Abstract

The long-term objectives of this proposal are to provide answers to three fundamental questions concerning translational regulation of adenovirus gene expression of infected cells. (1) How do adenoviruses overcome the interferon induced antiviral responses? (2) How do adenoviruses control the host cell translation machinery for the preferential translation of viral mRNAs at late times after infection? (3) What is the mechanism and function of the late viral 5' noncoding region (tripartite leader) in translation regulation? This proposal is designed to integrate two complementing areas of translation research; the enzymology of the interferon induced antiviral state, and the ability of adenovirus to take-over the host cell translation machinery. First, recombinant interferons will be used to elucidate the molecular mechanism by which adenovirus VA1 RNA inhibits activation of the interferon induced, P1/eIF2 alpha kinase. Adenoviruses are generally insensitive to the effects of interferon, and the anti-kinase activity associated with VA1 RNA is very likely responsible. Second, the role of the tripartite leader, and its possible interaction with VA1 RNA and the 18S ribosomal RNA, will be investigated to determine the mechanism for preferential translation of adenovirus MRNAs at late times after infection. A thorough genetic and biochemical analysis will be undertaken to determine the sequence requirements for tripartite leader function. Analysis of cells infected with adenoviruses in a VA1 + and - genetic background represents a unique and favorable system for investigation of translation regulateion. It is one of very few systems in which a mutational and biochemical analysis is possible for translation regulation by 5' noncoding regions, interferon induced antiviral activities, and viral responses to these cellular mechanisms.
The specific aims of this proposal are: (1) To investigate the mechanism by which Ad VA1 RNA antagonizes the activation of the interferon induced, P1/eIF2 alpha kinase. (2) To investigate the mechanism by which the Ad tripartite leader enhances translation. (3) To investigate the preferential translation of tripartite leader containing mRNAs at late times after infection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA042357-02
Application #
3183539
Study Section
Experimental Virology Study Section (EVR)
Project Start
1986-04-01
Project End
1989-03-31
Budget Start
1987-04-01
Budget End
1988-03-31
Support Year
2
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Type
Schools of Medicine
DUNS #
004514360
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Xi, Qiaoran; Cuesta, Rafael; Schneider, Robert J (2004) Tethering of eIF4G to adenoviral mRNAs by viral 100k protein drives ribosome shunting. Genes Dev 18:1997-2009
Cuesta, Rafael; Xi, Qiaoran; Schneider, Robert J (2004) Structural basis for competitive inhibition of eIF4G-Mnk1 interaction by the adenovirus 100-kilodalton protein. J Virol 78:7707-16
Schneider, Robert J; Mohr, Ian (2003) Translation initiation and viral tricks. Trends Biochem Sci 28:130-6
Cuesta, R; Xi, Q; Schneider, R J (2001) Preferential translation of adenovirus mRNAs in infected cells. Cold Spring Harb Symp Quant Biol 66:259-67
Cuesta, R; Xi, Q; Schneider, R J (2000) Adenovirus-specific translation by displacement of kinase Mnk1 from cap-initiation complex eIF4F. EMBO J 19:3465-74
Yueh, A; Schneider, R J (2000) Translation by ribosome shunting on adenovirus and hsp70 mRNAs facilitated by complementarity to 18S rRNA. Genes Dev 14:414-21
Cuesta, R; Laroia, G; Schneider, R J (2000) Chaperone hsp27 inhibits translation during heat shock by binding eIF4G and facilitating dissociation of cap-initiation complexes. Genes Dev 14:1460-70
Klein, N; Curatola, A M; Schneider, R J (1999) Calcium-induced stabilization of AU-rich short-lived mRNAs is a common default response. Gene Expr 7:357-65
Laroia, G; Cuesta, R; Brewer, G et al. (1999) Control of mRNA decay by heat shock-ubiquitin-proteasome pathway. Science 284:499-502
Feigenblum, D; Walker, R; Schneider, R J (1998) Adenovirus induction of an interferon-regulatory factor during entry into the late phase of infection. J Virol 72:9257-66

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