Uptake and presentation of malignant glioma tumor cell lysates by monocyte-derived dendritic cells

被引:0
作者
Steven De Vleeschouwer
Mohammed Arredouani
Martine Adé
Pascal Cadot
Elke Vermassen
Jan. L. Ceuppens
Stefaan W. Van Gool
机构
[1] Catholic University of Leuven,Laboratory of Experimental Immunology
[2] Catholic University of Leuven,Laboratory of Physiology
[3] Catholic University of Leuven,Department of Neurosurgery
[4] Catholic University of Leuven,Department of Pediatrics
[5] Harvard School of Public Health,Department of Environmental Health
[6] University Hospital Gasthuisberg,undefined
来源
Cancer Immunology, Immunotherapy | 2005年 / 54卷
关键词
Confocal microscopy; Cytotoxicity; Dendritic cells; Flow cytometry; Malignant glioma; Tumor proteins;
D O I
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中图分类号
学科分类号
摘要
Malignant glioma of the CNS is a tumor with a very bad prognosis. Development of adjuvant immunotherapy is hampered by interindividual and intratumoral antigenic heterogeneity of gliomas. To evaluate feasibility of tumor vaccination with (autologous) tumor cells, we have studied uptake of tumor cell lysates by dendritic cells (DCs), and the T-cell stimulatory capacity of the loaded DCs. DCs are professional antigen-presenting cells, which have already been used as natural adjuvants to initiate immune responses in human cancer. An efficacious uptake of tumor cell proteins, followed by processing and presentation of tumor-associated antigens by the DCs, is indeed one of the prerequisites for a potent and specific stimulation of T lymphocytes. Human monocytes were differentiated in vitro to immature DCs, and these were loaded with FITC-labeled tumor cell proteins. Uptake of the tumor cell proteins and presentation of antigens in the context of both MHC class I and II could be demonstrated using FACS analysis and confocal microscopy. After further maturation, the loaded DCs had the capacity to induce specific T-cell cytotoxic activity against tumor cells. We conclude that DCs loaded with crude tumor lysate are efficacious antigen-presenting cells able to initiate a T-cell response against malignant glioma tumor cells.
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页码:372 / 382
页数:10
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