Abstract

TMEV-induced demyelinating disease is a highly relevant model for multiple sclerosis (MS) in which epidemiologic evidence strongly indicates involvement of an environmental factor, probably a virus infection. Thus, Investigations into the pathogenesis of this experimental animal model may well provide insight into MS. Virus-cell receptor interactions are a major determinant of virus host specificity, and the identification of specific virus receptors has greatly increased our understanding of viral pathogenesis. It is also apparent that many viruses use more than one cell surface molecule for their attachment and cell entry. The overall goal of the proposed research is to elucidate the molecular basis of Theiler's murine encephalomyelitis virus (TMEV) infection primarily at the level of attachment and cell entry, and to relate this to the persistent infection in mice. These studies should provide new insight into the mechanisms underlying TMEV persistence. They plan to: (1) Characterize the recently identified TMEV receptor protein, UGT, which mediates cell entry and infection of viruses of both TMEV neurovirulence groups. UGT is a member of a family of intrinsic membrane nucleotide-sugar transporter proteins resident in the trans-Golgi network (TGN). Vesicles bud from theTGN and cycle to the plasma membrane, so it is likely that UGT is expressed on the cell surface. These experiments will entail: (a) Demonstrating surface expression of UGT in transfected R26 and other somatic cells. (b) Analyzing the level of UGT mRNA and protein expression in different cell lines and mouse tissues. (c) Determining the sequence of the mouse homologue. (d) Identifying the TMEV binding site on extracellular domains of UGT by competitive inhibition with peptides, mAbs and insertional mutagenesis. (e) Determining whether UGT:(chromosome 11, 56.0 cm) is Tmev-5, a recently reported genetic locus mapped at 52.0 cm on chromosome 11. Tmev-5 is responsible for clinical disease and possibly viral load in (C57BI/6 X 129Sv IFN gamma-/-) F2 mice. (f) Determining the molecular basis of the functional loss of UGT activity in receptor-negative BHK-21 clones. (2) investigate the effect of sialic acid binding by less virulent TMEV on neurovirulence and viral persistence as well as determine the molecular basis of this receptor interaction. (3) Investigate whether the DA virus L*-1 mutant is reduced in fitness, since it has never been shown that acute CNS virus growth in mice by L*-1 mutant is comparable to that of wild type DA virus.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS021913-27
Application #
6539625
Study Section
Special Emphasis Panel (ZRG1-BDCN-4 (01))
Program Officer
Utz, Ursula
Project Start
1984-07-01
Project End
2004-05-31
Budget Start
2002-06-01
Budget End
2003-05-31
Support Year
27
Fiscal Year
2002
Total Cost
$300,000
Indirect Cost

  Institution

Name
Northshore University Healthsystem
Department
Type
DUNS #
154538107
City
Evanston
State
IL
Country
United States
Zip Code
60201

  Publications

Hertzler, Shannon; Liang, Zhiguo; Treso, Balint et al. (2011) Adaptation of Saffold virus 2 for high-titer growth in mammalian cells. J Virol 85:7411-8
Liang, Zhiguo; Kumar, A S Manoj; Jones, Morris S et al. (2008) Phylogenetic analysis of the species Theilovirus: emerging murine and human pathogens. J Virol 82:11545-54
Lipton, Howard L; Liang, Zhiguo; Hertzler, Shannon et al. (2007) A specific viral cause of multiple sclerosis: one virus, one disease. Ann Neurol 61:514-23
Lipton, Howard L; Kallio, Patricia; Jelachich, Mary Lou (2005) Simplified quantitative analysis of spinal cord cells from Theiler's virus-infected mice without the requirement for myelin debris removal. J Immunol Methods 299:107-15
Reddi, Honey V; Kumar, A S Manoj; Kung, Aisha Y et al. (2004) Heparan sulfate-independent infection attenuates high-neurovirulence GDVII virus-induced encephalitis. J Virol 78:8909-16
Trottier, Mark; Schlitt, Brian P; Kung, Aisha Y et al. (2004) Transition from acute to persistent Theiler's virus infection requires active viral replication that drives proinflammatory cytokine expression and chronic demyelinating disease. J Virol 78:12480-8
Kumar, A S Manoj; Reddi, Honey V; Kung, Aisha Y et al. (2004) Virus persistence in an animal model of multiple sclerosis requires virion attachment to sialic acid coreceptors. J Virol 78:8860-7
Kumar, A S Manoj; Kallio, Patricia; Luo, Ming et al. (2003) Amino acid substitutions in VP2 residues contacting sialic acid in low-neurovirulence BeAn virus dramatically reduce viral binding and spread of infection. J Virol 77:2709-16
Reddi, Honey V; Lipton, Howard L (2002) Heparan sulfate mediates infection of high-neurovirulence Theiler's viruses. J Virol 76:8400-7
Jelachich, M L; Bramlage, C; Lipton, H L (1999) Differentiation of M1 myeloid precursor cells into macrophages results in binding and infection by Theiler's murine encephalomyelitis virus and apoptosis. J Virol 73:3227-35

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