Abstract

The Vector Core has been and will continue to serve as a critical component of the """"""""Cytokine Gone Therapy for Cancer Program, providing serotype 5 adenoviral viral vectors as well as additional novel reagents to Projects 1-3. The Vecto Core will function within the framework of the Program as a dynamic resource that can provide state-of-the-at adenoviral vector technology. In addition to the ability to construct and propagate adenoviral vectors, the Vector Cor also is able to generate retroviral, adeno-associated virus and lentivirus vectors for gone delivery and is developin expression vectors for use in liposome and particle-mediated gone transduction. While these are not """"""""line-itemed"""""""" in an of the projects, our ability to provide such diversified vector systems may prospectively facilitate individual project goals The Vector Core has also developed an algorithm for the generation of codon optimized cDNAs, allowing for highe levels of gone expression following gone transfer. Specifically, the role of the Vector Core in this PPG will be t construct and provide the necessary Ad5, and if needed novel serotype-based adenoviral vectors expressing th appropriate (and possibly codon-optimized) genes, as required for the performance of studies outlined in each of the thre proposed projects. In addition, the core will propagate already constructed adenoviral vectors, and provide high-titer quality-tested stocks of vectors for the broad range of experiments described in this application. There will be constan two-way dialogue between Core B and each of the projects at all times, and particularly in all cases where adenovira gone delivery must be further optimized. Furthermore, the Core will provide any technical assistance and training t individuals in the use of adenoviral viral vectors for gone transfer as needed.
The Specific Aims of the Vector Core are: 1. To provide each investigator with adenoviml vectors expressing the required therapeutic and possibly eodon-optimize genes appropriate for their proposed experiments. 2. To develop improved adenoviral vectors for more efficient gene transfer into tumor cells and dendritic cells. 3. To assist in the development of methods for efficient adenoviral gene delivery to mouse and human tumors cells an dendritic cells. 4. To provide technical assistance and protocols to each of the projects in the use of adenoviral gene delivery

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA100327-04
Application #
7596855
Study Section
Subcommittee G - Education (NCI)
Project Start
Project End
Budget Start
2008-04-01
Budget End
2009-03-31
Support Year
4
Fiscal Year
2008
Total Cost
$105,723
Indirect Cost

  Institution

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

  Publications

Yang, Chenjie; Ruffner, Melanie A; Kim, Seon-Hee et al. (2012) Plasma-derived MHC class II+ exosomes from tumor-bearing mice suppress tumor antigen-specific immune responses. Eur J Immunol 42:1778-84
Reay, J; Gambotto, A; Robbins, P D (2012) The antitumor effects of adenoviral-mediated, intratumoral delivery of interleukin 23 require endogenous IL-12. Cancer Gene Ther 19:135-43
Zhao, Xi; Bose, Anamika; Komita, Hideo et al. (2012) Vaccines targeting tumor blood vessel antigens promote CD8(+) T cell-dependent tumor eradication or dormancy in HLA-A2 transgenic mice. J Immunol 188:1782-8
Rao, Aparna; Taylor, Jennifer L; Chi-Sabins, Nina et al. (2012) Combination therapy with HSP90 inhibitor 17-DMAG reconditions the tumor microenvironment to improve recruitment of therapeutic T cells. Cancer Res 72:3196-206
Qu, Yanyan; Chen, Lu; Lowe, Devin B et al. (2012) Combined Tbet and IL12 gene therapy elicits and recruits superior antitumor immunity in vivo. Mol Ther 20:644-51
Qu, Y; Taylor, J L; Bose, A et al. (2011) Therapeutic effectiveness of intratumorally delivered dendritic cells engineered to express the pro-inflammatory cytokine, interleukin (IL)-32. Cancer Gene Ther 18:663-73
Lowe, Devin B; Storkus, Walter J (2011) Chronic inflammation and immunologic-based constraints in malignant disease. Immunotherapy 3:1265-74
Zhao, Xi; Bose, Anamika; Komita, Hideo et al. (2011) Intratumoral IL-12 gene therapy results in the crosspriming of Tc1 cells reactive against tumor-associated stromal antigens. Mol Ther 19:805-14
Zhu, Xinmei; Fallert-Junecko, Beth A; Fujita, Mitsugu et al. (2010) Poly-ICLC promotes the infiltration of effector T cells into intracranial gliomas via induction of CXCL10 in IFN-alpha and IFN-gamma dependent manners. Cancer Immunol Immunother 59:1401-9
Lipscomb, Michael W; Taylor, Jennifer L; Goldbach, Cristina J et al. (2010) DC expressing transgene Foxp3 are regulatory APC. Eur J Immunol 40:480-93

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