Ultrastructural and Biochemical Study of Frog Virus 3 Uptake by BHK-21 Cells

Groupe de Recherches de l'INSERM (U 74) sur la Pathogénie des Infections Virales et Laboratoire de Virologie de la Faculté de Médecine, Université Louis Pasteur, 3, rue Koeberlé, 67000 Strasbourg, France Ultrastructural studies of the uptake of enveloped and naked frog virus 3 (FV 3) particles...

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Published inJournal of general virology Vol. 66; no. 2; pp. 283 - 293
Main Authors Braunwald, Jacqueline, Nonnenmacher, Huguette, Tripier-Darcy, Francoise
Format Journal Article
LanguageEnglish
Published Reading Soc General Microbiol 01.02.1985
Society for General Microbiology
Subjects
Animals
BHK-21 cells
Biological and medical sciences
Cell Fusion
Cell Line
Chloroquine - pharmacology
Coated Pits, Cell-Membrane - physiology
Cricetinae
Endocytosis - drug effects
Fibroblasts - metabolism
Fibroblasts - ultrastructure
frog virus 3
Fundamental and applied biological sciences. Psychology
Iridoviridae - metabolism
Kidney
Mesocricetus
Microbiology
Morphology, structure, chemical composition, physicochemical properties
Virology
Membrane fusion
Animal origin
Electron microscopy
Host virus relation
Frog virus 3
Virus
Cell line BHK
Iridoviridae
Adsorption
Ultrastructure
Internalization
Ranavirus
Virus envelope
Virus penetration
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Summary:Groupe de Recherches de l'INSERM (U 74) sur la Pathogénie des Infections Virales et Laboratoire de Virologie de la Faculté de Médecine, Université Louis Pasteur, 3, rue Koeberlé, 67000 Strasbourg, France Ultrastructural studies of the uptake of enveloped and naked frog virus 3 (FV 3) particles by BHK-21 cells have shown that enveloped viruses are internalized by adsorptive endocytosis via coated pits. The enveloped particles then appear to move through endosomes and finally lysosomes. Naked viruses may also follow the same pathway but only rarely. Their more frequent mode of entry is by fusion between the virus shell and the cellular membranes, thus allowing the virus to shed its nucleoprotein content directly into the cytoplasm. This difference in the mechanism of penetration has been confirmed by the use of lysosomotropic agents: the inhibition of viral growth being far more drastic for enveloped FV 3 than for naked virus implies that a lysosomal step is required for the multiplication of enveloped viral particles. Keywords: FV 3 internalization, ultrastructure, envelope, fusion Received 23 August 1984; accepted 11 October 1984.
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ISSN:0022-1317
1465-2099
DOI:10.1099/0022-1317-66-2-283