Abstract

The discovery and characterization of oncogenes and tumor suppressor genes have provided excellent targets for the development of novel gene-directed antiproliferative agents. Antisense and anti-gene approaches have the goal of specifically inhibiting gene expression. During the previous funding period, the principal investigator of this application has demonstrated that the selective inhibition of expression of the c-myc gene by the GC-specific DNA binding drug mithramycin is caused by its ability to prevent the binding of specific regulatory proteins to the c-myc promoter. However, currently available DNA binding drugs are inadequately sequence specific to inhibit expression of single genes in a therapeutically useful manner. Triplex DNA provides such a sequence- specific approach. During the previous funding period, the applicant has identified triplex forming sequences in the promoters of the c-myc, c-Ha- Ras, c-Ki-Ras, and cyclin D genes. Triplex based DNA binding compounds have been developed which interact with the c-myc, N-Ras, and cyclin D1 promoters in a sequence-specific manner and which inhibit c- myc transcription in vitro and in vivo. In addition, a cDNA partially complementary to a putative triplex forming transcript targeted to the c-myc promoter has been cloned and partially sequenced. Thus, the overall goal of the application is to fully characterize the antiproliferative effects of a series of c-myc targeted agents and to develop them into therapeutically useful anti-leukemic compounds.
The specific aims i nclude: 1. To characterize the ability of oligonucleotide-drug conjugates targeted to the c-myc P1 and P2 promoters to form triplex and inhibit c-myc transcription by leukemic cells in vivo. 2. To characterize the potential antiproliferative synergy of simultaneous inhibition of c-myc and cyclin D1. 3. To determine the ability of c-myc, cyclin D1, and N-Ras targeted phosphorothioate triplex forming oligonucleotides (TFO) and oligonucleotide-drug conjugates to inhibit proliferation of human and murine leukemic cells in vivo and to investigate the potential synergistic effects of DNA binding drugs. 4. To develop adenovirus/polylysine and liposome systems to enhance nuclear delivery of c-myc targeted oligonucleotide in animal systems. 5. To characterize the biological significance and therapeutic potential of naturally occurring triplex forming RNA molecules which are complementary to the c-myc promoter.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA042664-11
Application #
2667895
Study Section
Hematology Subcommittee 2 (HEM)
Program Officer
Johnson, George S
Project Start
1985-09-15
Project End
2001-02-28
Budget Start
1998-03-01
Budget End
1999-02-28
Support Year
11
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Sharma, Vivek R; Thomas, Shelia D; Miller, Donald M et al. (2018) Nucleolin Overexpression Confers Increased Sensitivity to the Anti-Nucleolin Aptamer, AS1411. Cancer Invest 36:475-491
Dapic, Virna; Bates, Paula J; Trent, John O et al. (2002) Antiproliferative activity of G-quartet-forming oligonucleotides with backbone and sugar modifications. Biochemistry 41:3676-85
Stewart, Delisha A; Xu, Xiaohua; Thomas, Shelia D et al. (2002) Acridine-modified, clamp-forming antisense oligonucleotides synergize with cisplatin to inhibit c-Myc expression and B16-F0 tumor progression. Nucleic Acids Res 30:2565-74
Bates, Paula J; Reddoch, James F; Hansakul, Pintusorn et al. (2002) Biosensor detection of triplex formation by modified oligonucleotides. Anal Biochem 307:235-43
Stewart, D A; Thomas, S D; Mayfield, C A et al. (2001) Psoralen-modified clamp-forming antisense oligonucleotides reduce cellular c-Myc protein expression and B16-F0 proliferation. Nucleic Acids Res 29:4052-61
Blume, S W; Lebowitz, J; Zacharias, W et al. (1999) The integral divalent cation within the intermolecular purine*purine. pyrimidine structure: a variable determinant of the potential for and characteristics of the triple helical association. Nucleic Acids Res 27:695-702
Kim, H G; Reddoch, J F; Mayfield, C et al. (1998) Inhibition of transcription of the human c-myc protooncogene by intermolecular triplex. Biochemistry 37:2299-304
Kim, H G; Miller, D M (1998) A novel triplex-forming oligonucleotide targeted to human cyclin D1 (bcl-1, proto-oncogene) promoter inhibits transcription in HeLa cells. Biochemistry 37:2666-72
Blume, S W; Guarcello, V; Zacharias, W et al. (1997) Divalent transition metal cations counteract potassium-induced quadruplex assembly of oligo(dG) sequences. Nucleic Acids Res 25:617-25
Ebbinghaus, S W; Vigneswaran, N; Miller, C R et al. (1996) Efficient delivery of triplex forming oligonucleotides to tumor cells by adenovirus-polylysine complexes. Gene Ther 3:287-97

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