Abstract

This application for an IP/CP represents a collaborative effort by investigators with expertise in cellular and molecular immunology and in clinical and molecular virology to establish a preclinical and clinical research program. The purpose of the program is to develop and test novel strategies for establishing an effective T cell response to HIV by the adoptive transfer of HIV-specific T cell clones. Methods have been developed in the participating laboratories to isolate, expand, and genetically-modify virus-specific CD4+ and CD8+ T cells in vitro, adoptively transfer immunity by the infusion of such virus-specific T cell clones, and to analyze the effects of therapeutic interventions on viral burden and the generation of viral diversity. Preclinical studies are proposed to promote continued evolution of improved immunotherapeutic strategies, and clinical trials translating these laboratory advances are planned to began in the first year and continue throughout the granting period. The proposal is divided into 3 research projects and two scientific cores. Project 1 will focus on adoptive immunotherapy of HIV infection with autologous HIV-specific CD8+ CTL clones. Clinical studies are designed to determine if improve antiviral effects and sustained immune responses can be achieved by the concurrent administration of T cell clones and IL2. Preclinical studies are evaluating genetic modifications of the CD8+ T cells to provide an antigen-regulated helper-independent phenotype that would bypass the need for exogenous IL2 or CD4+ cells to sustain the CD8+ responses. Project 2 will focus on adoptive immunotherapy of HIV infection with HIV-specific CD4+ T cell clones. Preclinical studies will evaluate the expression of distinct genes in CD4+T cells that can potentially provide protection from infection with HIV. Clinical trials will pursue establishing competent CD4+ T cell response to HIV by transfer of clones genetically-modified to resist HIV and evaluate the immunologic and virologic consequences of such a response. Project 3 will focus on the effects of T cell therapy on virus reservoirs and viral diversity. Specimens will be obtained from patients prior to and after therapy to analyze viral evolutionary dynamics, viral and cell turnover and decay rates, viral migration between compartments, selection pressures, and emerging and waning variants. The three projects are supported by a Virology Core essential for the monitoring of antiviral activity and a retroviral Vector Core capable of producing the vector necessary for the proposed human trials.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI043650-02
Application #
2887832
Study Section
Special Emphasis Panel (ZAI1-ACS-A (M2))
Program Officer
Sarver, Nava
Project Start
1998-09-30
Project End
2002-08-31
Budget Start
1999-09-01
Budget End
2000-08-31
Support Year
2
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Fred Hutchinson Cancer Research Center
Department
Type
DUNS #
075524595
City
Seattle
State
WA
Country
United States
Zip Code
98109

  Publications

Pollack, Seth M; Jones, Robin L; Farrar, Erik A et al. (2014) Tetramer guided, cell sorter assisted production of clinical grade autologous NY-ESO-1 specific CD8(+) T cells. J Immunother Cancer 2:36
Ochsenbein, Adrian F; Riddell, Stanley R; Brown, Michele et al. (2004) CD27 expression promotes long-term survival of functional effector-memory CD8+ cytotoxic T lymphocytes in HIV-infected patients. J Exp Med 200:1407-17
Cooper, Laurence J N; Topp, Max S; Pinzon, Cris et al. (2004) Enhanced transgene expression in quiescent and activated human CD8+ T cells. Hum Gene Ther 15:648-58
Topp, Max S; Riddell, Stanley R; Akatsuka, Yoshiki et al. (2003) Restoration of CD28 expression in CD28- CD8+ memory effector T cells reconstitutes antigen-induced IL-2 production. J Exp Med 198:947-55
Cheng, Laurence E; Ohlen, Claes; Nelson, Brad H et al. (2002) Enhanced signaling through the IL-2 receptor in CD8+ T cells regulated by antigen recognition results in preferential proliferation and expansion of responding CD8+ T cells rather than promotion of cell death. Proc Natl Acad Sci U S A 99:3001-6
Lewinsohn, Deborah A; Lines, Rebecca; Lewinsohn, David M et al. (2002) HIV-1 Vpr does not inhibit CTL-mediated apoptosis of HIV-1 infected cells. Virology 294:13-21
Cheng, Laurence E; Greenberg, Philip D (2002) Selective delivery of augmented IL-2 receptor signals to responding CD8+ T cells increases the size of the acute antiviral response and of the resulting memory T cell pool. J Immunol 169:4990-7
Truong, Hong-Ha M; Berrey, M Michelle; Shea, Theresa et al. (2002) Concordance between HIV source partner identification and molecular confirmation in acute retroviral syndrome. J Acquir Immune Defic Syndr 29:232-43
Bonini, C; Lee, S P; Riddell, S R et al. (2001) Targeting antigen in mature dendritic cells for simultaneous stimulation of CD4+ and CD8+ T cells. J Immunol 166:5250-7
Georges, G E; Storb, R; Bruno, B et al. (2001) Engraftment of DLA-haploidentical marrow with ex vivo expanded, retrovirally transduced cytotoxic T lymphocytes. Blood 98:3447-55

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