Complex interactions between the replicating oncolytic effect and the enzyme/prodrug effect of vaccinia-mediated tumor regression

Complex interactions between the replicating oncolytic effect and the enzyme/prodrug effect of vaccinia-mediated tumor regression

Replicating viruses for cancer gene therapy have beneficial antitumor effects, however, in the setting of an enzyme/prodrug system, the interactions between these viruses and the activated agents are complex. A replicating vaccinia virus expressing the cytosine deaminase gene (VVCD), which converts...

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Bibliographic Details
Published in:Gene therapy Vol. 7; no. 14; pp. 1217 - 1223
Main Authors: MCCART, J. A, PUHLMANN, M, LEE, J, HU, Y, LIBUTTI, S. K, ALEXANDER, H. R, BARTLETT, D. L
Format: Journal Article
Language:English
Published: Basingstoke Nature Publishing Group 01-07-2000
Subjects:
Adenocarcinoma
Adenocarcinoma - therapy
Animals
Antitumor activity
Biological and medical sciences
Biotechnology
Colonic Neoplasms - therapy
Cytosine
Cytosine Deaminase
Cytotoxicity
Dose-Response Relationship, Drug
Drug Interactions
Enzymes
Flucytosine - metabolism
Flucytosine - therapeutic use
Fluorouracil - metabolism
Fluorouracil - therapeutic use
Fundamental and applied biological sciences. Psychology
Gene therapy
Genetic Therapy - methods
Health. Pharmaceutical industry
Industrial applications and implications. Economical aspects
Lysates
Mice
Mice, Inbred C57BL
Mice, Nude
Nucleoside Deaminases - genetics
Oncolysis
Pathogenicity
Prodrugs
Prodrugs - metabolism
Prodrugs - therapeutic use
Tumor Cells, Cultured
Tumors
Vaccinia virus - drug effects
Vaccinia virus - enzymology
Vaccinia virus - genetics
Virus Replication - drug effects
Viruses
Enzyme
Cytosine deaminase
Toxicity
Rodentia
Regression
Molecular interaction
Prodrug
Virus
Vertebrata
Mammalia
Cell line
Mouse
Hydrolases
Tumor
Gene therapy
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Summary:Replicating viruses for cancer gene therapy have beneficial antitumor effects, however, in the setting of an enzyme/prodrug system, the interactions between these viruses and the activated agents are complex. A replicating vaccinia virus expressing the cytosine deaminase gene (VVCD), which converts the prodrug 5-FC into 5-FU, was characterized in vitro and in vivo for its antitumor effects and pathogenicity. Replicating VVCD (+/-5-FC) at various MOIs was used to infect MC38 murine colon adenocarcinoma cells. At high MOIs (>0.1) virus alone was able to kill the majority (65-90%) of cells by day 5 with no additional benefit from prodrug. At low MOIs only the effect of prodrug is seen. Cell lysates demonstrated 300-fold reduced viral recovery from cells treated with both VVCD and 5-FC compared with controls treated with virus alone. Nude mice bearing subcutaneous MC38 tumors were injected with VVCD (or control) and treated with 5FC or control. Mice injected with VVCD (with or without 5FC treatment) had smaller tumors than the controls, suggesting that replicating vaccinia alone is cytotoxic to tumors in vivo. The addition of 5-FC improved the antitumor response when a low dose of virus was injected into tumors. Also, compared with mice that received virus alone, those that received VVCD and 5FC had significantly prolonged survival from virus-mediated death. In conclusion, the addition of an enzyme/prodrug system to a replicating virus can improve the antitumor response and decrease viral pathogenicity. Gene Therapy (2000) 7, 1217-1223.
ISSN:0969-7128
1476-5462
DOI:10.1038/sj.gt.3301237