Abstract

The CA protein is the major structural protein of the retrovirus core, yet its contribution to the virus replication cycle has never been determined. In the mature virion core, CA forms a protein shell that surrounds the ribonucleoprotein (RNP) complex of viral RNA and replication enzymes. The function of this capsid-like shell is entirely unknown. However, several lines of evidence indicate that the integrity of CA and the shell it forms is in some way necessary for reverse transcription of the viral genome. We have previously demonstrated that conservative amino acid substitutions in the major homology region (MHR, a sequence shared by most retroviruses, retrotransposons, and hepadnaviruses) cause a serious deficit in DNA synthesis ability of the particles and a failure of the virus to infect. Since these particles contain all the necessary protein constituents as well as an intact RNA genome, it appears that the MHR and CA itself has a critical role in forming the constituents of the core into an effective DNA synthesis machine. A sequence similarity with the P proteins of paramyxo- and rhabdoviruses suggests the possibility that the CA protein acts directly to facilitate utilization of the genomic RNA template by participating as a non-catalytic component of the polymerase complex. Our previous genetic studies of the MHR have yielded at least four revertant viruses that carry unmapped suppressors that fall outside of the gag gene, providing a compelling argument for functional interactions of CA with one or more other constituents of the virion. The major goals of the proposed research will be to determine the identity of the suppressors responsible, to test predictions that CA is in direct contact with the viral RNP, and to identify other portions of the CA carboxy-terminal domain that cooperate with the MHR to facilitate these activities. Achieving these goals will be a major step toward understanding one of the most mysterious aspects of the retroviral life cycle and the ultimate identification of new strategies for antiviral therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA100322-05
Application #
7239581
Study Section
Virology Study Section (VR)
Program Officer
Read-Connole, Elizabeth Lee
Project Start
2003-06-01
Project End
2009-05-31
Budget Start
2007-06-01
Budget End
2009-05-31
Support Year
5
Fiscal Year
2007
Total Cost
$235,980
Indirect Cost

  Institution

Name
Pennsylvania State University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
129348186
City
Hershey
State
PA
Country
United States
Zip Code
17033

  Publications

Heyrana, Katrina J; Goh, Boon Chong; Perilla, Juan R et al. (2016) Contributions of Charged Residues in Structurally Dynamic Capsid Surface Loops to Rous Sarcoma Virus Assembly. J Virol 90:5700-5714
Goh, Boon Chong; Perilla, Juan R; England, Matthew R et al. (2015) Atomic Modeling of an Immature Retroviral Lattice Using Molecular Dynamics and Mutagenesis. Structure 23:1414-1425
England, Matthew R; Purdy, John G; Ropson, Ira J et al. (2014) Potential role for CA-SP in nucleating retroviral capsid maturation. J Virol 88:7170-7
Keller, Paul W; Huang, Rick K; England, Matthew R et al. (2013) A two-pronged structural analysis of retroviral maturation indicates that core formation proceeds by a disassembly-reassembly pathway rather than a displacive transition. J Virol 87:13655-64
Dalessio, Paula M; Craven, Rebecca C; Lokhandwala, Parvez M et al. (2013) Lethal mutations in the major homology region and their suppressors act by modulating the dimerization of the rous sarcoma virus capsid protein C-terminal domain. Proteins 81:316-25
Butan, Carmen; Lokhandwala, Parvez M; Purdy, John G et al. (2010) Suppression of a morphogenic mutant in Rous sarcoma virus capsid protein by a second-site mutation: a cryoelectron tomography study. J Virol 84:6377-86
Cardone, Giovanni; Purdy, John G; Cheng, Naiqian et al. (2009) Visualization of a missing link in retrovirus capsid assembly. Nature 457:694-8
Purdy, John G; Flanagan, John M; Ropson, Ira J et al. (2009) Retroviral capsid assembly: a role for the CA dimer in initiation. J Mol Biol 389:438-51
Lokhandwala, Parvez M; Nguyen, Tam-Linh N; Bowzard, J Bradford et al. (2008) Cooperative role of the MHR and the CA dimerization helix in the maturation of the functional retrovirus capsid. Virology 376:191-8
Butan, Carmen; Winkler, Dennis C; Heymann, J Bernard et al. (2008) RSV capsid polymorphism correlates with polymerization efficiency and envelope glycoprotein content: implications that nucleation controls morphogenesis. J Mol Biol 376:1168-81

Showing the most recent 10 out of 14 publications