Literature DB >> 17284448

A role for molecular chaperone Hsc70 in reovirus outer capsid disassembly.

Tijana Ivanovic1, Melina A Agosto, Kartik Chandran, Max L Nibert.   

Abstract

After crossing the cellular membrane barrier during cell entry, most animal viruses must undergo further disassembly before initiating viral gene expression. In many cases, these disassembly mechanisms remain poorly defined. For this report, we examined a final step in disassembly of the mammalian reovirus outer capsid: cytoplasmic release of the central, delta fragment of membrane penetration protein mu1 to yield the transcriptionally active viral core particle. An in vitro assay with reticulocyte lysate recapitulated the release of intact delta molecules. Requirements for activity in this system were shown to include a protein factor, ATP, and Mg(2+) and K(+) ions, consistent with involvement of a molecular chaperone such as Hsc70. Immunodepletion of Hsc70 and Hsp70 impaired delta release, which was then rescued by addition of purified Hsc70. Hsc70 was associated with released delta molecules not only in the lysate but also during cell entry. We conclude that Hsc70 plays a defined role in reovirus outer capsid disassembly, during or soon after membrane penetration, to prepare the entering particle for gene expression and replication.

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Year:  2007        PMID: 17284448      PMCID: PMC4822165          DOI: 10.1074/jbc.M610258200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  36 in total

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Authors:  Kartik Chandran; Max L Nibert
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6.  Common and divergent peptide binding specificities of hsp70 molecular chaperones.

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Authors:  M L Nibert; B N Fields
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Review 10.  Dynamic remodeling of transcription complexes by molecular chaperones.

Authors:  Richard I Morimoto
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  32 in total

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7.  Differential Delivery of Genomic Double-Stranded RNA Causes Reovirus Strain-Specific Differences in Interferon Regulatory Factor 3 Activation.

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9.  Reovirus apoptosis and virulence are regulated by host cell membrane penetration efficiency.

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10.  Dynamin- and lipid raft-dependent entry of decay-accelerating factor (DAF)-binding and non-DAF-binding coxsackieviruses into nonpolarized cells.

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