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Neisseria meningitidis Type IV Pili Composed of Sequence Invariable Pilins Are Masked by Multisite Glycosylation
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نویسنده
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gault j. ,ferber m. ,machata s. ,imhaus a.-f. ,malosse c. ,charles-orszag a. ,millien c. ,bouvier g. ,bardiaux b. ,péhau-arnaudet g. ,klinge k. ,podglajen i. ,ploy m.c. ,seifert h.s. ,nilges m. ,chamot-rooke j. ,duménil g.
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منبع
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plos pathogens - 2015 - دوره : 11 - شماره : 9 - صفحه:1 -24
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چکیده
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The ability of pathogens to cause disease depends on their aptitude to escape the immune system. type iv pili are extracellular filamentous virulence factors composed of pilin monomers and frequently expressed by bacterial pathogens. as such they are major targets for the host immune system. in the human pathogen neisseria meningitidis,strains expressing class i pilins contain a genetic recombination system that promotes variation of the pilin sequence and is thought to aid immune escape. however,numerous hypervirulent clinical isolates express class ii pilins that lack this property. this raises the question of how they evade immunity targeting type iv pili. as glycosylation is a possible source of antigenic variation it was investigated using top-down mass spectrometry to provide the highest molecular precision on the modified proteins. unlike class i pilins that carry a single glycan,we found that class ii pilins display up to 5 glycosylation sites per monomer on the pilus surface. swapping of pilin class and genetic background shows that the pilin primary structure determines multisite glycosylation while the genetic background determines the nature of the glycans. absence of glycosylation in class ii pilins affects pilus biogenesis or enhances pilus-dependent aggregation in a strain specific fashion highlighting the extensive functional impact of multisite glycosylation. finally,molecular modeling shows that glycans cover the surface of class ii pilins and strongly decrease antibody access to the polypeptide chain. this strongly supports a model where strains expressing class ii pilins evade the immune system by changing their sugar structure rather than pilin primary structure. overall these results show that sequence invariable class ii pilins are cloaked in glycans with extensive functional and immunological consequences. © 2015 gault et al.
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آدرس
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structural mass spectrometry and proteomics unit,institut pasteur,cnrs umr 3528,paris,france,department of chemistry,physical and theoretical chemistry laboratory,university of oxford,oxford,ox1 3qz, United Kingdom, institut pasteur,unité de bioinformatique structurale,cnrs umr 3528,département de biologie structurale et chimie,paris, France, inserm,paris cardiovascular research center,paris,u970,france,université paris descartes,paris, France, inserm,paris cardiovascular research center,paris,u970,france,université paris descartes,paris, France, structural mass spectrometry and proteomics unit,institut pasteur,cnrs umr 3528,paris, France, inserm,paris cardiovascular research center,paris,u970,france,université paris descartes,paris, France, inserm,paris cardiovascular research center,paris,u970,france,université paris descartes,paris, France, institut pasteur,unité de bioinformatique structurale,cnrs umr 3528,département de biologie structurale et chimie,paris, France, institut pasteur,unité de bioinformatique structurale,cnrs umr 3528,département de biologie structurale et chimie,paris, France, cnrs,paris,umr3528, France, department of microbiology-immunology,northwestern university feinberg school of medicine,chicago,il, United States, service de microbiologie,assistance publique-hôpitaux de paris,hôpital européen georges-pompidou,paris, France, inserm umr1092,université de limoges,limoges, France, department of microbiology-immunology,northwestern university feinberg school of medicine,chicago,il, United States, institut pasteur,unité de bioinformatique structurale,cnrs umr 3528,département de biologie structurale et chimie,paris, France, structural mass spectrometry and proteomics unit,institut pasteur,cnrs umr 3528,paris, France, inserm,paris cardiovascular research center,paris,u970,france,université paris descartes,paris, France
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Authors
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