Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells

BACKGROUND: Metastatic, chemotherapy-resistant melanoma is an intractable cancer with a very poor prognosis. As to immunotherapy targeting metastatic melanoma, HLA-A2(+ )patients were mainly enrolled in the study in Western countries. However, HLA-A24(+ )melanoma patients-oriented immunotherapy has...

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Autores principales: Akiyama, Yasuto, Tanosaki, Ryuji, Inoue, Naoki, Shimada, Makiko, Hotate, Yukie, Yamamoto, Akifumi, Yamazaki, Naoya, Kawashima, Ichiro, Nukaya, Ikuei, Takesako, Kazutoh, Maruyama, Kouji, Takaue, Yoichi, Yamaguchi, Ken
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2005
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC549033/
https://www.ncbi.nlm.nih.gov/pubmed/15676080
http://dx.doi.org/10.1186/1479-5876-3-4
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author Akiyama, Yasuto
Tanosaki, Ryuji
Inoue, Naoki
Shimada, Makiko
Hotate, Yukie
Yamamoto, Akifumi
Yamazaki, Naoya
Kawashima, Ichiro
Nukaya, Ikuei
Takesako, Kazutoh
Maruyama, Kouji
Takaue, Yoichi
Yamaguchi, Ken
author_facet Akiyama, Yasuto
Tanosaki, Ryuji
Inoue, Naoki
Shimada, Makiko
Hotate, Yukie
Yamamoto, Akifumi
Yamazaki, Naoya
Kawashima, Ichiro
Nukaya, Ikuei
Takesako, Kazutoh
Maruyama, Kouji
Takaue, Yoichi
Yamaguchi, Ken
author_sort Akiyama, Yasuto
collection PubMed
description BACKGROUND: Metastatic, chemotherapy-resistant melanoma is an intractable cancer with a very poor prognosis. As to immunotherapy targeting metastatic melanoma, HLA-A2(+ )patients were mainly enrolled in the study in Western countries. However, HLA-A24(+ )melanoma patients-oriented immunotherapy has not been fully investigated. In the present study, we investigated the effect of dendritic cell (DC)-based immunotherapy on metastatic melanoma patients with HLA-A2 or A24 genotype. METHODS: Nine cases of metastatic melanoma were enrolled into a phase I study of monocyte-derived dendritic cell (DC)-based immunotherapy. HLA-genotype analysis revealed 4 cases of HLA-A*0201, 1 of A*0206 and 4 of A*2402. Enriched monocytes were obtained using OptiPrep™ from leukapheresis products, and then incubated with GM-CSF and IL-4 in a closed serum-free system. After pulsing with a cocktail of 5 melanoma-associated synthetic peptides (gp100, tyrosinase, MAGE-2, MAGE-3 and MART-1 or MAGE-1) restricted to HLA-A2 or A24 and KLH, cells were cryopreserved until used. Finally, thawed DCs were washed and injected subcutaneously (s.c.) into the inguinal region in a dose-escalation manner. RESULTS: The mean percentage of DCs rated as lin(-)HLA-DR(+ )in melanoma patients was 46.4 ± 15.6 %. Most of DCs expressed high level of co-stimulatory molecules and type1 phenotype (CD11c(+)HLA-DR(+)), while a moderate number of mature DCs with CD83 and CCR7 positive were contained in DC products. DC injections were well tolerated except for transient liver dysfunction (elevation of transaminases, Grade I-II). All 6 evaluable cases except for early PD showed positive immunological responses to more than 2 melanoma peptides in an ELISPOT assay. Two representative responders demonstrated strong HLA-class I protein expression in the tumor and very high scores of ELISPOT that might correlate to the regression of metastatic tumors. Clinical response through DC injections was as follows : 1CR, 1 PR, 1SD and 6 PD. All 59 DC injections in the phase I study were tolerable in terms of safety, however, the maximal tolerable dose of DCs was not determined. CONCLUSIONS: These results suggested that peptide cocktail-treated DC-based immunotherapy had the potential for utilizing as one of therapeutic tools against metastatic melanoma in Japan.
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spelling pubmed-5490332005-02-18 Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells Akiyama, Yasuto Tanosaki, Ryuji Inoue, Naoki Shimada, Makiko Hotate, Yukie Yamamoto, Akifumi Yamazaki, Naoya Kawashima, Ichiro Nukaya, Ikuei Takesako, Kazutoh Maruyama, Kouji Takaue, Yoichi Yamaguchi, Ken J Transl Med Research BACKGROUND: Metastatic, chemotherapy-resistant melanoma is an intractable cancer with a very poor prognosis. As to immunotherapy targeting metastatic melanoma, HLA-A2(+ )patients were mainly enrolled in the study in Western countries. However, HLA-A24(+ )melanoma patients-oriented immunotherapy has not been fully investigated. In the present study, we investigated the effect of dendritic cell (DC)-based immunotherapy on metastatic melanoma patients with HLA-A2 or A24 genotype. METHODS: Nine cases of metastatic melanoma were enrolled into a phase I study of monocyte-derived dendritic cell (DC)-based immunotherapy. HLA-genotype analysis revealed 4 cases of HLA-A*0201, 1 of A*0206 and 4 of A*2402. Enriched monocytes were obtained using OptiPrep™ from leukapheresis products, and then incubated with GM-CSF and IL-4 in a closed serum-free system. After pulsing with a cocktail of 5 melanoma-associated synthetic peptides (gp100, tyrosinase, MAGE-2, MAGE-3 and MART-1 or MAGE-1) restricted to HLA-A2 or A24 and KLH, cells were cryopreserved until used. Finally, thawed DCs were washed and injected subcutaneously (s.c.) into the inguinal region in a dose-escalation manner. RESULTS: The mean percentage of DCs rated as lin(-)HLA-DR(+ )in melanoma patients was 46.4 ± 15.6 %. Most of DCs expressed high level of co-stimulatory molecules and type1 phenotype (CD11c(+)HLA-DR(+)), while a moderate number of mature DCs with CD83 and CCR7 positive were contained in DC products. DC injections were well tolerated except for transient liver dysfunction (elevation of transaminases, Grade I-II). All 6 evaluable cases except for early PD showed positive immunological responses to more than 2 melanoma peptides in an ELISPOT assay. Two representative responders demonstrated strong HLA-class I protein expression in the tumor and very high scores of ELISPOT that might correlate to the regression of metastatic tumors. Clinical response through DC injections was as follows : 1CR, 1 PR, 1SD and 6 PD. All 59 DC injections in the phase I study were tolerable in terms of safety, however, the maximal tolerable dose of DCs was not determined. CONCLUSIONS: These results suggested that peptide cocktail-treated DC-based immunotherapy had the potential for utilizing as one of therapeutic tools against metastatic melanoma in Japan. BioMed Central 2005-01-28 /pmc/articles/PMC549033/ /pubmed/15676080 http://dx.doi.org/10.1186/1479-5876-3-4 Text en Copyright © 2005 Akiyama 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
Akiyama, Yasuto
Tanosaki, Ryuji
Inoue, Naoki
Shimada, Makiko
Hotate, Yukie
Yamamoto, Akifumi
Yamazaki, Naoya
Kawashima, Ichiro
Nukaya, Ikuei
Takesako, Kazutoh
Maruyama, Kouji
Takaue, Yoichi
Yamaguchi, Ken
Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title_full Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title_fullStr Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title_full_unstemmed Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title_short Clinical response in Japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
title_sort clinical response in japanese metastatic melanoma patients treated with peptide cocktail-pulsed dendritic cells
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC549033/
https://www.ncbi.nlm.nih.gov/pubmed/15676080
http://dx.doi.org/10.1186/1479-5876-3-4
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