Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway

S. Shamimi-Noori; W. S. Yeow; M. F. Ziauddin; H. Xin; T. L.N. Tran; J. Xie; A. Loehfelm; P. Patel; J. Yang; D. S. Schrump; B. L. Fang; D. M. Nguyen

doi:10.1038/sj.cgt.7701120

Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway

S. Shamimi-Noori, W. S. Yeow, M. F. Ziauddin, H. Xin, T. L.N. Tran, J. Xie, A. Loehfelm, P. Patel, J. Yang, D. S. Schrump, B. L. Fang, D. M. Nguyen

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

36 Scopus citations

Abstract

Despite adequately expressing tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptors DR4/DR5, malignant cells are frequently refractory to the cytotoxic effect of this apoptosis-inducing ligand. The susceptibility of cancer cells to TRAIL can be potentiated by cisplatin (CDDP). This study was designed to evaluate the ability of cisplatin to enhance the cytotoxic effect of TRAIL gene therapy using the recombinant adenovirus-mediated tumor-selective expression of membrane-bound green fluorescence protein (GFP)-TRAIL fusion protein (AdVgTRAIL) on thoracic cancer cells and to elucidate the putative mechanisms responsible for this synergistic combination effect. While causing little death of cultured thoracic cancer cells by itself, AdVgTRAIL in combination with CDDP, on the other hand, mediated profound supra-additive cytotoxicity and apoptosis via a strong bystander effect. CDDP/AdVgTRAIL-induced cytotoxicity was completely abrogated either by the pancaspase inhibitor zVAD-fmk or by the selective caspase 9 inhibitor or by transient knockdown of caspase 9 by siRNA, indicating that this process was caspase-mediated and mitochondria-dependent. This was confirmed by the observation that Bcl2 overexpression protected the cells from combination-induced cytotoxicity. Robust activation of caspase 8 activity in combination-treated cells was blocked by overexpression of Bcl2, indicating that caspase 8 activation was secondary to the mitochondria-mediated amplification feedback loop. Combining CDDP with AdVgTRAIL greatly enhances its tumoricidal efficacy in cultured thoracic cancer cells in vitro. The two agents interact to mediate profound activation of caspase cascade via recruitment of the mitochondria and positive feedback loop. The CDDP/AdVgTRAIL combination also exhibits a strong antitumor effect in in vivo animal model of human cancer xenografts.

Original language	English (US)
Pages (from-to)	356-370
Number of pages	15
Journal	Cancer Gene Therapy
Volume	15
Issue number	6
DOIs	https://doi.org/10.1038/sj.cgt.7701120
State	Published - Jun 2008
Externally published	Yes

Keywords

Adenovirus
Esophageal cancer
Lung cancer
Mesothelioma
Mitochondria
TRAIL

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1038/sj.cgt.7701120

Cite this

Shamimi-Noori, S., Yeow, W. S., Ziauddin, M. F., Xin, H., Tran, T. L. N., Xie, J., Loehfelm, A., Patel, P., Yang, J., Schrump, D. S., Fang, B. L., & Nguyen, D. M. (2008). Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway. Cancer Gene Therapy, 15(6), 356-370. https://doi.org/10.1038/sj.cgt.7701120

Shamimi-Noori, S, Yeow, WS, Ziauddin, MF, Xin, H, Tran, TLN, Xie, J, Loehfelm, A, Patel, P, Yang, J, Schrump, DS, Fang, BL & Nguyen, DM 2008, 'Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway', Cancer Gene Therapy, vol. 15, no. 6, pp. 356-370. https://doi.org/10.1038/sj.cgt.7701120

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title = "Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway",

abstract = "Despite adequately expressing tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptors DR4/DR5, malignant cells are frequently refractory to the cytotoxic effect of this apoptosis-inducing ligand. The susceptibility of cancer cells to TRAIL can be potentiated by cisplatin (CDDP). This study was designed to evaluate the ability of cisplatin to enhance the cytotoxic effect of TRAIL gene therapy using the recombinant adenovirus-mediated tumor-selective expression of membrane-bound green fluorescence protein (GFP)-TRAIL fusion protein (AdVgTRAIL) on thoracic cancer cells and to elucidate the putative mechanisms responsible for this synergistic combination effect. While causing little death of cultured thoracic cancer cells by itself, AdVgTRAIL in combination with CDDP, on the other hand, mediated profound supra-additive cytotoxicity and apoptosis via a strong bystander effect. CDDP/AdVgTRAIL-induced cytotoxicity was completely abrogated either by the pancaspase inhibitor zVAD-fmk or by the selective caspase 9 inhibitor or by transient knockdown of caspase 9 by siRNA, indicating that this process was caspase-mediated and mitochondria-dependent. This was confirmed by the observation that Bcl2 overexpression protected the cells from combination-induced cytotoxicity. Robust activation of caspase 8 activity in combination-treated cells was blocked by overexpression of Bcl2, indicating that caspase 8 activation was secondary to the mitochondria-mediated amplification feedback loop. Combining CDDP with AdVgTRAIL greatly enhances its tumoricidal efficacy in cultured thoracic cancer cells in vitro. The two agents interact to mediate profound activation of caspase cascade via recruitment of the mitochondria and positive feedback loop. The CDDP/AdVgTRAIL combination also exhibits a strong antitumor effect in in vivo animal model of human cancer xenografts.",

keywords = "Adenovirus, Esophageal cancer, Lung cancer, Mesothelioma, Mitochondria, TRAIL",

author = "S. Shamimi-Noori and Yeow, {W. S.} and Ziauddin, {M. F.} and H. Xin and Tran, {T. L.N.} and J. Xie and A. Loehfelm and P. Patel and J. Yang and Schrump, {D. S.} and Fang, {B. L.} and Nguyen, {D. M.}",

note = "Funding Information: This work was support by the Intramural Research Program of the National Cancer Institute of The National Institutes of Health and the start-up funds of the DeWitt Daughter Family Department of Surgery and the Sylvester Comprehensive Cancer Center, University of Miami. We acknowledge the contributions of Mr Arnold Mixon and Mr Shawn Farid of the Flow Cytometry Core Facility, Surgery Branch, Center for Cancer Research, NCI/NIH.",

year = "2008",

month = jun,

doi = "10.1038/sj.cgt.7701120",

language = "English (US)",

volume = "15",

pages = "356--370",

journal = "Cancer Gene Therapy",

issn = "0929-1903",

publisher = "Nature Publishing Group",

number = "6",

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TY - JOUR

T1 - Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway

AU - Shamimi-Noori, S.

AU - Yeow, W. S.

AU - Ziauddin, M. F.

AU - Xin, H.

AU - Tran, T. L.N.

AU - Xie, J.

AU - Loehfelm, A.

AU - Patel, P.

AU - Yang, J.

AU - Schrump, D. S.

AU - Fang, B. L.

AU - Nguyen, D. M.

N1 - Funding Information: This work was support by the Intramural Research Program of the National Cancer Institute of The National Institutes of Health and the start-up funds of the DeWitt Daughter Family Department of Surgery and the Sylvester Comprehensive Cancer Center, University of Miami. We acknowledge the contributions of Mr Arnold Mixon and Mr Shawn Farid of the Flow Cytometry Core Facility, Surgery Branch, Center for Cancer Research, NCI/NIH.

PY - 2008/6

Y1 - 2008/6

N2 - Despite adequately expressing tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptors DR4/DR5, malignant cells are frequently refractory to the cytotoxic effect of this apoptosis-inducing ligand. The susceptibility of cancer cells to TRAIL can be potentiated by cisplatin (CDDP). This study was designed to evaluate the ability of cisplatin to enhance the cytotoxic effect of TRAIL gene therapy using the recombinant adenovirus-mediated tumor-selective expression of membrane-bound green fluorescence protein (GFP)-TRAIL fusion protein (AdVgTRAIL) on thoracic cancer cells and to elucidate the putative mechanisms responsible for this synergistic combination effect. While causing little death of cultured thoracic cancer cells by itself, AdVgTRAIL in combination with CDDP, on the other hand, mediated profound supra-additive cytotoxicity and apoptosis via a strong bystander effect. CDDP/AdVgTRAIL-induced cytotoxicity was completely abrogated either by the pancaspase inhibitor zVAD-fmk or by the selective caspase 9 inhibitor or by transient knockdown of caspase 9 by siRNA, indicating that this process was caspase-mediated and mitochondria-dependent. This was confirmed by the observation that Bcl2 overexpression protected the cells from combination-induced cytotoxicity. Robust activation of caspase 8 activity in combination-treated cells was blocked by overexpression of Bcl2, indicating that caspase 8 activation was secondary to the mitochondria-mediated amplification feedback loop. Combining CDDP with AdVgTRAIL greatly enhances its tumoricidal efficacy in cultured thoracic cancer cells in vitro. The two agents interact to mediate profound activation of caspase cascade via recruitment of the mitochondria and positive feedback loop. The CDDP/AdVgTRAIL combination also exhibits a strong antitumor effect in in vivo animal model of human cancer xenografts.

AB - Despite adequately expressing tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptors DR4/DR5, malignant cells are frequently refractory to the cytotoxic effect of this apoptosis-inducing ligand. The susceptibility of cancer cells to TRAIL can be potentiated by cisplatin (CDDP). This study was designed to evaluate the ability of cisplatin to enhance the cytotoxic effect of TRAIL gene therapy using the recombinant adenovirus-mediated tumor-selective expression of membrane-bound green fluorescence protein (GFP)-TRAIL fusion protein (AdVgTRAIL) on thoracic cancer cells and to elucidate the putative mechanisms responsible for this synergistic combination effect. While causing little death of cultured thoracic cancer cells by itself, AdVgTRAIL in combination with CDDP, on the other hand, mediated profound supra-additive cytotoxicity and apoptosis via a strong bystander effect. CDDP/AdVgTRAIL-induced cytotoxicity was completely abrogated either by the pancaspase inhibitor zVAD-fmk or by the selective caspase 9 inhibitor or by transient knockdown of caspase 9 by siRNA, indicating that this process was caspase-mediated and mitochondria-dependent. This was confirmed by the observation that Bcl2 overexpression protected the cells from combination-induced cytotoxicity. Robust activation of caspase 8 activity in combination-treated cells was blocked by overexpression of Bcl2, indicating that caspase 8 activation was secondary to the mitochondria-mediated amplification feedback loop. Combining CDDP with AdVgTRAIL greatly enhances its tumoricidal efficacy in cultured thoracic cancer cells in vitro. The two agents interact to mediate profound activation of caspase cascade via recruitment of the mitochondria and positive feedback loop. The CDDP/AdVgTRAIL combination also exhibits a strong antitumor effect in in vivo animal model of human cancer xenografts.

KW - Adenovirus

KW - Esophageal cancer

KW - Lung cancer

KW - Mesothelioma

KW - Mitochondria

KW - TRAIL

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Cisplatin enhances the antitumor effect of tumor necrosis factor-related apoptosis-inducing ligand gene therapy via recruitment of the mitochondria-dependent death signaling pathway

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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