Role of Cellular Actin in the Gene Expression and Morphogenesis of Human Respiratory Syncytial Virus

Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression.In vitro,specific antibodies against actin inhibited RSV transcription, whereas antibodies against other cytoskeletal proteins had little or no effect. Affinity purifi...

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Published inVirology (New York, N.Y.) Vol. 252; no. 1; pp. 137 - 148
Main Authors Burke, Emily, Dupuy, Lesley, Wall, Cynthia, Barik, Sailen
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 05.12.1998
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Abstract Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression.In vitro,specific antibodies against actin inhibited RSV transcription, whereas antibodies against other cytoskeletal proteins had little or no effect. Affinity purified cellular actin or bacterially expressed recombinant actin activated RSV transcription. However, optimal transcription required additional cellular protein(s) that appeared to function as accessory factor(s) for actin. In the absence of actin, these proteins did not activate viral transcription. Purified viral nucleocapsids contained actin, but no cytokeratin, tubulin, or vimentin. Cytochalasin D or DNaseI—agents that destabilize actin polymers—had little effect on RSV transcription. RSV infection itself seemed to alter the structure of the cellular actin filaments. Treatment of infected cells with cytochalasin D produced a more severe disruption of the filaments and drastically reduced the production of infectious virus particles but still had little effect on intracellular synthesis of viral macromolecules. Thus actin seems to serve a dual role in RSV life cycle: its monomeric form as well as polymeric form activate viral transcription, while only the microfilament form may take part in viral morphogenesis and/or budding.
AbstractList Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression. In vitro, specific antibodies against actin inhibited RSV transcription, whereas antibodies against other cytoskeletal proteins had little or no effect. Affinity purified cellular actin or bacterially expressed recombinant actin activated RSV transcription. However, optimal transcription required additional cellular protein(s) that appeared to function as accessory factor(s) for actin. In the absence of actin, these proteins did not activate viral transcription. Purified viral nucleocapsids contained actin, but no cytokeratin, tubulin, or vimentin. Cytochalasin D or DNasel--agents that destabilize actin polymers--had little effect on RSV transcription. RSV infection itself seemed to alter the structure of the cellular actin filaments. Treatment of infected cells with cytochalasin D produced a more severe disruption of the filaments and drastically reduced the production of infectious virus particles but still had little effect on intracellular synthesis of viral macromolecules. Thus actin seems to serve a dual role in RSV life cycle: its monomeric form as well as polymeric form activate viral transcription, while only the microfilament form may take part in viral morphogenesis and/or budding.
Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression. In vitro,specific antibodies against actin inhibited RSV transcription, whereas antibodies against other cytoskeletal proteins had little or no effect. Affinity purified cellular actin or bacterially expressed recombinant actin activated RSV transcription. However, optimal transcription required additional cellular protein(s) that appeared to function as accessory factor(s) for actin. In the absence of actin, these proteins did not activate viral transcription. Purified viral nucleocapsids contained actin, but no cytokeratin, tubulin, or vimentin. Cytochalasin D or DNaseI-agents that destabilize actin polymers-had little effect on RSV transcription. RSV infection itself seemed to alter the structure of the cellular actin filaments. Treatment of infected cells with cytochalasin D produced a more severe disruption of the filaments and drastically reduced the production of infectious virus particles but still had little effect on intracellular synthesis of viral macromolecules. Thus actin seems to serve a dual role in RSV life cycle: its monomeric form as well as polymeric form activate viral transcription, while only the microfilament form may take part in viral morphogenesis and/or budding. Copyright 1998 Academic Press.
Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression.In vitro,specific antibodies against actin inhibited RSV transcription, whereas antibodies against other cytoskeletal proteins had little or no effect. Affinity purified cellular actin or bacterially expressed recombinant actin activated RSV transcription. However, optimal transcription required additional cellular protein(s) that appeared to function as accessory factor(s) for actin. In the absence of actin, these proteins did not activate viral transcription. Purified viral nucleocapsids contained actin, but no cytokeratin, tubulin, or vimentin. Cytochalasin D or DNaseI—agents that destabilize actin polymers—had little effect on RSV transcription. RSV infection itself seemed to alter the structure of the cellular actin filaments. Treatment of infected cells with cytochalasin D produced a more severe disruption of the filaments and drastically reduced the production of infectious virus particles but still had little effect on intracellular synthesis of viral macromolecules. Thus actin seems to serve a dual role in RSV life cycle: its monomeric form as well as polymeric form activate viral transcription, while only the microfilament form may take part in viral morphogenesis and/or budding.
Author Wall, Cynthia
Dupuy, Lesley
Burke, Emily
Barik, Sailen
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  surname: Wall
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  givenname: Sailen
  surname: Barik
  fullname: Barik, Sailen
BackLink https://www.ncbi.nlm.nih.gov/pubmed/9875324$$D View this record in MEDLINE/PubMed
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Issue 1
Keywords microfilament
actin
transcription
cytoskeleton
respiratory syncytial virus
Paramyxovirus
Language English
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Snippet Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression.In vitro,specific...
Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression. In vitro, specific...
Cytoskeletal protein actin and nonactin cellular proteins were essential for human respiratory syncytial virus (RSV) gene expression. In vitro,specific...
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StartPage 137
SubjectTerms actin
Actin Cytoskeleton - chemistry
Actin Cytoskeleton - metabolism
Actins - immunology
Actins - isolation & purification
Actins - physiology
Animals
Cell Line
Chickens
Chromatography, Affinity
Cytochalasin D - metabolism
Cytoskeletal Proteins - analysis
cytoskeleton
Gene Expression Regulation, Viral
Goats
Humans
Mice
microfilament
Paramyxovirus
Protein Conformation
Rabbits
Recombinant Proteins - metabolism
respiratory syncytial virus
Respiratory Syncytial Viruses - genetics
Respiratory Syncytial Viruses - growth & development
transcription
Transcription, Genetic
Transcriptional Activation
Virion - chemistry
Title Role of Cellular Actin in the Gene Expression and Morphogenesis of Human Respiratory Syncytial Virus
URI https://dx.doi.org/10.1006/viro.1998.9471
https://www.ncbi.nlm.nih.gov/pubmed/9875324
https://search.proquest.com/docview/18423328
https://search.proquest.com/docview/69114508
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