Abstract

Specific aspects of glucocorticoid-regulated transcription of the proviral genes of mouse mammary tumor virus (MMTV) will be investigated to address the long range goals of understanding the molecular mechanisms by which steroid hormones affect gene expression. A combination of molecular and genetic approaches will be taken with continuous tissue culture cell lines. Preliminary evidence has indicated that the MMTV long terminal repeat (LTR) contains a negative regulatory element that decreases transcription from the MMTV promoter in the absence of glucocorticoids; the function of this element may be to maintain regulated genes in an inactive state in the absence of hormone. The DNA sequences required for this negative element will be defined, and the element will be characterized with regard to its position, orientation and promoter specificity and its requirement for specific trans-acting factors utilizing transient expression assays. A number of endogenous MMTV proviral genes have been isolated by molecular cloning; these endogenous genes are normally not transcriptionally active. The ability of the LTRs of these isolated genes to function as regulated promoters will be compared in a defined experimental context to assess the relative extent to which DNA sequence defects and chromosomal position effects contribute to the lack of endogenous gene expression. The function of the LTRs in vivo will be correlated with the DNA sequence of regulatory elements and with glucocorticoid receptor binding in vitro. The potential role of DNA methylation in controlling the potential for steroid-regulated transcription will be investigated. Variants in glucocorticoid-responsive gene expression will be selected that take advantage of selectable markers expressed from the MMTV promoter. The proposed experiments will explore the molecular basis of regulatory and developmental phenomena that are potentially related to many human diseases. In addition, the increased understanding of transcriptional regulatory elements within the MMTV LTRs may aid in elucidating the mechanism of viral tumorigenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA032695-08
Application #
3170570
Study Section
Experimental Virology Study Section (EVR)
Project Start
1982-07-01
Project End
1995-04-30
Budget Start
1991-05-01
Budget End
1992-04-30
Support Year
8
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Texas A&M University
Department
Type
Schools of Earth Sciences/Natur
DUNS #
City
College Station
State
TX
Country
United States
Zip Code
77845

  Publications

Fee, Brian E; Steinke, John W; Pierce, Jennifer et al. (2002) Initiation site binding protein and the initiator-like promoter element of mouse mammary tumor virus. Virology 302:185-94
Kang, C J; Peterson, D O (2001) In vitro analysis of transcriptional repression of the mouse mammary tumor virus promoter. Biochem Biophys Res Commun 287:402-10
Steinke, J W; Kopytek, S J; Peterson, D O (2000) Discrete promoter elements affect specific properties of RNA polymerase II transcription complexes. Nucleic Acids Res 28:2726-35
Kang, C J; Peterson, D O (1999) Identification of a protein that recognizes a distal negative regulatory element within the mouse mammary tumor virus long terminal repeat. Virology 264:211-9
Kopytek, S J; Peterson, D O (1998) ATP-mediated activation of RNA polymerase II transcription complexes. Gene Expr 7:75-86
Bral, C M; Steinke, J W; Kang, C J et al. (1998) RNA polymerase II transcription complex assembly in nuclear extracts. Gene Expr 7:191-204
Kim, M H; Peterson, D O (1995) Stimulation of basal transcription from the mouse mammary tumor virus promoter by Oct proteins. J Virol 69:4717-26
Kim, M H; Peterson, D O (1995) Oct-1 protein promotes functional transcription complex assembly on the mouse mammary tumor virus promoter. J Biol Chem 270:27823-8
Pierce, J; Fee, B E; Toohey, M G et al. (1993) A mouse mammary tumor virus promoter element near the transcription initiation site. J Virol 67:415-24
Huang, M; Lee, J W; Peterson, D O (1993) Functional redundancy of octamer elements in the mouse mammary tumor virus promoter. Nucleic Acids Res 21:5235-41

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