Novel REIC/Dkk-3-encoding adenoviral vector as a promising therapeutic agent for pancreatic cancer

被引:0
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作者
H Sawahara
H Shiraha
D Uchida
H Kato
T Nagahara
M Iwamuro
J Kataoka
S Horiguchi
M Watanabe
M Sakaguchi
A Takaki
K Nouso
Y Nasu
H Kumon
H Okada
机构
[1] Okayama University Graduate School of Medicine,Departments of Gastroenterology and Hepatology
[2] Dentistry,Departments of General Medicine
[3] and Pharmaceutical Sciences,Departments of Urology
[4] Okayama University Graduate School of Medicine,Departments of Cell Biology
[5] Dentistry,undefined
[6] and Pharmaceutical Sciences,undefined
[7] Okayama University Graduate School of Medicine,undefined
[8] Dentistry,undefined
[9] and Pharmaceutical Sciences,undefined
[10] Center for Innovative Clinical Medicine,undefined
[11] Okayama University Hospital,undefined
[12] Okayama University Graduate School of Medicine,undefined
[13] Dentistry,undefined
[14] and Pharmaceutical Sciences,undefined
[15] Innovation Center Okayama for Nanobio-Targeted Therapy,undefined
[16] Okayama University Graduate School of Medicine,undefined
[17] Dentistry,undefined
[18] and Pharmaceutical Sciences,undefined
来源
Cancer Gene Therapy | 2016年 / 23卷
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摘要
Reduced expression in immortalized cells (REIC)/dickkopf-3 (Dkk-3), a tumor suppressor gene, is downregulated in various cancers. We previously reported the tumor-inhibitory effects of the REIC/Dkk-3 gene, delivered by a conventional adenoviral vector (Ad-CAG-REIC) in pancreatic cancer. Here, we developed an Ad-REIC vector with a novel gene expression system, termed the super gene expression (SGE) system, and assessed its therapeutic effects relative to those of Ad-CAG-REIC in pancreatic cancer cells. Human pancreatic cancer cell lines ASPC1 and MIAPaCa2 were used. REIC/Dkk-3 expression was assessed by western blot analysis. Relative cell viability and apoptotic effects were examined in vitro. The anti-tumor effects of Ad-REIC treatment were assessed in the mouse xenograft model. Compared with Ad-CAG-REIC, Ad-SGE-REIC elicited a significant increase in REIC protein expression in the cells studied. Relative to Ad-CAG-REIC, Ad-SGE-REIC reduced cell viability and induced apoptosis in the ASPC1 and MIAPaCa2 cell lines in vitro, and achieved superior tumor growth inhibition in the mouse xenograft model. Compared with conventional Ad-REIC agents, Ad-SGE-REIC provided enhanced inhibitory effects against tumor growth. Our results indicate that Ad-SGE-REIC is an innovative therapeutic tool for pancreatic cancer.
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页码:278 / 283
页数:5
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