Abstract

Great promise still exists for the use of gene therapy in cancer treatment. The most direct approach is expression of toxic or immunostimulatory genes within tumor cells in vivo. This requires an efficient and targeted vector system. Replication-selective vectors provide the most promising means of achieving this goal. While numerous tumor cell active replicating vectors have been studied and some are in clinical trial, there is significant room for improvement of these vectors. We have explored pox viruses as tumor-selective replicating vectors for tumor directed gene delivery and direct tumor destruction. The pox viruses have the advantage of being extremely efficient in vivo. We have intentionally utilized an efficient strain of vaccinia virus (WR strain), which can rapidly spread through and destroy tissue. We have performed mutations of this vector to make it selective for tumors. Remarkably a systemic injection of this virus can infect tumor cells and directly destroy tumors up to 1 cm in size in our preliminary studies. While we are currently exploring clinical trials with this vector we realize there are many ways to improve this system. The proposed research will address the limitations of this vector to continue the preclinical development for cancer gene therapy. Ultimately, the vector can be utilized as a direct """"""""oncolytic"""""""" virus to express toxic genes within tumors, or to take advantage of the tumor environment to express immunostimulatory genes for development of systemic immunity against the tumor.
The aims of this study are 1.) Enhance tumor selectivity and safety by combining deletions of vaccinia serpins with TK and VGF, and define the mechanism of tumor selective replication. 2: Develop a tetracycline inducible gene expression system with tight in vivo regulation and creation of a """"""""shut off"""""""" switch for viral replication. 3: Immunosuppress to enhance the safety and efficacy of Vaccinia treatment and to allow successful treatment of the pre-immunized host. The research will not only help develop vaccinia virus as a vector but should have implications for other replicating vectors used for cancer gene therapy. Our goal is to explore any advances over our current vector in clinical trials in metastatic gastrointestinal cancers.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA100415-01A1
Application #
6775755
Study Section
Cancer Immunopathology and Immunotherapy Study Section (CII)
Program Officer
Hecht, Toby T
Project Start
2004-03-01
Project End
2008-02-29
Budget Start
2004-03-01
Budget End
2005-02-28
Support Year
1
Fiscal Year
2004
Total Cost
$297,983
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Surgery
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Downs-Canner, Stephanie; Guo, Zong Sheng; Ravindranathan, Roshni et al. (2016) Phase 1 Study of Intravenous Oncolytic Poxvirus (vvDD) in Patients With Advanced Solid Cancers. Mol Ther 24:1492-501
Guo, Z S; Bartlett, D L (2014) Oncolytic viruses as platform for multimodal cancer therapeutics: a promising land. Cancer Gene Ther 21:261-3
Sathaiah, M; Thirunavukkarasu, P; O'Malley, M E et al. (2012) Oncolytic poxvirus armed with Fas ligand leads to induction of cellular Fas receptor and selective viral replication in FasR-negative cancer. Cancer Gene Ther 19:192-201
Ziauddin, M F; Guo, Z S; O'Malley, M E et al. (2010) TRAIL gene-armed oncolytic poxvirus and oxaliplatin can work synergistically against colorectal cancer. Gene Ther 17:550-9
Guo, Z S; Parimi, V; O'Malley, M E et al. (2010) The combination of immunosuppression and carrier cells significantly enhances the efficacy of oncolytic poxvirus in the pre-immunized host. Gene Ther 17:1465-75
Guo, Z Sheng; Thorne, Stephen H; Bartlett, David L (2008) Oncolytic virotherapy: molecular targets in tumor-selective replication and carrier cell-mediated delivery of oncolytic viruses. Biochim Biophys Acta 1785:217-31
Chalikonda, S; Kivlen, M H; O'Malley, M E et al. (2008) Oncolytic virotherapy for ovarian carcinomatosis using a replication-selective vaccinia virus armed with a yeast cytosine deaminase gene. Cancer Gene Ther 15:115-25
Yang, S; Guo, Z S; O'Malley, M E et al. (2007) A new recombinant vaccinia with targeted deletion of three viral genes: its safety and efficacy as an oncolytic virus. Gene Ther 14:638-47
Guo, Z Sheng; Naik, Arpana; O'Malley, Mark E et al. (2005) The enhanced tumor selectivity of an oncolytic vaccinia lacking the host range and antiapoptosis genes SPI-1 and SPI-2. Cancer Res 65:9991-8