Monoclonal Anti-MAGE-3 CTL Responses in Melanoma Patients Displaying Tumor Regression after Vaccination with a Recombinant Canarypox Virus

Karanikas, Vaios; Lurquin, Christophe; Colau, Didier; Baren, Nicolas van; Smet, Charles De; Bernard, Loris; Connerotte, Thierry; Corbière, Véronique; Demoitié, Marie-Ange; Líénard, Danielle; Dréno, Brigitte; Velu, Thierry; Boon, Thierry; Coulie, Pierre G.

doi:10.4049/jimmunol.171.9.4898

Cited by 99 publications

(97 citation statements)

References 21 publications

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“…Recent clinical studies could show that an immunotherapy with MAGE peptides had a minimal toxicity and caused induction of tumor-specific CTLs (35)(36)(37)(38). A significant tumor regression could also be observed in several patients, pointing out that a vaccination with a MAGE-A peptide could be promising for the treatment of tumor patients.…”

Section: Bmentioning

confidence: 98%

Promoter Demethylation and Histone Acetylation Mediate Gene Expression of MAGE-A1, -A2, -A3, and -A12 in Human Cancer Cells

Wischnewski

Pantel

Schwarzenbach

2006

Molecular Cancer Research

159

123

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The broad range of expression of cancer-testis antigens in various tumor types makes the proteins encoded by human MAGE gene family promising targets for anticancer immunotherapy. However, a major drawback is their heterogeneous expression. In the current study, we have examined the influence of the DNA methylase inhibitor 5-aza-2 ¶-deoxycytidine (5-aza-CdR) together with the histone deacetylase inhibitor trichostatin A on the expression of MAGE-A1, -A2, -A3, and -A12 genes in different cell lines. Reverse transcription-PCR, Western blot analyses, and immunocytochemical staining show that trichostatin A was able to significantly up-regulate 5-aza-CdR-induced MAGE gene expression. Transient transfection assays with methylated reporter plasmids containing promoter fragments of the different MAGE genes show that trichostatin A was able to overcome gene silencing. In addition, the methylation status of the MAGE promoters was assessed by sodium bisulfite mapping in the various cell lines before and after stimulation with 5-aza-CdR and/or trichostatin A. In contrast to the methylation patterns, which clearly correlated with the basal MAGE RNA transcripts, up-regulation of the MAGE-A mediated by both agents only resulted in a reduction in promoter methylation ranging between 1% and 19%. In conclusion, our data show for the first time that not only hypermethylation but also histone deacetylation is responsible for the mechanism underlying MAGE gene silencing.

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Section: Bmentioning

confidence: 98%

Promoter Demethylation and Histone Acetylation Mediate Gene Expression of MAGE-A1, -A2, -A3, and -A12 in Human Cancer Cells

Wischnewski

Pantel

Schwarzenbach

2006

Molecular Cancer Research

159

123

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“…After washing, they were distributed at 1 ϫ 10 4 -3 ϫ 10 4 cells/0.2 ml in microwells containing Iscove's medium with 10% HS, IL-2 (20 U/ml), IL-7 (10 ng/ml; R&D Systems, Minneapolis, MN). At variance with Karanikas et al (6), MAGE-3.A1 peptide at 1 M was added to the microculture. In some experiments, IL-4 was added at 10 U/ml.…”

Section: In Vitro Peptide Stimulation Of Pbmc (Mixed Lymphocyte-peptimentioning

confidence: 99%

“…CD8 ϩ tetramer ϩ cells were sorted, cloned at one cell per well, and restimulated under conditions that were very similar to those described by Karanikas et al (6), with some differences in the number of stimulator cells and the cells used as feeder cells. Sorted cells were stimulated by the addition of irradiated (100 Gy) peptide-pulsed (20 M for 60 min at room temperature, washed) cells, either 10 4 MZ2-MEL-3.0 HLA-A1 melanoma cells or 3 ϫ 10 4 allogenic HLA-A1 EBV-transformed B cells.…”

Section: Ex Vivo Sorting Of Tetramer-positive Cellsmentioning

confidence: 99%

“…We resorted to an approach based on stimulation of blood lymphocyte microcultures with the antigenic peptide, followed by labeling of the microcultures with an A1/MAGE-3 tetramer (5). Among 10 regressing HLA-A1 patients who were evaluated, 5 showed an anti-MAGE-3.A1 CTL response (5,6). The intensity of these responses varied widely, with CTL precursor (CTLp) 3 frequencies ranging from 4 ϫ 10 Ϫ7 to 10 Ϫ3 among blood CD8 cells.…”

mentioning

confidence: 99%

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Polyclonal CTL Responses Observed in Melanoma Patients Vaccinated with Dendritic Cells Pulsed with a MAGE-3.A1 Peptide

Godelaine

Carrasco

Lucas

et al. 2003

The Journal of Immunology

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Vaccination with mature, monocyte-derived dendritic cells (DC) pulsed with the MAGE-3168–176 peptide, which is presented by HLA-A1, has been reported to induce tumor regressions and CTL in some advanced stage IV melanoma patients. We present here a precise evaluation of the level of some of these anti-MAGE-3.A1 CTL responses and an analysis of their clonal diversity. Blood lymphocytes were stimulated with the MAGE-3.A1 peptide under limiting dilution conditions and assayed with an A1/MAGE-3 tetramer. This was followed by the cloning of the tetramer-positive cells and by TCR sequence analysis of the CTL clones that lysed targets expressing MAGE-3.A1. We also used direct ex vivo tetramer staining of CD8 cells, sorting, and cloning of the positive cells. In three patients who showed regression of some of their metastases after vaccination, CTL responses were observed with frequencies ranging from 7 × 10−6 to 9 × 10−4 of CD8+ blood T lymphocytes, representing an increase of 20- to 400-fold of the frequencies found before immunization. A fourth patient showed neither tumor regression nor an anti-MAGE-3.A1 CTL response. In each of the responses, several CTL clones were amplified. This polyclonality contrasts with the monoclonality of the CTL responses observed in patients vaccinated with MAGE-3.A1 peptide or with an ALVAC recombinant virus coding for this antigenic peptide.

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“…Melanoma patient EB81 showed complete regression of cutaneous metastatic lesions after repetitive vaccination with a recombinant canarypox virus of the ALVAC type encoding 2 HLA-A1-restricted peptides derived from MAGE-A1 and MAGE-A3. 14,15 This regression has been durable and was associated with a monoclonal CTL response to one of the vaccine antigens, the MAGE-A3 peptide. We established a tumor cell line from an invaded lymph node that had been resected from this patient, and we used it to stimulate autologous blood lymphocytes collected at the time of tumor regression.…”

mentioning

confidence: 99%

Two new tumor‐specific antigenic peptides encoded by gene MAGE‐C2 and presented to cytolytic T lymphocytes by HLA‐A2

Germeau

Vigneron

et al. 2004

Intl Journal of Cancer

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Monoclonal Anti-MAGE-3 CTL Responses in Melanoma Patients Displaying Tumor Regression after Vaccination with a Recombinant Canarypox Virus

Cited by 99 publications

References 21 publications

Promoter Demethylation and Histone Acetylation Mediate Gene Expression of MAGE-A1, -A2, -A3, and -A12 in Human Cancer Cells

Promoter Demethylation and Histone Acetylation Mediate Gene Expression of MAGE-A1, -A2, -A3, and -A12 in Human Cancer Cells

Polyclonal CTL Responses Observed in Melanoma Patients Vaccinated with Dendritic Cells Pulsed with a MAGE-3.A1 Peptide

Two new tumor‐specific antigenic peptides encoded by gene MAGE‐C2 and presented to cytolytic T lymphocytes by HLA‐A2

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