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DC vaccines loaded with glioma cells killed by photodynamic therapy induce Th17 anti-tumor immunity and provide a four-gene signature for glioma prognosis

Maria Vedunova, Victoria Turubanova, Olga Vershinina, Mariia Saviuk (UGent) , Iuliia Efimova (UGent) , Tatiana Mishchenko, Robrecht Raedt (UGent) , Anne Vral (UGent) , Christian Vanhove (UGent) , Daria Korsakova, et al.
(2022) CELL DEATH & DISEASE. 13(12).
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Abstract
Gliomas, the most frequent type of primary tumor of the central nervous system in adults, results in significant morbidity and mortality. Despite the development of novel, complex, multidisciplinary, and targeted therapies, glioma therapy has not progressed much over the last decades. Therefore, there is an urgent need to develop novel patient-adjusted immunotherapies that actively stimulate antitumor T cells, generate long-term memory, and result in significant clinical benefits. This work aimed to investigate the efficacy and molecular mechanism of dendritic cell (DC) vaccines loaded with glioma cells undergoing immunogenic cell death (ICD) induced by photosens-based photodynamic therapy (PS-PDT) and to identify reliable prognostic gene signatures for predicting the overall survival of patients. Analysis of the transcriptional program of the ICD-based DC vaccine led to the identification of robust induction of Th17 signature when used as a vaccine. These DCs demonstrate retinoic acid receptor-related orphan receptor-gamma t dependent efficacy in an orthotopic mouse model. Moreover, comparative analysis of the transcriptome program of the ICD-based DC vaccine with transcriptome data from the TCGA-LGG dataset identified a four-gene signature (CFH, GALNT3, SMC4, VAV3) associated with overall survival of glioma patients. This model was validated on overall survival of CGGA-LGG, TCGA-GBM, and CGGA-GBM datasets to determine whether it has a similar prognostic value. To that end, the sensitivity and specificity of the prognostic model for predicting overall survival were evaluated by calculating the area under the curve of the time-dependent receiver operating characteristic curve. The values of area under the curve for TCGA-LGG, CGGA-LGG, TCGA-GBM, and CGGA-GBM for predicting five-year survival rates were, respectively, 0.75, 0.73, 0.9, and 0.69. These data open attractive prospects for improving glioma therapy by employing ICD and PS-PDT-based DC vaccines to induce Th17 immunity and to use this prognostic model to predict the overall survival of glioma patients.
Keywords
Cancer Research, Cell Biology, Cellular and Molecular Neuroscience, Immunology

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MLA
Vedunova, Maria, et al. “DC Vaccines Loaded with Glioma Cells Killed by Photodynamic Therapy Induce Th17 Anti-Tumor Immunity and Provide a Four-Gene Signature for Glioma Prognosis.” CELL DEATH & DISEASE, vol. 13, no. 12, Springer Science and Business Media LLC, 2022, doi:10.1038/s41419-022-05514-0.
APA
Vedunova, M., Turubanova, V., Vershinina, O., Saviuk, M., Efimova, I., Mishchenko, T., … Krysko, D. (2022). DC vaccines loaded with glioma cells killed by photodynamic therapy induce Th17 anti-tumor immunity and provide a four-gene signature for glioma prognosis. CELL DEATH & DISEASE, 13(12). https://doi.org/10.1038/s41419-022-05514-0
Chicago author-date
Vedunova, Maria, Victoria Turubanova, Olga Vershinina, Mariia Saviuk, Iuliia Efimova, Tatiana Mishchenko, Robrecht Raedt, et al. 2022. “DC Vaccines Loaded with Glioma Cells Killed by Photodynamic Therapy Induce Th17 Anti-Tumor Immunity and Provide a Four-Gene Signature for Glioma Prognosis.” CELL DEATH & DISEASE 13 (12). https://doi.org/10.1038/s41419-022-05514-0.
Chicago author-date (all authors)
Vedunova, Maria, Victoria Turubanova, Olga Vershinina, Mariia Saviuk, Iuliia Efimova, Tatiana Mishchenko, Robrecht Raedt, Anne Vral, Christian Vanhove, Daria Korsakova, Claus Bachert, Frauke Coppieters, Patrizia Agostinis, Abhishek D. Garg, Mikhail Ivanchenko, Olga Krysko, and Dmitri Krysko. 2022. “DC Vaccines Loaded with Glioma Cells Killed by Photodynamic Therapy Induce Th17 Anti-Tumor Immunity and Provide a Four-Gene Signature for Glioma Prognosis.” CELL DEATH & DISEASE 13 (12). doi:10.1038/s41419-022-05514-0.
Vancouver
1.
Vedunova M, Turubanova V, Vershinina O, Saviuk M, Efimova I, Mishchenko T, et al. DC vaccines loaded with glioma cells killed by photodynamic therapy induce Th17 anti-tumor immunity and provide a four-gene signature for glioma prognosis. CELL DEATH & DISEASE. 2022;13(12).
IEEE
[1]
M. Vedunova et al., “DC vaccines loaded with glioma cells killed by photodynamic therapy induce Th17 anti-tumor immunity and provide a four-gene signature for glioma prognosis,” CELL DEATH & DISEASE, vol. 13, no. 12, 2022.
@article{01GPNHNKSR208R1CHWFM0M7760,
  abstract     = {{Gliomas, the most frequent type of primary tumor of the central nervous system in adults, results in significant morbidity and mortality. Despite the development of novel, complex, multidisciplinary, and targeted therapies, glioma therapy has not progressed much over the last decades. Therefore, there is an urgent need to develop novel patient-adjusted immunotherapies that actively stimulate antitumor T cells, generate long-term memory, and result in significant clinical benefits. This work aimed to investigate the efficacy and molecular mechanism of dendritic cell (DC) vaccines loaded with glioma cells undergoing immunogenic cell death (ICD) induced by photosens-based photodynamic therapy (PS-PDT) and to identify reliable prognostic gene signatures for predicting the overall survival of patients. Analysis of the transcriptional program of the ICD-based DC vaccine led to the identification of robust induction of Th17 signature when used as a vaccine. These DCs demonstrate retinoic acid receptor-related orphan receptor-gamma t dependent efficacy in an orthotopic mouse model. Moreover, comparative analysis of the transcriptome program of the ICD-based DC vaccine with transcriptome data from the TCGA-LGG dataset identified a four-gene signature (CFH, GALNT3, SMC4, VAV3) associated with overall survival of glioma patients. This model was validated on overall survival of CGGA-LGG, TCGA-GBM, and CGGA-GBM datasets to determine whether it has a similar prognostic value. To that end, the sensitivity and specificity of the prognostic model for predicting overall survival were evaluated by calculating the area under the curve of the time-dependent receiver operating characteristic curve. The values of area under the curve for TCGA-LGG, CGGA-LGG, TCGA-GBM, and CGGA-GBM for predicting five-year survival rates were, respectively, 0.75, 0.73, 0.9, and 0.69. These data open attractive prospects for improving glioma therapy by employing ICD and PS-PDT-based DC vaccines to induce Th17 immunity and to use this prognostic model to predict the overall survival of glioma patients.}},
  articleno    = {{1062}},
  author       = {{Vedunova, Maria and Turubanova, Victoria and Vershinina, Olga and Saviuk, Mariia and Efimova, Iuliia and Mishchenko, Tatiana and Raedt, Robrecht and Vral, Anne and Vanhove, Christian and Korsakova, Daria and Bachert, Claus and Coppieters, Frauke and Agostinis, Patrizia and Garg, Abhishek D. and Ivanchenko, Mikhail and Krysko, Olga and Krysko, Dmitri}},
  issn         = {{2041-4889}},
  journal      = {{CELL DEATH & DISEASE}},
  keywords     = {{Cancer Research,Cell Biology,Cellular and Molecular Neuroscience,Immunology}},
  language     = {{eng}},
  number       = {{12}},
  pages        = {{19}},
  publisher    = {{Springer Science and Business Media LLC}},
  title        = {{DC vaccines loaded with glioma cells killed by photodynamic therapy induce Th17 anti-tumor immunity and provide a four-gene signature for glioma prognosis}},
  url          = {{http://doi.org/10.1038/s41419-022-05514-0}},
  volume       = {{13}},
  year         = {{2022}},
}
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