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Cryo electron tomography of herpes simplex virus during axonal transport and secondary envelopment in primary neurons
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نویسنده
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ibiricu i. ,huiskonen j.t. ,döhner k. ,bradke f. ,sodeik b. ,grünewald k.
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منبع
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plos pathogens - 2011 - دوره : 7 - شماره : 12
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چکیده
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During herpes simplex virus 1 (hsv1) egress in neurons,viral particles travel from the neuronal cell body along the axon towards the synapse. whether hsv1 particles are transported as enveloped virions as proposed by the 'married' model or as non-enveloped capsids suggested by the 'separate' model is controversial. specific viral proteins may form a recruitment platform for microtubule motors that catalyze such transport. however,their subviral location has remained elusive. here we established a system to analyze herpesvirus egress by cryo electron tomography. at 16 h post infection,we observed intra-axonal transport of progeny hsv1 viral particles in dissociated hippocampal neurons by live-cell fluorescence microscopy. cryo electron tomography of frozen-hydrated neurons revealed that most egressing capsids were transported independently of the viral envelope. unexpectedly,we found not only dna-containing capsids (cytosolic c-capsids),but also capsids lacking dna (cytosolic a-/b-capsids) in mid-axon regions. subvolume averaging revealed lower amounts of tegument on cytosolic a-/b-capsids than on c-capsids. nevertheless,all capsid types underwent active axonal transport. therefore,even few tegument proteins on the capsid vertices seemed to suffice for transport. secondary envelopment of capsids was observed at axon terminals. on their luminal face,the enveloping vesicles were studded with typical glycoprotein-like spikes. furthermore,we noted an accretion of tegument density at the concave cytosolic face of the vesicle membrane in close proximity to the capsids. three-dimensional analysis revealed that these assembly sites lacked cytoskeletal elements,but that filamentous actin surrounded them and formed an assembly compartment. our data support the 'separate model' for hsv1 egress,i.e. progeny herpes viruses being transported along axons as subassemblies and not as complete virions within transport vesicles. © 2011 ibiricu et al.
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آدرس
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department of molecular structural biology,max planck institute of biochemistry,martinsried, Germany, department of molecular structural biology,max planck institute of biochemistry,martinsried,germany,institute of biotechnology,university of helsinki,helsinki,finland,oxford particle imaging centre,division of structural biology,wellcome trust centre for human genetics,university of oxford,oxford, United Kingdom, institute of virology,hannover medical school,hannover, Germany, research group axonal growth and regeneration,max planck institute of neurobiology,martinsried,germany,german center for neurodegenerative diseases (dzne),bonn, Germany, institute of virology,hannover medical school,hannover, Germany, department of molecular structural biology,max planck institute of biochemistry,martinsried,germany,oxford particle imaging centre,division of structural biology,wellcome trust centre for human genetics,university of oxford,oxford, United Kingdom
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Authors
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