Your search keyword '"Joel Lohr"' showing total 4 results

1. Multiple antigen-engineered DC vaccines with or without IFNα to promote antitumor immunity in melanoma

Author

Lisa H. Butterfield, Lazar Vujanovic, Patricia M. Santos, Deena M. Maurer, Andrea Gambotto, Joel Lohr, Chunlei Li, Jacob Waldman, Uma Chandran, Yan Lin, Huang Lin, Hussein A. Tawbi, Ahmad A. Tarhini, and John M. Kirkwood

Subjects

Cancer vaccine, Immune biomarkers, Tumor immunity, Shared antigens, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Cancer vaccines are designed to promote systemic antitumor immunity and tumor eradication. Cancer vaccination may be more efficacious in combination with additional interventions that may build on or amplify their effects. Methods Based on our previous clinical and in vitro studies, we designed an antigen-engineered DC vaccine trial to promote a polyclonal CD8+ and CD4+ T cell response against three shared melanoma antigens. The 35 vaccine recipients were then randomized to receive one month of high-dose IFNα or observation. Results The resulting clinical outcomes were 2 partial responses, 8 stable disease and 14 progressive disease among patients with measurable disease using RECIST 1.1, and, of 11 surgically treated patients with no evidence of disease (NED), 4 remain NED at a median follow-up of 3 years. The majority of vaccinated patients showed an increase in vaccine antigen-specific CD8+ and CD4+ T cell responses. The addition of IFNα did not appear to improve immune or clinical responses in this trial. Examination of the DC vaccine profiles showed that IL-12p70 secretion did not correlate with immune or clinical responses. In depth immune biomarker studies support the importance of circulating Treg and MDSC for development of antigen-specific T cell responses, and of circulating CD8+ and CD4+ T cell subsets in clinical responses. Conclusions DC vaccines are a safe and reliable platform for promoting antitumor immunity. This combination with one month of high dose IFNα did not improve outcomes. Immune biomarker analysis in the blood identified several predictive and prognostic biomarkers for further analysis, including MDSC. Trial registration NCT01622933.

Published

2019

2. CD56dim CD16− Natural Killer Cell Profiling in Melanoma Patients Receiving a Cancer Vaccine and Interferon-α

Author

Lazar Vujanovic, Christopher Chuckran, Yan Lin, Fei Ding, Cindy A. Sander, Patricia M. Santos, Joel Lohr, Afshin Mashadi-Hossein, Sarah Warren, Andy White, Alan Huang, John M. Kirkwood, and Lisa H. Butterfield

Subjects

melanoma, CD56dim CD16−, natural killer cell subsets, dendritic cells, recombinant adenoviral vector, interferon-α, Immunologic diseases. Allergy, RC581-607

Abstract

Natural killer (NK) cells are innate cytotoxic and immunoregulatory lymphocytes that have a central role in anti-tumor immunity and play a critical role in mediating cellular immunity in advanced cancer immunotherapies, such as dendritic cell (DC) vaccines. Our group recently tested a novel recombinant adenovirus-transduced autologous DC-based vaccine that simultaneously induces T cell responses against three melanoma-associated antigens for advanced melanoma patients. Here, we examine the impact of this vaccine as well as the subsequent systemic delivery of high-dose interferon-α2b (HDI) on the circulatory NK cell profile in melanoma patients. At baseline, patient NK cells, particularly those isolated from high-risk patients with no measurable disease, showed altered distribution of CD56dim CD16+ and CD56dim CD16− NK cell subsets, as well as elevated serum levels of immune suppressive MICA, TN5E/CD73 and tactile/CD96, and perforin. Surprisingly, patient NK cells displayed a higher level of activation than those from healthy donors as measured by elevated CD69, NKp44 and CCR7 levels, and enhanced K562 killing. Elevated cytolytic ability strongly correlated with increased representation of CD56dim CD16+ NK cells and amplified CD69 expression on CD56dim CD16+ NK cells. While intradermal DC immunizations did not significantly impact circulatory NK cell activation and distribution profiles, subsequent HDI injections enhanced CD56bright CD16− NK cell numbers when compared to patients that did not receive HDI. Phenotypic analysis of tumor-infiltrating NK cells showed that CD56dim CD16− NK cells are the dominant subset in melanoma tumors. NanoString transcriptomic analysis of melanomas resected at baseline indicated that there was a trend of increased CD56dim NK cell gene signature expression in patients with better clinical response. These data indicate that melanoma patient blood NK cells display elevated activation levels, that intra-dermal DC immunizations did not effectively promote systemic NK cell responses, that systemic HDI administration can modulate NK cell subset distributions and suggest that CD56dim CD16− NK cells are a unique non-cytolytic subset in melanoma patients that may associate with better patient outcome.

Published

2019

3. Multiple antigen-engineered DC vaccines with or without IFNα to promote antitumor immunity in melanoma

Author

John M. Kirkwood, Yan Lin, Huang Lin, Lisa H. Butterfield, Hussein Tawbi, Uma R. Chandran, Ahmad A. Tarhini, Chunlei Li, Andrea Gambotto, Lazar Vujanovic, Jacob K. Waldman, Joel Lohr, Patricia M. Santos, and Deena M. Maurer

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Male, and promotion of well-being, Cancer Research, Skin Neoplasms, CD8-Positive T-Lymphocytes, Protein Engineering, 0302 clinical medicine, Immunogenicity, Vaccine, Tumor immunity, 80 and over, Cancer vaccine, Immunology and Allergy, Medicine, Melanoma, Cancer, Aged, 80 and over, Vaccines, Vaccines, Synthetic, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Prognosis, Immunogenicity, Combined Modality Therapy, Progression-Free Survival, 3. Good health, Vaccination, medicine.anatomical_structure, 3.4 Vaccines, Oncology, 030220 oncology & carcinogenesis, HIV/AIDS, Molecular Medicine, Biomarker (medicine), Female, Drug, Biotechnology, Research Article, Adult, T cell, Clinical Trials and Supportive Activities, Immunology, Shared antigens, lcsh:RC254-282, Cancer Vaccines, Dose-Response Relationship, Vaccine Related, 03 medical and health sciences, Immune system, Antigen, Clinical Research, Antigens, Neoplasm, Humans, Antigens, Response Evaluation Criteria in Solid Tumors, Aged, Pharmacology, Dose-Response Relationship, Drug, business.industry, Prevention, Inflammatory and immune system, Synthetic, Interferon-alpha, Dendritic Cells, Prevention of disease and conditions, medicine.disease, Immune biomarkers, Good Health and Well Being, 030104 developmental biology, Neoplasm, Immunization, business, Vaccine, CD8, Follow-Up Studies

Abstract

Background Cancer vaccines are designed to promote systemic antitumor immunity and tumor eradication. Cancer vaccination may be more efficacious in combination with additional interventions that may build on or amplify their effects. Methods Based on our previous clinical and in vitro studies, we designed an antigen-engineered DC vaccine trial to promote a polyclonal CD8+ and CD4+ T cell response against three shared melanoma antigens. The 35 vaccine recipients were then randomized to receive one month of high-dose IFNα or observation. Results The resulting clinical outcomes were 2 partial responses, 8 stable disease and 14 progressive disease among patients with measurable disease using RECIST 1.1, and, of 11 surgically treated patients with no evidence of disease (NED), 4 remain NED at a median follow-up of 3 years. The majority of vaccinated patients showed an increase in vaccine antigen-specific CD8+ and CD4+ T cell responses. The addition of IFNα did not appear to improve immune or clinical responses in this trial. Examination of the DC vaccine profiles showed that IL-12p70 secretion did not correlate with immune or clinical responses. In depth immune biomarker studies support the importance of circulating Treg and MDSC for development of antigen-specific T cell responses, and of circulating CD8+ and CD4+ T cell subsets in clinical responses. Conclusions DC vaccines are a safe and reliable platform for promoting antitumor immunity. This combination with one month of high dose IFNα did not improve outcomes. Immune biomarker analysis in the blood identified several predictive and prognostic biomarkers for further analysis, including MDSC. Trial registration NCT01622933. Electronic supplementary material The online version of this article (10.1186/s40425-019-0552-x) contains supplementary material, which is available to authorized users.

Published

2019

4. CD56

Author

Lazar, Vujanovic, Christopher, Chuckran, Yan, Lin, Fei, Ding, Cindy A, Sander, Patricia M, Santos, Joel, Lohr, Afshin, Mashadi-Hossein, Sarah, Warren, Andy, White, Alan, Huang, John M, Kirkwood, and Lisa H, Butterfield

Subjects

Cytotoxicity, Immunologic, recombinant adenoviral vector, Immunology, Antigen-Presenting Cells, chemical and pharmacologic phenomena, Lymphocyte Activation, Cancer Vaccines, Immunophenotyping, CD56dim CD16−, interferon-α, natural killer cell subsets, Tumor Microenvironment, melanoma, Humans, dendritic cells, Neoplasm Staging, Original Research, Antigen Presentation, Clinical Trials, Phase I as Topic, Receptors, IgG, Interferon-alpha, Combined Modality Therapy, CD56 Antigen, Killer Cells, Natural, Treatment Outcome, Immunotherapy, Biomarkers

Abstract

Natural killer (NK) cells are innate cytotoxic and immunoregulatory lymphocytes that have a central role in anti-tumor immunity and play a critical role in mediating cellular immunity in advanced cancer immunotherapies, such as dendritic cell (DC) vaccines. Our group recently tested a novel recombinant adenovirus-transduced autologous DC-based vaccine that simultaneously induces T cell responses against three melanoma-associated antigens for advanced melanoma patients. Here, we examine the impact of this vaccine as well as the subsequent systemic delivery of high-dose interferon-α2b (HDI) on the circulatory NK cell profile in melanoma patients. At baseline, patient NK cells, particularly those isolated from high-risk patients with no measurable disease, showed altered distribution of CD56dim CD16+ and CD56dim CD16− NK cell subsets, as well as elevated serum levels of immune suppressive MICA, TN5E/CD73 and tactile/CD96, and perforin. Surprisingly, patient NK cells displayed a higher level of activation than those from healthy donors as measured by elevated CD69, NKp44 and CCR7 levels, and enhanced K562 killing. Elevated cytolytic ability strongly correlated with increased representation of CD56dim CD16+ NK cells and amplified CD69 expression on CD56dim CD16+ NK cells. While intradermal DC immunizations did not significantly impact circulatory NK cell activation and distribution profiles, subsequent HDI injections enhanced CD56bright CD16− NK cell numbers when compared to patients that did not receive HDI. Phenotypic analysis of tumor-infiltrating NK cells showed that CD56dim CD16− NK cells are the dominant subset in melanoma tumors. NanoString transcriptomic analysis of melanomas resected at baseline indicated that there was a trend of increased CD56dim NK cell gene signature expression in patients with better clinical response. These data indicate that melanoma patient blood NK cells display elevated activation levels, that intra-dermal DC immunizations did not effectively promote systemic NK cell responses, that systemic HDI administration can modulate NK cell subset distributions and suggest that CD56dim CD16− NK cells are a unique non-cytolytic subset in melanoma patients that may associate with better patient outcome.

Published

2018