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A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect

Cancer Targeting Gene-Viro-Therapy (CTGVT) is a promising cancer therapeutical strategy that strengthens the anti-tumour effect of oncolytic virus by expressing inserted foreign anti-tumour genes. In this work, we constructed a novel adenoviral vector controlled by the tumour-specific survivin promo...

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Detalles Bibliográficos
Autores principales: Liu, Xin-Ran, Cai, Ying, Cao, Xin, Wei, Rui-Cheng, Li, Hui-Ling, Zhou, Xiu-Mei, Zhang, Kang-Jian, Wu, Shuai, Qian, Qi-Jun, Cheng, Biao, Huang, Kun, Liu, Xin-Yuan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3823082/
https://www.ncbi.nlm.nih.gov/pubmed/21794078
http://dx.doi.org/10.1111/j.1582-4934.2011.01396.x
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author Liu, Xin-Ran
Cai, Ying
Cao, Xin
Wei, Rui-Cheng
Li, Hui-Ling
Zhou, Xiu-Mei
Zhang, Kang-Jian
Wu, Shuai
Qian, Qi-Jun
Cheng, Biao
Huang, Kun
Liu, Xin-Yuan
author_facet Liu, Xin-Ran
Cai, Ying
Cao, Xin
Wei, Rui-Cheng
Li, Hui-Ling
Zhou, Xiu-Mei
Zhang, Kang-Jian
Wu, Shuai
Qian, Qi-Jun
Cheng, Biao
Huang, Kun
Liu, Xin-Yuan
author_sort Liu, Xin-Ran
collection PubMed
description Cancer Targeting Gene-Viro-Therapy (CTGVT) is a promising cancer therapeutical strategy that strengthens the anti-tumour effect of oncolytic virus by expressing inserted foreign anti-tumour genes. In this work, we constructed a novel adenoviral vector controlled by the tumour-specific survivin promoter on the basis of the ZD55 vector, which is an E1B55KD gene deleted vector we previously constructed. Compared with the original ZD55 vector, this new adenoviral vector (ZD55SP/E1A) showed much better ability of replication and reporter gene expression. We then combined anti-tumour gene interleukine-24 (IL-24) with an RNA polymerase III-dependent U6 promoter driving short hairpin RNA (shRNA) that targets M-phase phosphoprotein 1 (MPHOSPH1, a newly identified oncogene) by inserting the IL-24 and the shRNA of MPHOSPH1 (shMPP1) expression cassettes into the new ZD55SP/E1A vector. Our results demonstrated excellent anti-tumour effect of ZD55SP/E1A-IL-24-shMPP1 in vitro on multiple cancer cell lines such as lung cancer, liver cancer and ovarian caner. At high multiplicity-of-infection (MOI), ZD55SP/E1A-IL-24-shMPP1 triggered post-mitotic apoptosis in cancer cells by inducing prolonged mitotic arrest; while at low MOI, senescence was induced. More importantly, ZD55SP/E1A-IL-24-shMPP1 also showed excellent anti-tumour effects in vivo on SW620 xenograft nude mice. In conclusion, our strategy of constructing an IL-24 and shMPP1 dual gene expressing oncolytic adenoviral vector, which is regulated by the survivin promoter and E1B55KD deletion, could be a promising method of cancer gene therapy.
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spelling pubmed-38230822015-03-27 A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect Liu, Xin-Ran Cai, Ying Cao, Xin Wei, Rui-Cheng Li, Hui-Ling Zhou, Xiu-Mei Zhang, Kang-Jian Wu, Shuai Qian, Qi-Jun Cheng, Biao Huang, Kun Liu, Xin-Yuan J Cell Mol Med Original Articles Cancer Targeting Gene-Viro-Therapy (CTGVT) is a promising cancer therapeutical strategy that strengthens the anti-tumour effect of oncolytic virus by expressing inserted foreign anti-tumour genes. In this work, we constructed a novel adenoviral vector controlled by the tumour-specific survivin promoter on the basis of the ZD55 vector, which is an E1B55KD gene deleted vector we previously constructed. Compared with the original ZD55 vector, this new adenoviral vector (ZD55SP/E1A) showed much better ability of replication and reporter gene expression. We then combined anti-tumour gene interleukine-24 (IL-24) with an RNA polymerase III-dependent U6 promoter driving short hairpin RNA (shRNA) that targets M-phase phosphoprotein 1 (MPHOSPH1, a newly identified oncogene) by inserting the IL-24 and the shRNA of MPHOSPH1 (shMPP1) expression cassettes into the new ZD55SP/E1A vector. Our results demonstrated excellent anti-tumour effect of ZD55SP/E1A-IL-24-shMPP1 in vitro on multiple cancer cell lines such as lung cancer, liver cancer and ovarian caner. At high multiplicity-of-infection (MOI), ZD55SP/E1A-IL-24-shMPP1 triggered post-mitotic apoptosis in cancer cells by inducing prolonged mitotic arrest; while at low MOI, senescence was induced. More importantly, ZD55SP/E1A-IL-24-shMPP1 also showed excellent anti-tumour effects in vivo on SW620 xenograft nude mice. In conclusion, our strategy of constructing an IL-24 and shMPP1 dual gene expressing oncolytic adenoviral vector, which is regulated by the survivin promoter and E1B55KD deletion, could be a promising method of cancer gene therapy. Blackwell Publishing Ltd 2012-06 2012-05-28 /pmc/articles/PMC3823082/ /pubmed/21794078 http://dx.doi.org/10.1111/j.1582-4934.2011.01396.x Text en Copyright © 2012 Foundation for Cellular and Molecular Medicine/Blackwell Publishing Ltd.
spellingShingle Original Articles
Liu, Xin-Ran
Cai, Ying
Cao, Xin
Wei, Rui-Cheng
Li, Hui-Ling
Zhou, Xiu-Mei
Zhang, Kang-Jian
Wu, Shuai
Qian, Qi-Jun
Cheng, Biao
Huang, Kun
Liu, Xin-Yuan
A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title_full A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title_fullStr A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title_full_unstemmed A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title_short A new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
title_sort new oncolytic adenoviral vector carrying dual tumour suppressor genes shows potent anti-tumour effect
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3823082/
https://www.ncbi.nlm.nih.gov/pubmed/21794078
http://dx.doi.org/10.1111/j.1582-4934.2011.01396.x
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