Abstract

We found that administration of peptide-loaded CD34-DC vaccine can lead to therapeutic immunity in? metastatic melanoma. This """"""""composite vaccine"""""""" includes several DC subsets, the combination of which may? contribute to vaccine efficacy. We have also found that culturing monocytes with GM-CSF and TNF yields a? composite vaccine that is phenotypically different from the """"""""traditional"""""""" GM-CSF/IL-4 monocyte-derived DCs,? while it appears similar to CD34-DCs. Such vaccine would offer a great advantage for clinical trials as it can? be generated within 3 days and does not require G-CSF treatment of the patients. The feasibility of? administering such vaccine has already been shown with ten patients. We also found that monocyte-derived? IL4-DCs loaded with killed allogeneic melanoma cells induce clinical and immunological responses. We? hypothesize that monocyte-derived composite DC vaccines loaded with killed allogeneic melanoma cells? activated with TLR agonists ex vivo will induce clinical and immunological responses. Therefore, AIM 1 will? optimize the TNF-MDCs vaccine loaded with killed allogeneic Colo829 melanoma cells and activated via? TRLs and CD40.
AIM 2 will establish in vivo the immunogenicity of TNF-MDCs loaded with killed allogeneic? melanoma cells in patients This will be a Phase l/ll single arm clinical trial which Primary Objective is? induction of melanoma antigen-specific CD8+T cells and Secondary Objective is induction of objective? clinical responses. The trial is powered based on the rate of induction of melanoma-specific CD8+T cell? immunity and will accrue up to 51 metastatic melanoma patients. Interim analyses will be conducted after 9? and 24 patients are enrolled to assess toxicity and immunogenicity. Immune responses will be assessed? using EPIMAX strategy. The 2 main quantitative assays involve melanoma antigen-specific IFN-gamma? release (effector memory cells) and cell proliferation (CFSE and flow cytometry; recall memory) by T cells in? short term PBMCs cultures with selected melanoma antigen-peptides.
AIM 3 will determine the breadth and? the quality of melanoma-specific CD8+T cell immunity in patients vaccinated with composite DCs loaded with? killed allogeneic melanoma cells. We will determine 1) the breadth of immune response, i.e. beyond the five? antigens selected for immunomonitoring; 2) the function of elicited CD8+T cells; and 3) the authentic killing of? melanoma tumors in vivo in the OncoHumouse.?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA084512-07
Application #
7631316
Study Section
Subcommittee G - Education (NCI)
Project Start
Project End
Budget Start
2008-06-01
Budget End
2009-05-31
Support Year
7
Fiscal Year
2008
Total Cost
$148,117
Indirect Cost

  Institution

Name
Baylor Research Institute
Department
Type
DUNS #
145745022
City
Dallas
State
TX
Country
United States
Zip Code
75204

  Publications

Speake, Cate; Presnell, Scott; Domico, Kelly et al. (2015) An interactive web application for the dissemination of human systems immunology data. J Transl Med 13:196
Rongvaux, Anthony; Willinger, Tim; Martinek, Jan et al. (2014) Development and function of human innate immune cells in a humanized mouse model. Nat Biotechnol 32:364-72
Palucka, Karolina; Banchereau, Jacques (2013) Human dendritic cell subsets in vaccination. Curr Opin Immunol 25:396-402
Palucka, Karolina; Banchereau, Jacques (2013) Dendritic-cell-based therapeutic cancer vaccines. Immunity 39:38-48
Obermoser, Gerlinde; Presnell, Scott; Domico, Kelly et al. (2013) Systems scale interactive exploration reveals quantitative and qualitative differences in response to influenza and pneumococcal vaccines. Immunity 38:831-44
Banchereau, Jacques; Thompson-Snipes, LuAnn; Zurawski, Sandra et al. (2012) The differential production of cytokines by human Langerhans cells and dermal CD14(+) DCs controls CTL priming. Blood 119:5742-9
Banchereau, Jacques; Zurawski, Sandra; Thompson-Snipes, LuAnn et al. (2012) Immunoglobulin-like transcript receptors on human dermal CD14+ dendritic cells act as a CD8-antagonist to control cytotoxic T cell priming. Proc Natl Acad Sci U S A 109:18885-90
Palucka, Karolina; Banchereau, Jacques (2012) Cancer immunotherapy via dendritic cells. Nat Rev Cancer 12:265-77
Palucka, Karolina; Ueno, Hideki; Roberts, Lee et al. (2011) Dendritic cell subsets as vectors and targets for improved cancer therapy. Curr Top Microbiol Immunol 344:173-92
McNab, Finlay W; Berry, Matthew P R; Graham, Christine M et al. (2011) Programmed death ligand 1 is over-expressed by neutrophils in the blood of patients with active tuberculosis. Eur J Immunol 41:1941-7

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