In vitro evaluation of cancer-specific NF-κB-CEA enhancer–promoter system for 5-fluorouracil prodrug gene therapy in colon cancer cell lines

Guo, Xiaoxia; Evans, T.R. Jeffry; Somanath, Sangeeta; Armesilla, Ángel Luis; Darling, John L.; Schätzlein, Andreas G.; Cassidy, James T.; Wang, Weiguang

doi:10.1038/sj.bjc.6603930

Cited by 15 publications

(7 citation statements)

References 31 publications

(42 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We found the highest expression among all colon cancer cells in HTC-116 cell lines (33.4%) and the lowest in T-84 cells (3.49%); whereas normal CCD18co cells revealed practically undetectable levels of CEA. These results for CEA promoter activity are similar to those described by Gou et al [ 31 ] and Dąbrowska et al [ 32 ], who also observed a greater CEA promoter activity in colon cancer cell lines than in non-tumor cancer cell lines using a luciferase assay.…”

Section: Discussionsupporting

confidence: 91%

Specific Colon Cancer Cell Cytotoxicity Induced by Bacteriophage E Gene Expression under Transcriptional Control of Carcinoembryonic Antigen Promoter

Rama

Hernández

Perazzoli

et al. 2015

IJMS

View full text Add to dashboard Cite

Colorectal cancer is one of the most prevalent cancers in the world. Patients in advanced stages often develop metastases that require chemotherapy and usually show a poor response, have a low survival rate and develop considerable toxicity with adverse symptoms. Gene therapy may act as an adjuvant therapy in attempts to destroy the tumor without affecting normal host tissue. The bacteriophage E gene has demonstrated significant antitumor activity in several cancers, but without any tumor-specific activity. The use of tumor-specific promoters may help to direct the expression of therapeutic genes so they act against specific cancer cells. We used the carcinoembryonic antigen promoter (CEA) to direct E gene expression (pCEA-E) towards colon cancer cells. pCEA-E induced a high cell growth inhibition of human HTC-116 colon adenocarcinoma and mouse MC-38 colon cancer cells in comparison to normal human CCD18co colon cells, which have practically undetectable levels of CEA. In addition, in vivo analyses of mice bearing tumors induced using MC-38 cells showed a significant decrease in tumor volume after pCEA-E treatment and a low level of Ki-67 in relation to untreated tumors. These results suggest that the CEA promoter is an excellent candidate for directing E gene expression specifically toward colon cancer cells.

show abstract

Section: Discussionsupporting

confidence: 91%

Specific Colon Cancer Cell Cytotoxicity Induced by Bacteriophage E Gene Expression under Transcriptional Control of Carcinoembryonic Antigen Promoter

Rama

Hernández

Perazzoli

et al. 2015

IJMS

View full text Add to dashboard Cite

show abstract

“…Few reports described the incorporation of genetic responsive elements to promoters for enhanced transcriptional regulation of therapeutic genes (Yew et al , 2001; Greco et al , 2002; Lee et al , 2002; Liu et al , 2004; Lee et al , 2006; Guo et al , 2007; Poulsen et al , 2008), but only one study attempted to combine NF-κB and HRE elements in a plasmid that conferred only a slight enhanced activity to the KDR promoter when assessed in primary murine endothelial cells (Modlich et al , 2000). Here we observed that both in a plasmid and in an adenoviral context the triple chimeric promoter increased its transcriptional activity greatly, leading to enhanced viral efficacy under hypoxia and upon TNF-α addition in human melanoma cells and fetal fibroblasts.…”

Section: Discussionmentioning

confidence: 99%

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Viale

Cafferata

Gould

et al. 2013

Journal of Investigative Dermatology

View full text Add to dashboard Cite

We have previously designed a conditionally replicative oncolytic adenovirus (CRAd) named Ad-F512 that can target both the stromal and the malignant melanoma cell compartments. The replication capacity of this CRAd is driven by a 0.5-Kb SPARC promoter fragment (named F512). To improve CRAd’s efficacy, we cloned into F512 motives responsive to hypoxia (hypoxia-responsive element (HRE)) and inflammation (nuclear factor kappa B) to obtain a chimeric promoter named κBF512HRE. Using luciferase as a reporter gene, we observed 10–15-fold increased activity under hypoxia and 10–80-fold induction upon tumor necrosis factor-α addition. We next constructed a CRAd (Ad-κBF512HRE) where E1A activity was under κBF512HRE regulation. Treatment of nude mice harboring established tumors made of a mix of SB2 melanoma cells and WI-38 fibroblasts with Ad-κBF512HRE led to the complete elimination of tumors in 100% of mice (8/8). Moreover, Ad-5/3-κBF512HRE, a viral variant pseudotyped with a chimeric 5/3 fiber, exerted a strong lytic effect on CAR-negative melanoma cells and was highly effective in vivo on established tumors made of melanoma cells and WI-38 fibroblasts, leading to the complete elimination of 4/5 tumors. These results indicate that this improved stroma-targeted oncolytic adenovirus can override the resistance of melanoma tumors and might become of significant importance for melanoma therapeutics.

show abstract

“…Carcinoembryonic antigen (CEA) promoter is active only in CEA-positive cells, an exclusive characteristic of vast tumor cells; the CEA promoter-controlled CD strategy confers toxic specificity for CEA-producing colorectal cancer cells while preserving activity [54]. Furthermore, by taking advantage of the knowledge that nuclear transcriptional factor NFkB is often highly transcribed in cancer cells, the addition of NF-kB enhancer to the CEA promoter significantly enhanced the efficacy of its driven CD/5-FC system in colon cancer cells [65]. In a study to select the optimal promoter to drive CD in a GDEPT strategy against gastric cancer, promoters of SEL1L, mucin-1 and KRT19 displayed the highest activity levels among several genes that are significantly highly expressed in gastric tumors [66].…”

Section: Gene-directed Enzyme Prodrug Therapymentioning

confidence: 99%

Viral-based gene delivery and regulated gene expression for targeted cancer therapy

Lü

Madu

2009

Expert Opinion on Drug Delivery

View full text Add to dashboard Cite

show abstract

In vitro evaluation of cancer-specific NF-κB-CEA enhancer–promoter system for 5-fluorouracil prodrug gene therapy in colon cancer cell lines

Cited by 15 publications

References 31 publications

Specific Colon Cancer Cell Cytotoxicity Induced by Bacteriophage E Gene Expression under Transcriptional Control of Carcinoembryonic Antigen Promoter

Specific Colon Cancer Cell Cytotoxicity Induced by Bacteriophage E Gene Expression under Transcriptional Control of Carcinoembryonic Antigen Promoter

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Viral-based gene delivery and regulated gene expression for targeted cancer therapy

Contact Info

Product

Resources

About