The immunological response and post-treatment survival of DC-vaccinated melanoma patients are associated with increased Th1/Th17 and reduced Th3 cytokine responses
Author
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Durán Aniotz, Claudia
Author
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Segal, Gabriela
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Author
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Salazar, Lorena
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Pereda, Cristián
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Author
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Falcón, Cristián
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Author
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Tempio, Fabián
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Author
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Aguilera, Raquel
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Author
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González González, Rodrigo
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Author
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Pérez Núñez, Claudio
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Author
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Tittarelli, Andrés
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Author
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Catalán Martina, Diego
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Author
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Nervi, Bruno
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Author
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Larrondo Lillo, Milton
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Author
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Salazar Onfray, Flavio
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Author
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López Nitsche, Mercedes
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Admission date
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2014-01-29T12:29:25Z
Available date
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2014-01-29T12:29:25Z
Publication date
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2013
Cita de ítem
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Cancer Immunol Immunother (2013) 62:761–772
en_US
Identifier
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DOI 10.1007/s00262-012-1377-3
Identifier
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https://repositorio.uchile.cl/handle/2250/129202
General note
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Artículo de publicación ISI
en_US
Abstract
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Introduction Immunization with autologous dendritic
cells (DCs) loaded with a heat shock-conditioned allogeneic
melanoma cell lysate caused lysate-specific delayed
type hypersensitivity (DTH) reactions in a number of
patients. These responses correlated with a threefold prolonged
long-term survival of DTH? with respect to DTH-
unresponsive patients. Herein, we investigated whether the
immunological reactions associated with prolonged survival
were related to dissimilar cellular and cytokine
responses in blood.
Materials and methods Healthy donors and melanoma
patient’s lymphocytes obtained from blood before and after
vaccinations and from DTH biopsies were analyzed for T
cell population distribution and cytokine release.
Results/discussion Peripheral blood lymphocytes from
melanoma patients have an increased proportion of Th3
(CD4? TGF-b?) regulatory T lymphocytes compared with
healthy donors. Notably, DTH? patients showed a threefold
reduction of Th3 cells compared with DTH- patients after
DCs vaccine treatment. Furthermore, DCs vaccination
resulted in a threefold augment of the proportion of IFN-c
releasing Th1 cells and in a twofold increase of the
IL-17-producing Th17 population in DTH? with respect to
DTH- patients. Increased Th1 and Th17 cell populations in
both blood and DTH-derived tissues suggest that these
profiles may be related to a more effective anti-melanoma
response.
Conclusions Our results indicate that increased proinflammatory
cytokine profiles are related to detectable
immunological responses in vivo (DTH) and to prolonged
patient survival. Our study contributes to the understanding
of immunological responses produced by DCs vaccines and
to the identification of follow-up markers for patient outcome
that may allow a closer individual monitoring of patients.
The immunological response and post-treatment survival of DC-vaccinated melanoma patients are associated with increased Th1/Th17 and reduced Th3 cytokine responses