Melanoma differentiation-associated gene-7/interleukin-24 (mda-7/IL-24), a unique member of the IL-10 gene family, displays a broad range of antitumor properties including cancer-specific induction of apoptosis, inhibition of tumor angiogenesis, and modulation of anti-tumor immune responses. Here, we identify clusterin (CLU) as a MDA-7/IL-24 interacting protein in DU-145 cells and investigate the role of MDA-7/IL-24 in regulating CLU expression and mediating the antitumor properties of mda-7/IL-24 in prostate cancer. Ad.mda-7 decreased expression of soluble CLU (sCLU) and increased expression of nuclear CLU (nCLU). In the initial phase of Ad.mda-7 infection sCLU expression increased and CLU interacted with MDA-7/IL-24 producing a cytoprotective effect. Infection of stable clones of DU-145 prostate cancer cells expressing sCLU with Ad.mda-7 resulted in generation of nCLU that correlated with decreased cell viability and increased apoptosis. In the presence of mda-7/IL-24, sCLU-DU-145 cells displayed G2/M phase arrest followed by apoptosis. Similarly, Ad.mda-7 infection decreased cell migration by altering cytoskeleton in sCLU-DU-145 cells. Ad.mda-7-treated sCLU-DU-145 cells displayed a significant reduction in tumor growth in mouse xenograft models and reduced angiogenesis when compared to the vector control group. Tumor tissue lysates demonstrated enhanced nCLU generated from sCLU with increased apoptosis in the presence of MDA-7/IL-24. Our findings reveal novel aspects relative to the role of sCLU/nCLU in regulating the anticancer properties of MDA-7/IL-24 that may be exploited for developing enhanced therapies for prostate cancer.

mda-7/IL-24 differentially regulates soluble and nuclear clusterin in prostate cancer / Bhutia, Sk; Das, Sk; Kegelman, Tp; Azab, B; Dash, R; Su, Zz; Wang, Xy; Rizzi, Federica Maria Angela; Bettuzzi, Saverio; Lee, Sg; Dent, P; Grant, S; Curiel, Dt; Sarkar, D; Fisher, Pb. - In: JOURNAL OF CELLULAR PHYSIOLOGY. - ISSN 0021-9541. - 227(5):(2012), pp. 1805-1813. [10.1002/jcp.22904]

mda-7/IL-24 differentially regulates soluble and nuclear clusterin in prostate cancer

RIZZI, Federica Maria Angela;BETTUZZI, Saverio;
2012-01-01

Abstract

Melanoma differentiation-associated gene-7/interleukin-24 (mda-7/IL-24), a unique member of the IL-10 gene family, displays a broad range of antitumor properties including cancer-specific induction of apoptosis, inhibition of tumor angiogenesis, and modulation of anti-tumor immune responses. Here, we identify clusterin (CLU) as a MDA-7/IL-24 interacting protein in DU-145 cells and investigate the role of MDA-7/IL-24 in regulating CLU expression and mediating the antitumor properties of mda-7/IL-24 in prostate cancer. Ad.mda-7 decreased expression of soluble CLU (sCLU) and increased expression of nuclear CLU (nCLU). In the initial phase of Ad.mda-7 infection sCLU expression increased and CLU interacted with MDA-7/IL-24 producing a cytoprotective effect. Infection of stable clones of DU-145 prostate cancer cells expressing sCLU with Ad.mda-7 resulted in generation of nCLU that correlated with decreased cell viability and increased apoptosis. In the presence of mda-7/IL-24, sCLU-DU-145 cells displayed G2/M phase arrest followed by apoptosis. Similarly, Ad.mda-7 infection decreased cell migration by altering cytoskeleton in sCLU-DU-145 cells. Ad.mda-7-treated sCLU-DU-145 cells displayed a significant reduction in tumor growth in mouse xenograft models and reduced angiogenesis when compared to the vector control group. Tumor tissue lysates demonstrated enhanced nCLU generated from sCLU with increased apoptosis in the presence of MDA-7/IL-24. Our findings reveal novel aspects relative to the role of sCLU/nCLU in regulating the anticancer properties of MDA-7/IL-24 that may be exploited for developing enhanced therapies for prostate cancer.
2012
mda-7/IL-24 differentially regulates soluble and nuclear clusterin in prostate cancer / Bhutia, Sk; Das, Sk; Kegelman, Tp; Azab, B; Dash, R; Su, Zz; Wang, Xy; Rizzi, Federica Maria Angela; Bettuzzi, Saverio; Lee, Sg; Dent, P; Grant, S; Curiel, Dt; Sarkar, D; Fisher, Pb. - In: JOURNAL OF CELLULAR PHYSIOLOGY. - ISSN 0021-9541. - 227(5):(2012), pp. 1805-1813. [10.1002/jcp.22904]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11381/2426797
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