Evaluation of radiation effects against C6 glioma in combination with vaccinia virus-p53 gene therapy

Daila S. Gridley; Melba L. Andres; Jun Li; Tatyana Timiryasova; Bing Chen; Istvan Fodor

doi:10.3892/ijo.13.5.1093

Evaluation of radiation effects against C6 glioma in combination with vaccinia virus-p53 gene therapy

Daila S. Gridley
, Melba L. Andres
, Jun Li
, Tatyana Timiryasova
, Bing Chen
, Istvan Fodor

Research output: Contribution to journal › Article › peer-review

Abstract

The primary objective of this study was to evaluate the antitumor effects of recombinant vaccinia virus-p53 (rVV-p53) in combination with radiation therapy against the C6 rat glioma, a p53 deficient tumor that is relatively radioresistant. VV-LIVP, the parental virus (Lister strain), was used as a control. Localized treatment of subcutaneous C6 tumors in athymic mice with either rVV-p53 or VV-LIVP together with tumor irradiation resulted in low tumor incidence and significantly slower tumor progression compared to the agents given as single modalities. Assays of blood and spleen indicated that immune system activation may account, at least partly, for the enhance tumor inhibition seen with combined treatment. No overt signs of treatment- related toxicity were noted.

Original language	English
Pages (from-to)	1093-1098
Number of pages	6
Journal	International Journal of Oncology
Volume	13
Issue number	5
DOIs	https://doi.org/10.3892/ijo.13.5.1093
State	Published - Nov 1998

ASJC Scopus Subject Areas

Oncology
Cancer Research

Keywords

Gene therapy
Glioma
Radiation
Vaccinia virus
p53

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title = "Evaluation of radiation effects against C6 glioma in combination with vaccinia virus-p53 gene therapy",

abstract = "The primary objective of this study was to evaluate the antitumor effects of recombinant vaccinia virus-p53 (rVV-p53) in combination with radiation therapy against the C6 rat glioma, a p53 deficient tumor that is relatively radioresistant. VV-LIVP, the parental virus (Lister strain), was used as a control. Localized treatment of subcutaneous C6 tumors in athymic mice with either rVV-p53 or VV-LIVP together with tumor irradiation resulted in low tumor incidence and significantly slower tumor progression compared to the agents given as single modalities. Assays of blood and spleen indicated that immune system activation may account, at least partly, for the enhance tumor inhibition seen with combined treatment. No overt signs of treatment- related toxicity were noted.",

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note = "The primary objective of this study was to evaluate the antitumor effects of recombinant vaccinia virus-p53 (rVV-p53) in combination with radiation therapy against the C6 rat glioma, a p53 deficient tumor that is relatively radioresistant.",

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AU - Li, Jun

AU - Timiryasova, Tatyana

AU - Chen, Bing

AU - Fodor, Istvan

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N2 - The primary objective of this study was to evaluate the antitumor effects of recombinant vaccinia virus-p53 (rVV-p53) in combination with radiation therapy against the C6 rat glioma, a p53 deficient tumor that is relatively radioresistant. VV-LIVP, the parental virus (Lister strain), was used as a control. Localized treatment of subcutaneous C6 tumors in athymic mice with either rVV-p53 or VV-LIVP together with tumor irradiation resulted in low tumor incidence and significantly slower tumor progression compared to the agents given as single modalities. Assays of blood and spleen indicated that immune system activation may account, at least partly, for the enhance tumor inhibition seen with combined treatment. No overt signs of treatment- related toxicity were noted.

AB - The primary objective of this study was to evaluate the antitumor effects of recombinant vaccinia virus-p53 (rVV-p53) in combination with radiation therapy against the C6 rat glioma, a p53 deficient tumor that is relatively radioresistant. VV-LIVP, the parental virus (Lister strain), was used as a control. Localized treatment of subcutaneous C6 tumors in athymic mice with either rVV-p53 or VV-LIVP together with tumor irradiation resulted in low tumor incidence and significantly slower tumor progression compared to the agents given as single modalities. Assays of blood and spleen indicated that immune system activation may account, at least partly, for the enhance tumor inhibition seen with combined treatment. No overt signs of treatment- related toxicity were noted.

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KW - Glioma

KW - Radiation

KW - Vaccinia virus

KW - p53

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Evaluation of radiation effects against C6 glioma in combination with vaccinia virus-p53 gene therapy

Abstract

ASJC Scopus Subject Areas

Keywords

Access to Document

OpenUrl availability

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