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Your search keyword '"Krendelchtchikova V"' showing total 5 results
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5 results on '"Krendelchtchikova V"'

1. CRAdRGDflt-IL24 virotherapy in combination with chemotherapy of experimental glioma.

Author

Kaliberova, L. N., Krendelchtchikova, V., Harmon, D. K., Stockard, C. R., Petersen, A. S., Markert, J. M., Gillespie, G. Y., Grizzle, W. E., Buchsbaum, D. J., and Kaliberov, S. A.

Subjects
*GLIOMAS, *DRUG therapy, *APOPTOSIS, *INTERLEUKINS, *XENOGRAFTS, *INTRACRANIAL tumors
Abstract

Malignant forms of glioma, the most common primary brain tumors, remain poorly responsive to multimodality therapeutic interventions, including chemotherapy. Suppressed apoptosis and extraordinary invasiveness are important distinctive features that contribute to the malignant phenotype of glioma. We have developed the vascular endothelial growth factor receptor 1 (VEGFR-1/flt-1) conditional replicating adenoviral vector (CRAdRGDflt-IL24) encoding the interleukin-24 (IL-24) gene. We investigated whether a combination of CRAdRGDflt-IL24-mediated oncolytic virotherapy and chemotherapy using temozolomide (TMZ) produces increased cytotoxicity against human glioma cells in comparison with these agents alone. Combination of CRAdRGDflt-IL24 and TMZ significantly enhanced cytotoxicity in vitro, inhibited D54MG tumor growth and prolonged survival of mice harboring intracranial human glioma xenografts in comparison with CRAdRGDflt-IL24 or TMZ alone. These data indicate that combined treatment with CRAdRGDflt-IL24-mediated oncolytic virotherapy and TMZ chemotherapy provides a promising approach for glioma therapy. [ABSTRACT FROM AUTHOR]

Published
2009
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3. Mutation of Escherichia coli cytosine deaminase significantly enhances molecular chemotherapy of human glioma.

Author

Kaliberov, S. A., Market, J. M., Gillespie, G. Y., Krendelchtchikova, V., Della Manna, D., Sellers, J. C., Kaliberova, L. N., Black, M. E., and Buchsbaum, D. J.

Subjects
*ANTIBODY-directed enzyme prodrug therapy, *ADENOSINE deaminase, *PRODRUGS, *GLIOMAS, *NERVOUS system tumors, *BACTERIAL genetics, *ESCHERICHIA coli
Abstract

Combined treatment using adenoviral (Ad)-directed enzyme/prodrug therapy and radiation therapy has the potential to become a powerful method of cancer therapy. We have developed an Ad vector encoding a mutant bacterial cytosine deaminase (bCD) gene (AdbCD-D314A), which has a higher affinity for cytosine than wild-type bCD (bCDwt). The purpose of this study was to evaluate cytotoxicity in vitro and therapeutic efficacy in vivo of the combination of AdbCD-D314A with the prodrug 5-fluorocytosine (5-FC) and ionizing radiation against human glioma. The present study demonstrates that AdbCD-D314A infection resulted in increased 5-FC-mediated cell killing, compared with AdbCDwt. Furthermore, a significant increase in cytotoxicity following AdbCD-D314A and radiation treatment of glioma cells in vitro was demonstrated as compared to AdbCDwt. Animal studies showed significant inhibition of subcutaneous or intracranial tumor growth of D54MG glioma xenografts by the combination of AdbCD-D314A/5-FC with ionizing radiation as compared with either agent alone, and with AdbCDwt/5-FC plus radiation. The results suggest that the combination of AdbCD-D314A/5-FC with radiation produces markedly increased cytotoxic effects in cancer cells in vitro and in vivo. These data indicate that combined treatment with this novel mutant enzyme/prodrug therapy and radiotherapy provides a promising approach for cancer therapy.Gene Therapy (2007) 14, 1111–1119; doi:10.1038/sj.gt.3302965; published online 10 May 2007 [ABSTRACT FROM AUTHOR]

Published
2007
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4. Combination of cytosine deaminase suicide gene expression with DR5 antibody treatment increases cancer cell cytotoxicity.

Author

Kaliberov, S. A., Chiz, S., Kaliberova, L. N., Krendelchtchikova, V., Della Manna, D., Zhou, T., and Buchsbaum, D. J.

Subjects
*GENE expression, *GENE therapy, *IMMUNOTHERAPY, *TUMOR necrosis factors, *APOPTOSIS, *CELL lines, *CELL culture
Abstract

Combined treatment using adenoviral-directed enzyme/prodrug therapy and immunotherapy has the potential to become a powerful alternative method of cancer therapy. We have developed adenoviral vectors encoding the cytosine deaminase gene (Ad-CD) and cytosine deaminase:uracil phosphoribosyltransferase fusion gene (Ad-CD:UPRT). A monoclonal antibody, TRA-8, specifically binds to death receptor 5, one of two death receptors bound by tumor necrosis factor-related apoptosis-inducing ligand (TRAIL). The purpose of this study was to evaluate cytotoxicity in vitro and therapeutic efficacy in vivo of the combination of Ad-CD:UPRT and TRA-8 against human pancreatic cancer and glioma cell lines. The present study demonstrates that Ad-CD:UPRT infection resulted in increased 5-FC-mediated cell killing, compared with Ad-CD. Furthermore, a significant increase of cytotoxicity following Ad-CD:UPRT/5-FC and TRA-8 treatment of cancer cells in vitro was demonstrated. Animal studies showed significant inhibition of tumor growth of MIA PaCa-2 pancreatic and D54MG glioma xenografts by the combination of Ad-CD:UPRT/5-FC plus TRA-8 as compared with either agent alone or no treatment. The results suggest that the combination of Ad-CD:UPRT/5-FC with TRA-8 produces an additive cytotoxic effect in cancer cells in vitro and in vivo. These data indicate that combined treatment with enzyme/prodrug therapy and TRAIL immunotherapy provides a promising approach for cancer therapy.Cancer Gene Therapy (2006) 13, 203–214. doi:10.1038/sj.cgt.7700874; published online 5 August 2005 [ABSTRACT FROM AUTHOR]

Published
2006
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