Abstract

CMV infection of hematopoietic cell transplant (HCT) recipients is a continuing problem that impacts the? outcome of this very successful therapy. Anti-viral treatment with ganciclovir/foscarnet is the main treatment? strategy to prevent CMV disease post-transplant (Tx). Despite significant advances in formulation and? delivery of anti-virals, their use complicates and extends the post-Tx recovery period and risk for CMV? disease. Considering these caveats, we are pursuing a novel therapeutic strategy that focuses on priming or? enhancing CMV-specific T cell immunity in healthy volunteers and HCT donors. In developing this vaccine? strategy, it is assumed that the target population will be immunocompetent, and vaccination judged? successful if immunity to CMV in response to the vaccine is equivalent in individuals with self-limited CMV? infection, which at first approximation represents a protective response. Towards this end in Specific Aim? (SA1) attenuated poxviruses (MVA) will be constructed that express four CMV antigens (CMV-MVA)? including UL32, UL44, UL83, and UL123-exon4 for stimulation of cellular immunity to CMV. MVA has? several advantages including avirulence, low inflammatory response and pathogenicity in humans, and? inclusion of multiple CMV antigens will ensure broad vaccine coverage for the USA. Lack of viral assembly? in mammals, together with studies showing its safety in heavily immunosuppressed macaques, rodents, and? in HIV-AIDS patients is evidence of its candidacy for use in HCT recipients. CMV-MVA constructed in SA1? will be qualified as immunologically functional, and subsequently transferred to a certified cGMP? manufacturer for clinical production. To ensure safety of the rMVA for Tx recipients, a safety study in SA2? will be conducted in healthy CMV positive and negative volunteers. The immunization regimen will model? the time frame required for providing two doses of vaccine to Tx donors without delaying Tx. A Phase II trial? using a randomized balanced cohort of 140 vaccinees and unvaccinated controls is proposed in SA3 to? establish whether immunization of a donor with CMV-MVA prior to Tx will result in modification of the course? and magnitude of CMV-viremia in a Tx recipient. This trial will be sufficiently powered that a 62% reduction? in viremia will be statistically meaningful as a measure of the success of the vaccine. Successful limitation of? acute CMV infection by this approach lays the foundation for addressing the important problem of late CMV? disease by immunizing Tx recipients with the same or an improved version of CMV-MVA.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA030206-26
Application #
7624219
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2008-04-01
Budget End
2009-03-31
Support Year
26
Fiscal Year
2008
Total Cost
$633,228
Indirect Cost

  Institution

Name
City of Hope/Beckman Research Institute
Department
Type
DUNS #
027176833
City
Duarte
State
CA
Country
United States
Zip Code
91010

  Publications

Limaye, Ajit P; La Rosa, Corinna; Longmate, Jeff et al. (2016) Plasma IL-10 Levels to Guide Antiviral Prophylaxis Prevention of Late-Onset Cytomegalovirus Disease, in High Risk Solid Kidney and Liver Transplant Recipients. Transplantation 100:210-6
Jonnalagadda, Mahesh; Mardiros, Armen; Urak, Ryan et al. (2015) Chimeric antigen receptors with mutated IgG4 Fc spacer avoid fc receptor binding and improve T cell persistence and antitumor efficacy. Mol Ther 23:757-68
Wang, Xiuli; Wong, ChingLam W; Urak, Ryan et al. (2015) CMVpp65 Vaccine Enhances the Antitumor Efficacy of Adoptively Transferred CD19-Redirected CMV-Specific T Cells. Clin Cancer Res 21:2993-3002
Mardiros, Armen; Forman, Stephen J; Budde, Lihua E (2015) T cells expressing CD123 chimeric antigen receptors for treatment of acute myeloid leukemia. Curr Opin Hematol 22:484-8
Caruso, Hillary G; Hurton, Lenka V; Najjar, Amer et al. (2015) Tuning Sensitivity of CAR to EGFR Density Limits Recognition of Normal Tissue While Maintaining Potent Antitumor Activity. Cancer Res 75:3505-18
Israyelyan, A; Goldstein, L; Tsai, W et al. (2015) Real-time assessment of relapse risk based on the WT1 marker in acute leukemia and myelodysplastic syndrome patients after hematopoietic cell transplantation. Bone Marrow Transplant 50:26-33
Wussow, Felix; Chiuppesi, Flavia; Martinez, Joy et al. (2014) Human cytomegalovirus vaccine based on the envelope gH/gL pentamer complex. PLoS Pathog 10:e1004524
Rushworth, David; Jena, Bipulendu; Olivares, Simon et al. (2014) Universal artificial antigen presenting cells to selectively propagate T cells expressing chimeric antigen receptor independent of specificity. J Immunother 37:204-13
Jena, Bipulendu; Moyes, Judy S; Huls, Helen et al. (2014) Driving CAR-based T-cell therapy to success. Curr Hematol Malig Rep 9:50-6
Singh, Harjeet; Huls, Helen; Kebriaei, Partow et al. (2014) A new approach to gene therapy using Sleeping Beauty to genetically modify clinical-grade T cells to target CD19. Immunol Rev 257:181-90

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