mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience

Irina V. Lebedeva; Luni Emdad; Zao Zhong Su; Pankaj Gupta; Moira Sauane; Devanand Sarkar; Michelle R. Staudt; Shi Jian Liu; Mohiuddin M. Taher; Ruoyu Xiao; Paola Barral; Seok Geun Lee; Dongning Wang; Nicollaq Vozhilla; Eun Sook Park; Lejuan Chatman; Habib Boukerche; Rajagopal Ramesh; Satoshi Inoue; Sunil Chada; Rong Li; Anthony L. De Pass; Parameshwar J. Mahasreshti; Igor P. Dmitriev; David T. Curiel; Adly Yacoub; Steven Grant; Paul Dent; Neil Senzer; John J. Nemunaitis; Paul B. Fisher

mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience

Irina V. Lebedeva, Luni Emdad, Zao Zhong Su, Pankaj Gupta, Moira Sauane, Devanand Sarkar, Michelle R. Staudt, Shi Jian Liu, Mohiuddin M. Taher, Ruoyu Xiao, Paola Barral, Seok Geun Lee, Dongning Wang, Nicollaq Vozhilla, Eun Sook Park, Lejuan Chatman, Habib Boukerche, Rajagopal Ramesh, Satoshi Inoue, Sunil ChadaRong Li, Anthony L. De Pass, Parameshwar J. Mahasreshti, Igor P. Dmitriev, David T. Curiel, Adly Yacoub, Steven Grant, Paul Dent, Neil Senzer, John J. Nemunaitis, Paul B. Fisher

Medicine - Veteran's Administration Medical Center

Research output: Contribution to journal › Review article › peer-review

93 Scopus citations

Abstract

Subtraction hybridization applied to a 'differentiation therapy' model of cancer employing human melanoma cells resulted in the cloning of melanoma differentiation associated gene-7/interleukin-24 (mda-7/IL-24). Initial studies confirm an inverse correlation between mda-7 expression and melanoma development and progression. Forced expression of mda-7 by means of a plasmid or via a replication incompetent adenovirus (Ad.mda-7) promotes growth suppression and induces apoptosis in a broad array of human cancers. In contrast, mda-7 does not induce growth suppressive or toxic effects in normal cells. Based on structure (containing an IL-10 signature motif), secretion by cells (including subsets of T-cells) and location on chromosome 1q (in an area containing IL-10-family genes), mda-7 has now been renamed mda-7/IL-24. Studies by several laboratories have uncovered many of mda-7/ IL-24's unique properties, including cancer-specific apoptosis-induction, cell cycle regulation, an ability to inhibit angiogenesis, potent 'bystander antitumor activity' and a capacity to enhance the sensitivity of tumor cells to radiation, chemotherapy and monoclonal antibody therapy. Moreover, based on its profound cancer tropism, substantiated by in vivo human xenograft studies in nude mice, mda-7/IL-24 (administered as Ad.mda-7) was evaluated in a phase I clinical trial in patients with melanomas and solid cancers. These studies document that mda-7/IL-24 is well tolerated and demonstrates evidence of significant clinical activity. In these contexts, mda-7/IL-24 represents a unique cytokine gene with potential for therapy of human cancers. The present review focuses on three unique properties of mda-7/IL-24, namely its potent 'bystander antitumor activity', ability to sensitize tumor cells to radiation, and its antiangiogenesis properties. Additionally, an overview of the phase I clinical trial is provided. These studies affirm that mda-7/IL-24 has promise for the management of diverse cancers.

Original language	English (US)
Pages (from-to)	985-1007
Number of pages	23
Journal	International Journal of Oncology
Volume	31
Issue number	5
State	Published - Nov 2007

Keywords

Antiangiogenesis
Apoptosis
Bystander effect
Phase I clinical trial
Radio-sensitization
mda-7/IL-24

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

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Lebedeva, I. V., Emdad, L., Su, Z. Z., Gupta, P., Sauane, M., Sarkar, D., Staudt, M. R., Liu, S. J., Taher, M. M., Xiao, R., Barral, P., Lee, S. G., Wang, D., Vozhilla, N., Park, E. S., Chatman, L., Boukerche, H., Ramesh, R., Inoue, S., ... Fisher, P. B. (2007). mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience. International Journal of Oncology, 31(5), 985-1007.

mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience. / Lebedeva, Irina V.; Emdad, Luni; Su, Zao Zhong et al.
In: International Journal of Oncology, Vol. 31, No. 5, 11.2007, p. 985-1007.

Research output: Contribution to journal › Review article › peer-review

Lebedeva, IV, Emdad, L, Su, ZZ, Gupta, P, Sauane, M, Sarkar, D, Staudt, MR, Liu, SJ, Taher, MM, Xiao, R, Barral, P, Lee, SG, Wang, D, Vozhilla, N, Park, ES, Chatman, L, Boukerche, H, Ramesh, R, Inoue, S, Chada, S, Li, R, De Pass, AL, Mahasreshti, PJ, Dmitriev, IP, Curiel, DT, Yacoub, A, Grant, S, Dent, P, Senzer, N, Nemunaitis, JJ & Fisher, PB 2007, 'mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience', International Journal of Oncology, vol. 31, no. 5, pp. 985-1007.

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abstract = "Subtraction hybridization applied to a 'differentiation therapy' model of cancer employing human melanoma cells resulted in the cloning of melanoma differentiation associated gene-7/interleukin-24 (mda-7/IL-24). Initial studies confirm an inverse correlation between mda-7 expression and melanoma development and progression. Forced expression of mda-7 by means of a plasmid or via a replication incompetent adenovirus (Ad.mda-7) promotes growth suppression and induces apoptosis in a broad array of human cancers. In contrast, mda-7 does not induce growth suppressive or toxic effects in normal cells. Based on structure (containing an IL-10 signature motif), secretion by cells (including subsets of T-cells) and location on chromosome 1q (in an area containing IL-10-family genes), mda-7 has now been renamed mda-7/IL-24. Studies by several laboratories have uncovered many of mda-7/ IL-24's unique properties, including cancer-specific apoptosis-induction, cell cycle regulation, an ability to inhibit angiogenesis, potent 'bystander antitumor activity' and a capacity to enhance the sensitivity of tumor cells to radiation, chemotherapy and monoclonal antibody therapy. Moreover, based on its profound cancer tropism, substantiated by in vivo human xenograft studies in nude mice, mda-7/IL-24 (administered as Ad.mda-7) was evaluated in a phase I clinical trial in patients with melanomas and solid cancers. These studies document that mda-7/IL-24 is well tolerated and demonstrates evidence of significant clinical activity. In these contexts, mda-7/IL-24 represents a unique cytokine gene with potential for therapy of human cancers. The present review focuses on three unique properties of mda-7/IL-24, namely its potent 'bystander antitumor activity', ability to sensitize tumor cells to radiation, and its antiangiogenesis properties. Additionally, an overview of the phase I clinical trial is provided. These studies affirm that mda-7/IL-24 has promise for the management of diverse cancers.",

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language = "English (US)",

volume = "31",

pages = "985--1007",

journal = "International Journal of Oncology",

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T1 - mda-7/IL-24, novel anticancer cytokine

T2 - Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience

AU - Lebedeva, Irina V.

AU - Emdad, Luni

AU - Su, Zao Zhong

AU - Gupta, Pankaj

AU - Sauane, Moira

AU - Sarkar, Devanand

AU - Staudt, Michelle R.

AU - Liu, Shi Jian

AU - Taher, Mohiuddin M.

AU - Xiao, Ruoyu

AU - Barral, Paola

AU - Lee, Seok Geun

AU - Wang, Dongning

AU - Vozhilla, Nicollaq

AU - Park, Eun Sook

AU - Chatman, Lejuan

AU - Boukerche, Habib

AU - Ramesh, Rajagopal

AU - Inoue, Satoshi

AU - Chada, Sunil

AU - Li, Rong

AU - De Pass, Anthony L.

AU - Mahasreshti, Parameshwar J.

AU - Dmitriev, Igor P.

AU - Curiel, David T.

AU - Yacoub, Adly

AU - Grant, Steven

AU - Dent, Paul

AU - Senzer, Neil

AU - Nemunaitis, John J.

AU - Fisher, Paul B.

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Y1 - 2007/11

N2 - Subtraction hybridization applied to a 'differentiation therapy' model of cancer employing human melanoma cells resulted in the cloning of melanoma differentiation associated gene-7/interleukin-24 (mda-7/IL-24). Initial studies confirm an inverse correlation between mda-7 expression and melanoma development and progression. Forced expression of mda-7 by means of a plasmid or via a replication incompetent adenovirus (Ad.mda-7) promotes growth suppression and induces apoptosis in a broad array of human cancers. In contrast, mda-7 does not induce growth suppressive or toxic effects in normal cells. Based on structure (containing an IL-10 signature motif), secretion by cells (including subsets of T-cells) and location on chromosome 1q (in an area containing IL-10-family genes), mda-7 has now been renamed mda-7/IL-24. Studies by several laboratories have uncovered many of mda-7/ IL-24's unique properties, including cancer-specific apoptosis-induction, cell cycle regulation, an ability to inhibit angiogenesis, potent 'bystander antitumor activity' and a capacity to enhance the sensitivity of tumor cells to radiation, chemotherapy and monoclonal antibody therapy. Moreover, based on its profound cancer tropism, substantiated by in vivo human xenograft studies in nude mice, mda-7/IL-24 (administered as Ad.mda-7) was evaluated in a phase I clinical trial in patients with melanomas and solid cancers. These studies document that mda-7/IL-24 is well tolerated and demonstrates evidence of significant clinical activity. In these contexts, mda-7/IL-24 represents a unique cytokine gene with potential for therapy of human cancers. The present review focuses on three unique properties of mda-7/IL-24, namely its potent 'bystander antitumor activity', ability to sensitize tumor cells to radiation, and its antiangiogenesis properties. Additionally, an overview of the phase I clinical trial is provided. These studies affirm that mda-7/IL-24 has promise for the management of diverse cancers.

AB - Subtraction hybridization applied to a 'differentiation therapy' model of cancer employing human melanoma cells resulted in the cloning of melanoma differentiation associated gene-7/interleukin-24 (mda-7/IL-24). Initial studies confirm an inverse correlation between mda-7 expression and melanoma development and progression. Forced expression of mda-7 by means of a plasmid or via a replication incompetent adenovirus (Ad.mda-7) promotes growth suppression and induces apoptosis in a broad array of human cancers. In contrast, mda-7 does not induce growth suppressive or toxic effects in normal cells. Based on structure (containing an IL-10 signature motif), secretion by cells (including subsets of T-cells) and location on chromosome 1q (in an area containing IL-10-family genes), mda-7 has now been renamed mda-7/IL-24. Studies by several laboratories have uncovered many of mda-7/ IL-24's unique properties, including cancer-specific apoptosis-induction, cell cycle regulation, an ability to inhibit angiogenesis, potent 'bystander antitumor activity' and a capacity to enhance the sensitivity of tumor cells to radiation, chemotherapy and monoclonal antibody therapy. Moreover, based on its profound cancer tropism, substantiated by in vivo human xenograft studies in nude mice, mda-7/IL-24 (administered as Ad.mda-7) was evaluated in a phase I clinical trial in patients with melanomas and solid cancers. These studies document that mda-7/IL-24 is well tolerated and demonstrates evidence of significant clinical activity. In these contexts, mda-7/IL-24 represents a unique cytokine gene with potential for therapy of human cancers. The present review focuses on three unique properties of mda-7/IL-24, namely its potent 'bystander antitumor activity', ability to sensitize tumor cells to radiation, and its antiangiogenesis properties. Additionally, an overview of the phase I clinical trial is provided. These studies affirm that mda-7/IL-24 has promise for the management of diverse cancers.

KW - Antiangiogenesis

KW - Apoptosis

KW - Bystander effect

KW - Phase I clinical trial

KW - Radio-sensitization

KW - mda-7/IL-24

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AN - SCOPUS:38449096542

SN - 1019-6439

VL - 31

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JO - International Journal of Oncology

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ER -

mda-7/IL-24, novel anticancer cytokine: Focus on bystander antitumor, radiosensitization and antiangiogenic properties and overview of the phase I clinical experience

Abstract

Keywords

UN SDGs

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