Local tumor irradiation augments the antitumor effect of cytokine-producing autologous cancer cell vaccines in a murine glioma model

Lumniczky, Katalin; Desaknai, Szilvia; Mangel, László; Szende, B.; Hamada, Hirofumi; Hidvégi, Egon J.; Sáfrány, Géza

doi:10.1038/sj/cgt/7700398

Cited by 21 publications

(29 citation statements)

References 15 publications

(16 reference statements)

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“…Indeed, in a therapeutic vaccination approach against intracranial GL261-derived tumors, depletion of either CD4 þ or CD8 þ T lymphocytes proved to impair the antitumor effect of the vaccine. 24 In conclusion, the present study shows that the interaction of PVs with cancer cells can lead not only to direct oncolysis, but also to a break of the immune tolerance to tumors, resulting in synergistic effects of virus infection and host immune reactions on tumor suppression. In at least some tumor models, as the one studied in this work, immune cells appear to be the main effectors of PV-dependent tumor destruction.…”

Section: Discussionmentioning

confidence: 59%

Activation of a glioma-specific immune response by oncolytic parvovirus Minute Virus of Mice infection

et al. 2012

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Rodent autonomous parvoviruses (PVs) are endowed with oncotropic properties and represent virotherapeutics with inherent oncolytic features. This work aimed to evaluate the capacity of Minute Virus of Mice (MVMp) to act as an adjuvant stimulating a mouse glioblastoma-specific immune response. MVMp was shown to induce cell death through apoptosis in glioma GL261 cells. Antigen-presenting cells (APCs) provide the initial cue for innate and adaptive immune responses, and thus MVMp-infected GL261 cells were tested for their ability to activate dendritic cells (DCs) and microglia (MG), two distinct cell types that are able to act as APCs. MG and discrete DC subsets were activated after co-culture with MVMp-infected glioma GL261 cells, as evidenced by upregulation of specific activation markers (CD80, CD86) and release of proinflammatory cytokines (tumor necrosis factor-a and interleukin-6). The in vivo analysis of immunodeficient and immunocompetent mice revealed a clear difference in their susceptibility to MVMp-mediated tumor suppression. Immunocompetent mice were fully protected from tumor outgrowth of GL261 cells infected ex vivo with MVMp. In contrast, immunodeficient animals were less competent for MVMp-dependent tumor inhibition, with only 20% of the recipients being protected, arguing for an additional immune component to allow full tumor suppression. In keeping with this conclusion, immunocompetent mice engrafted with MVMp-infected glioma cells developed a level of anti-tumor immunity with isolated splenocytes producing elevated levels of interferon-g. In rechallenge experiments using uninfected GL261 cells, we could show complete protection against the tumor, arguing for the induction of a T-cell-mediated, tumor-specific, long-term memory response. These findings indicate that the anticancer effect of PVs can be traced back not only for their direct oncolytic effect, but also to their ability to break tumor tolerance.

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Section: Discussionmentioning

confidence: 59%

Activation of a glioma-specific immune response by oncolytic parvovirus Minute Virus of Mice infection

et al. 2012

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“…The GL261 cell line was induced by intracerebral implantation of methylcholanthrene (MCA) pellets and later established as a permanent cell line. 20 The pMG plasmid (Invivogen, San Diego, CA) containing the gene for murine GM-CSF was used for transducing the GL261 cell line (GL-GM). Cytokine production was measured in supernatants from 1 3 10 5 GL-GM cells cultured for 48 hr with a mouse GM-CSF ELISA kit (Pharmingen, San Diego, CA).…”

Section: Animals and Cell Linesmentioning

confidence: 99%

Synergism between GM–CSF and IFNγ: Enhanced immunotherapy in mice with glioma

Smith

Janelidze

Visse

et al. 2006

Intl Journal of Cancer

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Glioblastoma multiforme is the most common malignant primary brain tumor and also one of the most therapy-resistant tumors. Because of the dismal prognosis, various therapies modulating the immune system have been developed in experimental models. Previously, we have shown a 37-70% cure in a rat glioma model where rats were peripherally immunized with tumor cells producing IFNc. On the basis of these results, we wanted to investigate whether a combination of GM-CSF and IFNc could improve the therapeutic effect in a mouse glioma model, GL261 (GL-wt). Three biweekly intraperitoneal (i.p.) immunizations with irradiated GM-CSF-transduced GL261 cells (GL-GM) induced a 44% survival in mice with intracranial glioma. While treatment of GLwt and GL-GM with IFNc in vitro induced upregulation of MHC I and MHC II on the tumor cells, it could not enhance survival after immunization. However, immunizations with GL-GM combined with recombinant IFNc at the immunization site synergistically enhanced survival with a cure rate of 88%. Tumors from mice receiving only 1 immunization on Day 10 after tumor inoculation were sectioned on Day 20 for analysis of leukocyte infiltration. Tumor volume was reduced and the infiltration of macrophages was denser in mice immunized with GL-GM combined with IFNc compared with that of both wildtype and nonimmunized mice. To our knowledge, this is the first study to demonstrate a synergy between GM-CSF and IFNc in experimental immunotherapy of tumors, by substantially increasing survival as well as inducing a potent anti-tumor response after only 1 postponed immunization. ' 2006 Wiley-Liss, Inc.

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“…The Gl261 cell line was established in our lab from the in vivo growing Gl261 tumor. [12][13][14] All cell lines were cultured in Dulbecco's Modified Eagle's Medium (DMEM) supplemented with 10% fetal calf serum and appropriate antibiotics.…”

Section: Methodsmentioning

confidence: 99%

“…13 To determine transduction efficiency, Gl261, U373 and C6 cells were infected with an adenoviral vector (AdexCAlacZ) encoding the bacterial b-galactosidase (lacZ) gene at different multiplicities of infection (MOI) and lacZ activity measured as described. 13 In vitro sensitivity of glioma cell lines to dCK overexpression, gemcitabine treatment and irradiation To determine the sensitivity of the Gl261, C6 and U373 cell lines to gemcitabine, cells were seeded in 25 cm 2 tissue culture dishes at day 1 using the following cell densities: 20 Â 10 3 , 12 Â 10 3 and 6 Â 10 3 cells cm À2 for Gl261, U373 and C6 cells, respectively. The next day, cells were treated with increasing concentrations of gemcitabine.…”

Section: Methodsmentioning

confidence: 99%

Adenoviral vector transduction of the human deoxycytidine kinase gene enhances the cytotoxic and radiosensitizing effect of gemcitabine on experimental gliomas

et al. 2008

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The aim of this work was to improve the cytotoxic and radiosensitizing effects of gemcitabine using a gene-directed enzyme prodrug therapy approach. Murine Gl261, rat C6 and human U373 glioma cell lines were transduced with an adenoviral vector encoding the human deoxycytidine kinase gene (Ad-HudCK). Intracranial tumors were established in C57BL/6 mice and Wistar rats using either wild-type or Ad-HudCK-transduced Gl261 and C6 glioma cells. In vitro growing cells and established tumors were treated with gemcitabine and irradiation either alone or in combination. Deoxycytidine kinase overexpression substantially increased both the toxic and radiosensitizing effects of gemcitabine in each cell line, but the enhancement rate varied: it was mild in the Gl261 cells and much stronger in the C6 and U373 cells. In vivo experiments showed a mild radiosensitizing effect of dCK overexpression both in the Gl261 and C6 models. The combination of dCK overexpression, gemcitabine treatment and irradiation improved the survival rate of C6 bearing rats significantly. In conclusion, overexpression of the dCK gene can improve the cytotoxic and radiosensitizing effect of gemcitabine both in vitro and in vivo in a tumor-specific manner.

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Local tumor irradiation augments the antitumor effect of cytokine-producing autologous cancer cell vaccines in a murine glioma model

Cited by 21 publications

References 15 publications

Activation of a glioma-specific immune response by oncolytic parvovirus Minute Virus of Mice infection

Activation of a glioma-specific immune response by oncolytic parvovirus Minute Virus of Mice infection

Synergism between GM–CSF and IFNγ: Enhanced immunotherapy in mice with glioma

Adenoviral vector transduction of the human deoxycytidine kinase gene enhances the cytotoxic and radiosensitizing effect of gemcitabine on experimental gliomas

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