A Novel Three-Pronged Approach to Kill Cancer Cells Selectively: Concomitant Viral, Double Suicide Gene, and Radiotherapy

Freytag, Svend O.; Rogulski, Kenneth; Paielli, Dell; Gilbert, Jeff D.; Kim, Jae H O

doi:10.1089/hum.1998.9.9-1323

Cited by 300 publications

(208 citation statements)

References 23 publications

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“…The intrinsic oncolytic effects of E1B-55K-deleted adenoviruses could be significantly enhanced in several solid xenograft tumor models when prodrug (GCV alone or in combination with 5-fluorocytosine (5-FC)) was withheld until maximum vector replication and gene expression occurred. [68][69][70] However, GCV administration was not beneficial to the intrinsic oncolytic activity of an adenovirus (Ad.OW34) with a much more robust replication than the E1B-55K-deleted vector Ad.TK RC , expressing the entire adenovirus E1 region as well as HSV-tk under conditions that favor active viral replication and spread, 14 probably because the potential HSV-tk/GCV-mediated enhancement of the intrinsic viral oncolytic activity was balanced out by the virostatic effects of GCV.…”

Section: Discussionmentioning

confidence: 99%

Comparison of HSV-1 thymidine kinase-dependent and -independent inhibition of replication-competent adenoviral vectors by a panel of drugs

et al. 2003

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Replication-competent adenoviral vectors hold the promise to be more efficient gene delivery vehicles than their replicationdeficient counterparts, but they are also associated with a higher risk for adverse effects, especially in light of the fact that there is no established effective therapy for serious, disseminated adenovirus infection. To assess whether the therapeutic options to inhibit adenoviral replication can be enhanced by expressing a suicide gene, we examined the antiadenoviral effects of 15 drugs against wild-type adenovirus type 5 (Ad5) and an Ad5-based replication-competent vector expressing herpes simplex virus-1 thymidine kinase (HSV-tk) (Ad.OW34) using a real-time polymerase chain reaction -based assay and flow cytometry. Ad5 and Ad.OW34 were highly susceptible to the fluorinated pyrimidine analogs 5-fluoro-2 0 -deoxyuridine (FUdR), 5-fluorouridine (FUR), and trifluorothymidine (TFT), with a mean 50% inhibitory concentration (IC 50 ) ranging from 0.12 to 0.32 mM. The mean IC 50 of ribavirin and cidofovir (CDV) for Ad5, the most frequently used drugs to treat adenovirus disease, was 6.87 and 3.19 mM, respectively. In contrast to Ad5, the Ad.OW34 vector was susceptible to (E)-5-(2-bromovinyl)-2 0 -deoxyuridine (BVdU, IC 50 0.09 mM), ganciclovir (GCV, IC 50 0.19 mM), and acyclovir (ACV, IC 50 32.04 mM). Additionally, we demonstrated in an animal model that Ad.OW34 vector replication can be inhibited significantly by GCV, CDV, and TFT by 35.2, 7.7, and 3.7-fold, respectively, compared to untreated animals. The observed antiadenoviral effects were primarily not through cell killing, since the in vitro 50% cytotoxic concentrations (CC 50 ) were more than 1000 times higher than the antiadenoviral IC 50 of the drugs examined, even in cells stably expressing HSV-tk. Since for HSV-tk-dependent inhibition of adenoviral vectors, stability of HSV-tk expression is crucial, we examined Ad.OW34 vector stability, by passaging the vector 10 times serially in the presence of 10 mM GCV. The HSV-tk/GCV system neither changed the susceptibility of Ad.OW34 to GCV significantly nor detectable vector rearrangements occurred, suggesting that the system might be suitable as a fail-safe mechanism to stop adenoviral vector replication.

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Section: Discussionmentioning

confidence: 99%

Comparison of HSV-1 thymidine kinase-dependent and -independent inhibition of replication-competent adenoviral vectors by a panel of drugs

et al. 2003

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“…Some of them, including fusion of CD and HSVtk genes, combination with radiation, or utilization of tumor-or tissue-specific promoter, are effective in increasing the killing of tumor cells and reducing its toxicity. [25][26][27][28] Among these approaches, co-transfection of suicide gene and cytokine gene has been found to elicit potent antitumor effects and induce potent antitumor immunity efficiently. Various cytokine genes, including GM-CSF, IL-2, IL-4, IFN-␣ and IFN-␥ have been transferred into tumor cells in combination with HSVtk or CD suicide gene therapy, and more potent antitumor effects and more efficient induction of antitumor immune response have been observed with these combination therapies.…”

Section: Discussionmentioning

confidence: 99%

Adenovirus-mediated lymphotactin gene transfer improves therapeutic efficacy of cytosine deaminase suicide gene therapy in established murine colon carcinoma

Tao

Cheng

et al. 2000

Gene Ther

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Lymphotactin (Ltn) is the sole member of C chemokines which attracts T cells and NK cells specially. Ltn gene was transferred in vivo to improve the antitumor efficacy of cytosine deaminase (CD) gene therapy. Upregulation of CD80 and CD54 on murine CT26 colon carcinoma cells was observed after combined transfection with adenovirus encoding CD (AdCD) and adenovirus encoding murine Ltn (AdLtn) followed by administration of 5-fluorocytosine (5FC) in vitro. AdCD/5FC treatment also increased the expression of CD95 and induced obvious apoptosis of CT26 cells. After combined treatment with AdLtn and AdCD/5FC, the preestablished murine model with subcutaneous CT26 colon carcinoma exhibited most significant tumor growth inhibition, and four of eight tumor-bearing mice were tumor free, while tumors in other mice grew more progressively. Examination of lymphocyte infiltration and cytokine gene expression in

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“…Adenoviruses are the most widely studied engineered oncolytic viruses clinically. Adenoviral constructs include Onyx 015, 1,2 CG7060, 3 CG7870, 4 dl922-947, 5 Ad5-CD/tk-rep, 6 Ad-delta24, 7 Ad DF3-E1, 8 Onyx 411, 9 OAV001, 10 KD3, 11 01/PEME 12 and Telomelysin. 13,14 Historically, evidence of viral oncolytic activity was published in case reports as early as 1912.…”

Section: Introductionmentioning

confidence: 99%

Clinical development directions in oncolytic viral therapy

Eager

Nemunaitis

2011

Cancer Gene Ther

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Oncolytic virotherapy is an emerging experimental treatment platform for cancer therapy. Oncolytic viruses are replicativecompetent viruses that are engineered to replicate selectively in cancer cells with specified oncogenic phenotypes. Multiple DNA and RNA viruses have been clinically tested in a variety of tumors. This review will provide a brief description of these novel anticancer biologics and will summarize the results of clinical investigation. To date oncolytic virotherapy has shown to be safe, and has generated clinical responses in tumors that are resistant to chemotherapy or radiotherapy. The major challenge for researchers is to maximize the efficacy of these viral therapeutics, and to establish stable systemic delivery mechanisms.

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A Novel Three-Pronged Approach to Kill Cancer Cells Selectively: Concomitant Viral, Double Suicide Gene, and Radiotherapy

Cited by 300 publications

References 23 publications

Comparison of HSV-1 thymidine kinase-dependent and -independent inhibition of replication-competent adenoviral vectors by a panel of drugs

Comparison of HSV-1 thymidine kinase-dependent and -independent inhibition of replication-competent adenoviral vectors by a panel of drugs

Adenovirus-mediated lymphotactin gene transfer improves therapeutic efficacy of cytosine deaminase suicide gene therapy in established murine colon carcinoma

Clinical development directions in oncolytic viral therapy

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