cross-reactivity,we determined the crystal structure of the fab region of the mab 17.2 alone at 2.31 å resolution and in complex with the r13 peptide at 1.89 å resolution. we identified as key contact residues on r13 peptide glu3,asp6 and phe9 as was previously shown by alanine scanning. additionally,we generated a model of human β1-ar to elucidate the interaction with anti-r13 antibodies. these data provide an understanding of the molecular basis of cross-reactive antibodies induced by chronic infection with trypanosoma cruzi. © 2011 pizarro et al.
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آدرس
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unité d'immunologie structurale,institut pasteur,paris,france,centre national de la recherche scientifique,unité de recherche associée 2185,paris,france,structural genomic consortium (sgc),university of toronto,toronto, Canada, unité d'immunologie structurale,institut pasteur,paris,france,centre national de la recherche scientifique,unité de recherche associée 2185,paris, France, unité d'immunologie structurale,institut pasteur,paris,france,centre national de la recherche scientifique,unité de recherche associée 2185,paris, France, laboratorio de biología molecular de la enfermedad de chagas,ingebi-conicet,buenos aires, Argentina, upr9021 du cnrs,strasbourg, France, institut pasteur,paris, France, laboratorio de biología molecular de la enfermedad de chagas,ingebi-conicet,buenos aires, Argentina, laboratorio de biología molecular de la enfermedad de chagas,ingebi-conicet,buenos aires,argentina,upr9021 du cnrs,strasbourg, France
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Authors
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