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Binding of Glutathione to Enterovirus Capsids Is Essential for Virion Morphogenesis
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نویسنده
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thibaut h.j. ,van der linden l. ,jiang p. ,thys b. ,canela m.-d. ,aguado l. ,rombaut b. ,wimmer e. ,paul a. ,pérez-pérez m.-j. ,van kuppeveld f.j.m. ,neyts j.
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منبع
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plos pathogens - 2014 - دوره : 10 - شماره : 4
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چکیده
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Enteroviruses (family of the picornaviridae) cover a large group of medically important human pathogens for which no antiviral treatment is approved. although these viruses have been extensively studied,some aspects of the viral life cycle,in particular morphogenesis,are yet poorly understood. we report the discovery of tp219 as a novel inhibitor of the replication of several enteroviruses,including coxsackievirus and poliovirus. we show that tp219 binds directly glutathione (gsh),thereby rapidly depleting intracellular gsh levels and that this interferes with virus morphogenesis without affecting viral rna replication. the inhibitory effect on assembly was shown not to depend on an altered reducing environment. using tp219,we show that gsh is an essential stabilizing cofactor during the transition of protomeric particles into pentameric particles. sequential passaging of coxsackievirus b3 in the presence of low gsh-levels selected for gsh-independent mutants that harbored a surface-exposed methionine in vp1 at the interface between two protomers. in line with this observation,enteroviruses that already contained this surface-exposed methionine,such as ev71,did not rely on gsh for virus morphogenesis. biochemical and microscopical analysis provided strong evidence for a direct interaction between gsh and wildtype vp1 and a role for this interaction in localizing assembly intermediates to replication sites. consistently,the interaction between gsh and mutant vp1 was abolished resulting in a relocalization of the assembly intermediates to replication sites independent from gsh. this study thus reveals gsh as a novel stabilizing host factor essential for the production of infectious enterovirus progeny and provides new insights into the poorly understood process of morphogenesis. © 2014 thibaut et al.
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آدرس
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department of microbiology and immunology,rega institute for medical research,university of leuven,leuven,belgium,virology division,department of infectious diseases and immunology,utrecht university,utrecht, Netherlands, department of microbiology and immunology,rega institute for medical research,university of leuven,leuven,belgium,department medical microbiology,radboud university nijmegen medical centre,nijmegen centre for molecular life sciences,nijmegen, Netherlands, department of molecular genetics and microbiology,school of medicine,stony brook university,stony brook,ny, United States, department of pharmaceutical biotechnology and molecular biology,vrije universiteit brussel,brussel, Belgium, instituto de química médica (iqm-csic),madrid, Spain, instituto de química médica (iqm-csic),madrid, Spain, department of pharmaceutical biotechnology and molecular biology,vrije universiteit brussel,brussel, Belgium, department of molecular genetics and microbiology,school of medicine,stony brook university,stony brook,ny, United States, department of molecular genetics and microbiology,school of medicine,stony brook university,stony brook,ny, United States, instituto de química médica (iqm-csic),madrid, Spain, virology division,department of infectious diseases and immunology,utrecht university,utrecht,netherlands,department medical microbiology,radboud university nijmegen medical centre,nijmegen centre for molecular life sciences,nijmegen, Netherlands, department of microbiology and immunology,rega institute for medical research,university of leuven,leuven, Belgium
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Authors
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