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01.06.2003 | Original Article

Durable complete clinical responses in a phase I/II trial using an autologous melanoma cell/dendritic cell vaccine

verfasst von: Michael G. E. O'Rourke, Maree Johnson, Catherine Lanagan, Janet See, Jie Yang, John R. Bell, Greg J. Slater, Beverley M. Kerr, Beth Crowe, David M. Purdie, Suzanne L. Elliott, Kay A. O. Ellem, Christopher W. Schmidt

Erschienen in: Cancer Immunology, Immunotherapy | Ausgabe 6/2003

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Abstract

Advanced metastatic melanoma is incurable by standard treatments, but occasionally responds to immunotherapy. Recent trials using dendritic cells (DC) as a cellular adjuvant have concentrated on defined peptides as the source of antigens, and rely on foreign proteins as a source of help to generate a cell-mediated immune response. This approach limits patient accrual, because currently defined, non-mutated epitopes are restricted by a small number of human leucocyte antigens. It also fails to take advantage of mutated epitopes peculiar to the patient's own tumour, and of CD4+ T lymphocytes as potential effectors of anti-tumour immunity. We therefore sought to determine whether a fully autologous DC vaccine is feasible, and of therapeutic benefit. Patients with American Joint Cancer Committee stage IV melanoma were treated with a fully autologous immunotherapy consisting of monocyte-derived DC, matured after culture with irradiated tumour cells. Of 19 patients enrolled into the trial, sufficient tumour was available to make treatments for 17. Of these, 12 received a complete priming phase of six cycles of either 0.9×10⁶ or 5×10⁶ DC/intradermal injection, at 2-weekly intervals. Where possible, treatment continued with the lower dose at 6-weekly intervals. The remaining five patients could not complete priming, due to progressive disease. Three of the 12 patients who completed priming have durable complete responses (average duration 35 months+), three had partial responses, and the remaining six had progressive disease (WHO criteria). Disease regression was not correlated with dose or with the development of delayed type hypersensitivity responses to intradermal challenge with irradiated, autologous tumour. However, plasma S-100B levels prior to the commencement of treatment correlated with objective clinical response (P=0.05) and survival (log rank P<0.001). The treatment had minimal side-effects and was well tolerated by all patients. Mature, monocyte-derived DC preparations exposed to appropriate tumour antigen sources can be reliably produced for patients with advanced metastatic melanoma, and in a subset of those patients with lower volume disease their repeated administration results in durable complete responses.

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Titel: Durable complete clinical responses in a phase I/II trial using an autologous melanoma cell/dendritic cell vaccine
verfasst von: Michael G. E. O'Rourke
Maree Johnson
Catherine Lanagan
Janet See
Jie Yang
John R. Bell
Greg J. Slater
Beverley M. Kerr
Beth Crowe
David M. Purdie
Suzanne L. Elliott
Kay A. O. Ellem
Christopher W. Schmidt
Publikationsdatum: 01.06.2003
Verlag: Springer-Verlag
Erschienen in: Cancer Immunology, Immunotherapy / Ausgabe 6/2003
Print ISSN: 0340-7004
Elektronische ISSN: 1432-0851
DOI: https://doi.org/10.1007/s00262-003-0375-x

Neu im Fachgebiet Onkologie

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Springer Medizin

Durable complete clinical responses in a phase I/II trial using an autologous melanoma cell/dendritic cell vaccine

Abstract

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