First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients

BACKGROUND: DepoVax(TM) is a novel non-emulsion depot-forming vaccine platform with the capacity to significantly enhance the immunogenicity of peptide cancer antigens. Naturally processed HLA-A2 restricted peptides presented by breast, ovarian and prostate cancer cells were used as antigens to crea...

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Autores principales: Berinstein, Neil L, Karkada, Mohan, Morse, Michael A, Nemunaitis, John J, Chatta, Gurkamal, Kaufman, Howard, Odunsi, Kunle, Nigam, Rita, Sammatur, Leeladhar, MacDonald, Lisa D, Weir, Genevieve M, Stanford, Marianne M, Mansour, Marc
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3479010/
https://www.ncbi.nlm.nih.gov/pubmed/22862954
http://dx.doi.org/10.1186/1479-5876-10-156
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author Berinstein, Neil L
Karkada, Mohan
Morse, Michael A
Nemunaitis, John J
Chatta, Gurkamal
Kaufman, Howard
Odunsi, Kunle
Nigam, Rita
Sammatur, Leeladhar
MacDonald, Lisa D
Weir, Genevieve M
Stanford, Marianne M
Mansour, Marc
author_facet Berinstein, Neil L
Karkada, Mohan
Morse, Michael A
Nemunaitis, John J
Chatta, Gurkamal
Kaufman, Howard
Odunsi, Kunle
Nigam, Rita
Sammatur, Leeladhar
MacDonald, Lisa D
Weir, Genevieve M
Stanford, Marianne M
Mansour, Marc
author_sort Berinstein, Neil L
collection PubMed
description BACKGROUND: DepoVax(TM) is a novel non-emulsion depot-forming vaccine platform with the capacity to significantly enhance the immunogenicity of peptide cancer antigens. Naturally processed HLA-A2 restricted peptides presented by breast, ovarian and prostate cancer cells were used as antigens to create a therapeutic cancer vaccine, DPX-0907. METHODS: A phase I clinical study was designed to examine the safety and immune activating potential of DPX-0907 in advanced stage breast, ovarian and prostate cancer patients. A total of 23 late stage cancer patients were recruited and were divided into two dose/volume cohorts in a three immunization protocol. RESULTS: DPX-0907 was shown to be safe with injection site reactions being the most commonly reported adverse event. All breast cancer patients (3/3), most of ovarian (5/6) and one third of prostate (3/9) cancer patients exhibited detectable immune responses, resulting in a 61% immunological response rate. Immune responses were generally observed in patients with better disease control after their last prior treatment. Antigen-specific responses were detected in 73% of immune responders (44% of evaluable patients) after the first vaccination. In 83% of immune responders (50% of evaluable patients), peptide-specific T cell responses were detected at ≥2 time points post vaccination with 64% of the responders (39% of evaluable patients) showing evidence of immune persistence. Immune monitoring also demonstrated the generation of antigen-specific T cell memory with the ability to secrete multiple Type 1 cytokines. CONCLUSIONS: The novel DepoVax formulation promotes multifunctional effector memory responses to peptide-based tumor associated antigens. The data supports the capacity of DPX-0907 to elicit Type-1 biased immune responses, warranting further clinical development of the vaccine. This study underscores the importance of applying vaccines in clinical settings in which patients are more likely to be immune competent. TRIAL REGISTRATION: ClinicalTrials.gov NCT01095848
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spelling pubmed-34790102012-10-24 First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients Berinstein, Neil L Karkada, Mohan Morse, Michael A Nemunaitis, John J Chatta, Gurkamal Kaufman, Howard Odunsi, Kunle Nigam, Rita Sammatur, Leeladhar MacDonald, Lisa D Weir, Genevieve M Stanford, Marianne M Mansour, Marc J Transl Med Research BACKGROUND: DepoVax(TM) is a novel non-emulsion depot-forming vaccine platform with the capacity to significantly enhance the immunogenicity of peptide cancer antigens. Naturally processed HLA-A2 restricted peptides presented by breast, ovarian and prostate cancer cells were used as antigens to create a therapeutic cancer vaccine, DPX-0907. METHODS: A phase I clinical study was designed to examine the safety and immune activating potential of DPX-0907 in advanced stage breast, ovarian and prostate cancer patients. A total of 23 late stage cancer patients were recruited and were divided into two dose/volume cohorts in a three immunization protocol. RESULTS: DPX-0907 was shown to be safe with injection site reactions being the most commonly reported adverse event. All breast cancer patients (3/3), most of ovarian (5/6) and one third of prostate (3/9) cancer patients exhibited detectable immune responses, resulting in a 61% immunological response rate. Immune responses were generally observed in patients with better disease control after their last prior treatment. Antigen-specific responses were detected in 73% of immune responders (44% of evaluable patients) after the first vaccination. In 83% of immune responders (50% of evaluable patients), peptide-specific T cell responses were detected at ≥2 time points post vaccination with 64% of the responders (39% of evaluable patients) showing evidence of immune persistence. Immune monitoring also demonstrated the generation of antigen-specific T cell memory with the ability to secrete multiple Type 1 cytokines. CONCLUSIONS: The novel DepoVax formulation promotes multifunctional effector memory responses to peptide-based tumor associated antigens. The data supports the capacity of DPX-0907 to elicit Type-1 biased immune responses, warranting further clinical development of the vaccine. This study underscores the importance of applying vaccines in clinical settings in which patients are more likely to be immune competent. TRIAL REGISTRATION: ClinicalTrials.gov NCT01095848 BioMed Central 2012-08-03 /pmc/articles/PMC3479010/ /pubmed/22862954 http://dx.doi.org/10.1186/1479-5876-10-156 Text en Copyright ©2012 Berinstein et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Berinstein, Neil L
Karkada, Mohan
Morse, Michael A
Nemunaitis, John J
Chatta, Gurkamal
Kaufman, Howard
Odunsi, Kunle
Nigam, Rita
Sammatur, Leeladhar
MacDonald, Lisa D
Weir, Genevieve M
Stanford, Marianne M
Mansour, Marc
First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title_full First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title_fullStr First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title_full_unstemmed First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title_short First-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional T cell responses in ovarian, breast and prostate cancer patients
title_sort first-in-man application of a novel therapeutic cancer vaccine formulation with the capacity to induce multi-functional t cell responses in ovarian, breast and prostate cancer patients
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3479010/
https://www.ncbi.nlm.nih.gov/pubmed/22862954
http://dx.doi.org/10.1186/1479-5876-10-156
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