Abstract

Within the past year there have been encouraging results in the treatment of HIV-1 infection resulting from the combinatorial use of drugs targeted against HIV-1 encoded reverse transcriptase and protease. Multiple targeting based upon rational drug design has therefore proven to be an effective method for dramatically inhibiting viral infectivity. Despite the success of the combinatorial drug therapy, there are cautious optimism and concerns about viral resistance, potential toxicity from long term use of the drugs, and long lived viral reservoirs that fully justify further development and testing of other types of antiviral therapies. One form of antiviral therapy that is actively being pursued by a number of laboratories is gene therapy, whereby antiviral genes are permanently introduced into hematopoietic cells to ameliorate viral infectivity. Within the past year, several different gene therapy trials have been initiated. One class of reagents currently in phase 1 clinical trials is ribozymes, which are site-specific RNA cleaving agents. These RNA molecules can be engineered to cleave at hundreds of different sites along the length of the HIV genome, thereby providing a multiple drug targeting strategy. The proposed research extends and takes advantage of lessons learned from our ongoing research efforts with anti-HIV ribozymes. The overall goal of this program is the enhancement of intracellular efficacy of anti-HIV ribozymes by understanding and utilizing intracellular and viral encoded proteins and novel RNA expression strategies to facilitate ribozyme-target co-localization. Concurrent with studies for improving ribozyme efficacy, combinations or ribozyme-expression cassettes will be inserted into Adeno Associated Viral vectors and HIV based lentiviral vectors for transduction into CD34+ hematopoietic progenitor cells, and transfusion into a SCID-hu mouse model. In this system the effects of anti-HIV-1 ribozyme expression on CD34+ cell differentiation and HIV-1 infection will be evaluated. The studies proposed encompass the most comprehensive study of anti-HIV-1 ribozyme function and pre-clinical analyses of ribozymes model to date. The results from this program will greatly facilitate the effective use of ribozyme treatment for HIV-1 infection in a gene therapy setting.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI029329-11
Application #
2886640
Study Section
AIDS and Related Research Study Section 1 (ARRA)
Program Officer
Sarver, Nava
Project Start
1996-07-03
Project End
2002-06-30
Budget Start
1999-07-01
Budget End
2000-06-30
Support Year
11
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
City of Hope/Beckman Research Institute
Department
Type
DUNS #
City
Duarte
State
CA
Country
United States
Zip Code
91010

  Publications

Pang, Ka Ming; Castanotto, Daniela; Li, Haitang et al. (2018) Incorporation of aptamers in the terminal loop of shRNAs yields an effective and novel combinatorial targeting strategy. Nucleic Acids Res 46:e6
Zhou, Jiehua; Lazar, Daniel; Li, Haitang et al. (2018) Receptor-targeted aptamer-siRNA conjugate-directed transcriptional regulation of HIV-1. Theranostics 8:1575-1590
Satheesan, Sangeetha; Li, Haitang; Burnett, John C et al. (2018) HIV Replication and Latency in a Humanized NSG Mouse Model during Suppressive Oral Combinational Antiretroviral Therapy. J Virol 92:
Zhou, Jiehua; Rossi, John (2017) Aptamers as targeted therapeutics: current potential and challenges. Nat Rev Drug Discov 16:181-202
Song, Min-Sun; Rossi, John J (2017) Molecular mechanisms of Dicer: endonuclease and enzymatic activity. Biochem J 474:1603-1618
Yoon, Sorah; Rossi, John J (2017) Future strategies for the discovery of therapeutic aptamers. Expert Opin Drug Discov 12:317-319
Yoon, Sorah; Huang, Kai-Wen; Reebye, Vikash et al. (2017) Aptamer-Drug Conjugates of Active Metabolites of Nucleoside Analogs and Cytotoxic Agents Inhibit Pancreatic Tumor Cell Growth. Mol Ther Nucleic Acids 6:80-88
Yoon, Sorah; Armstrong, Brian; Habib, Nagy et al. (2017) Blind SELEX Approach Identifies RNA Aptamers That Regulate EMT and Inhibit Metastasis. Mol Cancer Res 15:811-820
Yoon, Sorah; Rossi, John J (2017) Emerging cancer-specific therapeutic aptamers. Curr Opin Oncol 29:366-374
Takahashi, Mayumi; Wu, Xiwei; Ho, Michelle et al. (2016) High throughput sequencing analysis of RNA libraries reveals the influences of initial library and PCR methods on SELEX efficiency. Sci Rep 6:33697

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