Abstract

Our long term goal is to understand the molecular mechanisms by which viruses occasionally jump from their normal host species to a new species, a process that may lead to emerging viral diseases in the new host species. We will focus on the interactions of the spike glycoprotein of murine coronavirus MHV with host cell receptors in the CEA family of glycoproteins. Several labs have shown that persistent infection of murine cell lines with MHV leads to markedly reduced expression of the CEACAMla receptor glycoprotein. In the persistently infected cultures, viruses with mutations in their spike glycoproteins and some other genes rapidly replace the wild type virus. The mutations in the spike genes are associated with acquisition of the ability of the virus to replicate in cell lines from cats, pigs, rats, monkeys and humans. We will identify amino acid residues in both the viral spike glycoprotein and the CEACAMla receptor that determine the specificity of binding virus. We will study the effects of mutations in S and in the receptor upon the specificity of virus-receptor interactions. We will continue our work on determining the crystal structures of CEACAM1 proteins to learn how the functional CEACAMla receptor differs from CEACAM1 b proteins from MHV-resistant mice and human CEACAMI. We will engineer spike and receptor proteins that will form co-crystals in order to determine the crystal structure of the complex. We will analyze the conformational changes in the viral spike protein induced by soluble receptor or by pH 8 at 37oC that are associated with membrane fusion and virus entry. To develop strains of inbred mice that are resistant to MHV infection, we will manipulate the Ceacaml gene in mice to reduce or eliminate expression of CEACAM1 proteins. We will also substitute chimeric CeacamlaJl b genes for the normal Ceacaml gene in mice. The animals will be tested for MHV-susceptibility and immune responses. These studies will provide important information about the mechanism of changing receptor specificity in a model virus that causes disease in its natural host.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI025231-20
Application #
7163034
Study Section
Experimental Virology Study Section (EVR)
Program Officer
Park, Eun-Chung
Project Start
1988-02-01
Project End
2008-12-31
Budget Start
2007-01-01
Budget End
2008-12-31
Support Year
20
Fiscal Year
2007
Total Cost
$525,523
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
041096314
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Hirai, Asuka; Ohtsuka, Nobuhisa; Ikeda, Toshio et al. (2010) Role of mouse hepatitis virus (MHV) receptor murine CEACAM1 in the resistance of mice to MHV infection: studies of mice with chimeric mCEACAM1a and mCEACAM1b. J Virol 84:6654-66
Miura, Tanya A; Holmes, Kathryn V (2009) Host-pathogen interactions during coronavirus infection of primary alveolar epithelial cells. J Leukoc Biol 86:1145-51
Miura, Tanya A; Wang, Jieru; Mason, Robert J et al. (2006) Rat coronavirus infection of primary rat alveolar epithelial cells. Adv Exp Med Biol 581:351-6
Thackray, Larissa B; Turner, Brian C; Holmes, Kathryn V (2005) Substitutions of conserved amino acids in the receptor-binding domain of the spike glycoprotein affect utilization of murine CEACAM1a by the murine coronavirus MHV-A59. Virology 334:98-110
Jeffers, Scott A; Tusell, Sonia M; Gillim-Ross, Laura et al. (2004) CD209L (L-SIGN) is a receptor for severe acute respiratory syndrome coronavirus. Proc Natl Acad Sci U S A 101:15748-53
Schickli, Jeanne H; Thackray, Larissa B; Sawicki, Stanley G et al. (2004) The N-terminal region of the murine coronavirus spike glycoprotein is associated with the extended host range of viruses from persistently infected murine cells. J Virol 78:9073-83
Tripet, Brian; Howard, Megan W; Jobling, Michael et al. (2004) Structural characterization of the SARS-coronavirus spike S fusion protein core. J Biol Chem 279:20836-49
Turner, Brian C; Hemmila, Erin M; Beauchemin, Nicole et al. (2004) Receptor-dependent coronavirus infection of dendritic cells. J Virol 78:5486-90
Thackray, Larissa B; Holmes, Kathryn V (2004) Amino acid substitutions and an insertion in the spike glycoprotein extend the host range of the murine coronavirus MHV-A59. Virology 324:510-24
Godfraind, C; Havaux, N; Holmes, K V et al. (1997) Role of virus receptor-bearing endothelial cells of the blood-brain barrier in preventing the spread of mouse hepatitis virus-A59 into the central nervous system. J Neurovirol 3:428-34