Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells

T. Yokoyama; E. Iwado; Y. Kondo; H. Aoki; Y. Hayashi; M. M. Georgescu; R. Sawaya; K. R. Hess; G. B. Mills; H. Kawamura; Y. Hashimoto; Y. Urata; T. Fujiwara; S. Kondo

doi:10.1038/gt.2008.98

Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells

T. Yokoyama, E. Iwado, Y. Kondo, H. Aoki, Y. Hayashi, M. M. Georgescu, R. Sawaya, K. R. Hess, G. B. Mills, H. Kawamura, Y. Hashimoto, Y. Urata, T. Fujiwara, S. Kondo

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Abstract

Oncolytic adenoviruses are a promising tool in cancer therapy. In this study, we characterized the role of autophagy in oncolytic adenovirus-induced therapeutic effects. OBP-405, an oncolytic adenovirus regulated by the human telomerase reverse transcriptase promoter (hTERT-Ad, OBP-301) with a tropism modification (RGD) exhibited a strong antitumor effect on glioblastoma cells. When autophagy was inhibited pharmacologically, the cytotoxicity of OBP-405 was attenuated. In addition, autophagy-deficient Atg5^-/- mouse embryonic fibroblasts (MEFs) were less sensitive than wild-type MEFs to OBP-405. These findings indicate that OBP-405-induced autophagy is a cell killing effect. Moreover, autophagy-inducing therapies (temozolomide and rapamycin) synergistically sensitized tumor cells to OBP-405 by stimulating the autophagic pathway without altering OBP-405 replication. Mice harboring intracranial tumors treated with OBP-405 and temozolomide survived significantly longer than those treated with temozolomide alone, and mice treated with OBP-405 and the rapamycin analog RAD001 survived significantly longer than those treated with RAD001 alone. The observation that autophagy inducers increase OBP-405 antitumor activity suggests a novel strategy for treating patients with glioblastoma.

Original language	English
Pages (from-to)	1233-1239
Number of pages	7
Journal	Gene Therapy
Volume	15
Issue number	17
DOIs	https://doi.org/10.1038/gt.2008.98
Publication status	Published - 2008

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics

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Yokoyama, T., Iwado, E., Kondo, Y., Aoki, H., Hayashi, Y., Georgescu, M. M., Sawaya, R., Hess, K. R., Mills, G. B., Kawamura, H., Hashimoto, Y., Urata, Y., Fujiwara, T., & Kondo, S. (2008). Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells. Gene Therapy, 15(17), 1233-1239. https://doi.org/10.1038/gt.2008.98

Yokoyama, T, Iwado, E, Kondo, Y, Aoki, H, Hayashi, Y, Georgescu, MM, Sawaya, R, Hess, KR, Mills, GB, Kawamura, H, Hashimoto, Y, Urata, Y, Fujiwara, T & Kondo, S 2008, 'Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells', Gene Therapy, vol. 15, no. 17, pp. 1233-1239. https://doi.org/10.1038/gt.2008.98

@article{dd6c20efa0304fa3b74373231f847917,

title = "Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells",

abstract = "Oncolytic adenoviruses are a promising tool in cancer therapy. In this study, we characterized the role of autophagy in oncolytic adenovirus-induced therapeutic effects. OBP-405, an oncolytic adenovirus regulated by the human telomerase reverse transcriptase promoter (hTERT-Ad, OBP-301) with a tropism modification (RGD) exhibited a strong antitumor effect on glioblastoma cells. When autophagy was inhibited pharmacologically, the cytotoxicity of OBP-405 was attenuated. In addition, autophagy-deficient Atg5-/- mouse embryonic fibroblasts (MEFs) were less sensitive than wild-type MEFs to OBP-405. These findings indicate that OBP-405-induced autophagy is a cell killing effect. Moreover, autophagy-inducing therapies (temozolomide and rapamycin) synergistically sensitized tumor cells to OBP-405 by stimulating the autophagic pathway without altering OBP-405 replication. Mice harboring intracranial tumors treated with OBP-405 and temozolomide survived significantly longer than those treated with temozolomide alone, and mice treated with OBP-405 and the rapamycin analog RAD001 survived significantly longer than those treated with RAD001 alone. The observation that autophagy inducers increase OBP-405 antitumor activity suggests a novel strategy for treating patients with glioblastoma.",

author = "T. Yokoyama and E. Iwado and Y. Kondo and H. Aoki and Y. Hayashi and Georgescu, {M. M.} and R. Sawaya and Hess, {K. R.} and Mills, {G. B.} and H. Kawamura and Y. Hashimoto and Y. Urata and T. Fujiwara and S. Kondo",

note = "Funding Information: Grant support: This study was supported in part by National Cancer Institute Grants CA088936 and CA108558, a start-up fund from The University of Texas MD Anderson Cancer Center (SK), a generous donation from the Anthony D Bullock III Foundation (YK, RS and SK) and the cancer center support grant (CCSG)/shared resources of MD Anderson Cancer Center. Funding Information: We thank Dr Noboru Mizushima for the GFP-LC3 expression vector and the wild-type and Atg5−/− MEFs. We also thank E Faith Hollingsworth for technical support and Elizabeth L Hess for editing the manuscript. This work was supported in part by Grant CA-088936 from the National Cancer Institute (to S Kondo), by a generous donation from the Anthony D Bullock III Foundation (to Y Kondo, R Sawaya and S Kondo) and the Institutional Core Grant CA-16672 High Resolution Electron Microscopy Facility, MD Anderson Cancer Center.",

year = "2008",

doi = "10.1038/gt.2008.98",

language = "English",

volume = "15",

pages = "1233--1239",

journal = "Gene Therapy",

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T1 - Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells

AU - Yokoyama, T.

AU - Iwado, E.

AU - Kondo, Y.

AU - Aoki, H.

AU - Hayashi, Y.

AU - Georgescu, M. M.

AU - Sawaya, R.

AU - Hess, K. R.

AU - Mills, G. B.

AU - Kawamura, H.

AU - Hashimoto, Y.

AU - Urata, Y.

AU - Fujiwara, T.

AU - Kondo, S.

N1 - Funding Information: Grant support: This study was supported in part by National Cancer Institute Grants CA088936 and CA108558, a start-up fund from The University of Texas MD Anderson Cancer Center (SK), a generous donation from the Anthony D Bullock III Foundation (YK, RS and SK) and the cancer center support grant (CCSG)/shared resources of MD Anderson Cancer Center. Funding Information: We thank Dr Noboru Mizushima for the GFP-LC3 expression vector and the wild-type and Atg5−/− MEFs. We also thank E Faith Hollingsworth for technical support and Elizabeth L Hess for editing the manuscript. This work was supported in part by Grant CA-088936 from the National Cancer Institute (to S Kondo), by a generous donation from the Anthony D Bullock III Foundation (to Y Kondo, R Sawaya and S Kondo) and the Institutional Core Grant CA-16672 High Resolution Electron Microscopy Facility, MD Anderson Cancer Center.

PY - 2008

Y1 - 2008

N2 - Oncolytic adenoviruses are a promising tool in cancer therapy. In this study, we characterized the role of autophagy in oncolytic adenovirus-induced therapeutic effects. OBP-405, an oncolytic adenovirus regulated by the human telomerase reverse transcriptase promoter (hTERT-Ad, OBP-301) with a tropism modification (RGD) exhibited a strong antitumor effect on glioblastoma cells. When autophagy was inhibited pharmacologically, the cytotoxicity of OBP-405 was attenuated. In addition, autophagy-deficient Atg5-/- mouse embryonic fibroblasts (MEFs) were less sensitive than wild-type MEFs to OBP-405. These findings indicate that OBP-405-induced autophagy is a cell killing effect. Moreover, autophagy-inducing therapies (temozolomide and rapamycin) synergistically sensitized tumor cells to OBP-405 by stimulating the autophagic pathway without altering OBP-405 replication. Mice harboring intracranial tumors treated with OBP-405 and temozolomide survived significantly longer than those treated with temozolomide alone, and mice treated with OBP-405 and the rapamycin analog RAD001 survived significantly longer than those treated with RAD001 alone. The observation that autophagy inducers increase OBP-405 antitumor activity suggests a novel strategy for treating patients with glioblastoma.

AB - Oncolytic adenoviruses are a promising tool in cancer therapy. In this study, we characterized the role of autophagy in oncolytic adenovirus-induced therapeutic effects. OBP-405, an oncolytic adenovirus regulated by the human telomerase reverse transcriptase promoter (hTERT-Ad, OBP-301) with a tropism modification (RGD) exhibited a strong antitumor effect on glioblastoma cells. When autophagy was inhibited pharmacologically, the cytotoxicity of OBP-405 was attenuated. In addition, autophagy-deficient Atg5-/- mouse embryonic fibroblasts (MEFs) were less sensitive than wild-type MEFs to OBP-405. These findings indicate that OBP-405-induced autophagy is a cell killing effect. Moreover, autophagy-inducing therapies (temozolomide and rapamycin) synergistically sensitized tumor cells to OBP-405 by stimulating the autophagic pathway without altering OBP-405 replication. Mice harboring intracranial tumors treated with OBP-405 and temozolomide survived significantly longer than those treated with temozolomide alone, and mice treated with OBP-405 and the rapamycin analog RAD001 survived significantly longer than those treated with RAD001 alone. The observation that autophagy inducers increase OBP-405 antitumor activity suggests a novel strategy for treating patients with glioblastoma.

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Autophagy-inducing agents augment the antitumor effect of telerase-selve oncolytic adenovirus OBP-405 on glioblastoma cells

Abstract

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