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Immunogenicity, including vitiligo, and feasibility of vaccination with autologous GM-CSF-transduced tumor cells in metastatic melanoma patients.

Rosalie M Luiten ,
Esther W M Kueter ,
Wolter Mooi ,
Maarten P W Gallee ,
Elaine M Rankin ,
Winald R Gerritsen ,
Shirley M Clift ,
Willem J Nooijen ,
Pauline Weder ,
Willeke F van de Kasteele ,
Johan Sein ,
Paul C M van den Berk ,
Omgo E Nieweg ,
Anton M Berns ,
Hergen Spits ,
Gijsbert C de Gast

Abstract

PATIENTS AND METHODS

Sixty-four patients were randomly assigned to receive three vaccinations of high-dose or low-dose tumor cells at 3-week intervals. Tumor cell vaccine preparation succeeded for 56 patients (88%), but because of progressive disease, the well-tolerated vaccination was completed in only 28 patients. We analyzed the priming of T cells against melanoma antigens, MART-1, tyrosinase, gp100, MAGE-A1, and MAGE-A3 using human leukocyte antigen/peptide tetramers and functional assays.

CONCLUSION

We conclude that vaccination with GM-CSF-transduced autologous tumor cells has limited toxicity and can enhance T-cell activation against melanocyte differentiation antigens, which can lead to vitiligo. Whether the induction of autoimmune vitiligo may prolong disease-free survival of metastatic melanoma patients who are surgically rendered as having no evidence of disease before vaccination is worthy of further investigation.

RESULTS

The high-dose vaccination induced the infiltration of T cells into the tumor tissue. Three of 14 patients receiving the high-dose vaccine showed an increase in MART-1- or gp100-specific T cells in the peripheral blood during vaccination. Six patients experienced disease-free survival for more than 5 years, and two of these patients developed vitiligo at multiple sites after vaccination. MART-1- and gp100-specific T cells were found infiltrating in vitiligo skin. Upon vaccination, the T cells acquired an effector phenotype and produced interferon-gamma on specific antigenic stimulation.

PURPOSE

To determine the feasibility, toxicity, and immunologic effects of vaccination with autologous tumor cells retrovirally transduced with the GM-CSF gene, we performed a phase I/II vaccination study in stage IV metastatic melanoma patients.

More about this publication

Journal of clinical oncology : official journal of the American Society of Clinical Oncology

Volume 23
Issue nr. 35
Pages 8978-91
Publication date 10-12-2005

Full text links

Publisher website (DOI) 10.1200/JCO.2005.01.6816
Europe PubMed Central 16260696
Pubmed 16260696

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