Literature DB >> 19640986

Genetic and pharmacologic alteration of cathepsin expression influences reovirus pathogenesis.

Elizabeth M Johnson1, Joshua D Doyle, J Denise Wetzel, R Paul McClung, Nobuhiko Katunuma, James D Chappell, M Kay Washington, Terence S Dermody.   

Abstract

The cathepsin family of endosomal proteases is required for proteolytic processing of several viruses during entry into host cells. Mammalian reoviruses utilize cathepsins B (Ctsb), L (Ctsl), and S (Ctss) for disassembly of the virus outer capsid and activation of the membrane penetration machinery. To determine whether cathepsins contribute to reovirus tropism, spread, and disease outcome, we infected 3-day-old wild-type (wt), Ctsb(-/-), Ctsl(-/-), and Ctss(-/-) mice with the virulent reovirus strain T3SA+. The survival rate of Ctsb(-/-) mice was enhanced in comparison to that of wt mice, whereas the survival rates of Ctsl(-/-) and Ctss(-/-) mice were diminished. Peak titers at sites of secondary replication in all strains of cathepsin-deficient mice were lower than those in wt mice. Clearance of the virus was delayed in Ctsl(-/-) and Ctss(-/-) mice in comparison to the levels for wt and Ctsb(-/-) mice, consistent with a defect in cell-mediated immunity in mice lacking cathepsin L or S. Cathepsin expression was dispensable for establishment of viremia, but cathepsin L was required for maximal reovirus growth in the brain. Treatment of wt mice with an inhibitor of cathepsin L led to amelioration of reovirus infection. Collectively, these data indicate that cathepsins B, L, and S influence reovirus pathogenesis and suggest that pharmacologic modulation of cathepsin activity diminishes reovirus disease severity.

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Year:  2009        PMID: 19640986      PMCID: PMC2748054          DOI: 10.1128/JVI.01095-09

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  87 in total

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Review 2.  Lysosomal cysteine proteases: facts and opportunities.

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4.  A role for cathepsin L and cathepsin S in peptide generation for MHC class II presentation.

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Journal:  J Immunol       Date:  2002-03-15       Impact factor: 5.422

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Authors:  Daniel H Ebert; Jan Deussing; Christoph Peters; Terence S Dermody
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6.  Structure-based design of specific cathepsin inhibitors and their application to protection of bone metastases of cancer cells.

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Review 7.  Towards specific functions of lysosomal cysteine peptidases: phenotypes of mice deficient for cathepsin B or cathepsin L.

Authors:  T Reinheckel; J Deussing; W Roth; C Peters
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Review 9.  Thiol-dependent cathepsins: pathophysiological implications and recent advances in inhibitor design.

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Journal:  J Exp Med       Date:  2002-05-20       Impact factor: 14.307

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  20 in total

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2.  Activation of the Nipah virus fusion protein in MDCK cells is mediated by cathepsin B within the endosome-recycling compartment.

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3.  In search of cathepsins: how reovirus enters host cells.

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Journal:  DNA Cell Biol       Date:  2012-11-07       Impact factor: 3.311

4.  The Nogo receptor NgR1 mediates infection by mammalian reovirus.

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Review 6.  Reovirus receptors, cell entry, and proapoptotic signaling.

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7.  The reovirus μ2 C-terminal loop inversely regulates NTPase and transcription functions versus binding to factory-forming μNS and promotes replication in tumorigenic cells.

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8.  Genetic determinants of reovirus pathogenesis in a murine model of respiratory infection.

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9.  Apoptosis induction influences reovirus replication and virulence in newborn mice.

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10.  Structural and Functional Features of the Reovirus σ1 Tail.

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Journal:  J Virol       Date:  2018-06-29       Impact factor: 5.103

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