Tumor suppressor in lung cancer-1 (TSLC1) mediated by dual-regulated oncolytic adenovirus exerts specific antitumor actions in a mouse model

Lei, Wen; Liu, Hongbin; Wang, Shibing; Zhou, Xiumei; Zheng, Shui-di; Guo, Keni; Ma, Bo; Xia, Yu-long; Tan, Wen‐Song; Liu, Xinyuan; Wang, Yigang

doi:10.1038/aps.2012.196

Cited by 21 publications

(11 citation statements)

References 39 publications

(49 reference statements)

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“…Oncolytic virus has emerged as one of the most prospective anticancer drugs because the engineered viruses can successfully tackle cancer cells without damaging normal tissue [ 15 ]. Several excellent genetically modified oncolytic virus including vaccine virus JX-594, herpes simplex virus OncoVEX-GM-CSF, adenovirus H101, and reovirus Reolysin have been successfully used to treat various cancers in clinic and obtained specific cancer-killing effect [ 14 ]. In addition, oncolytic virus can induce the immune response against the tumor through releasing antigens when virus attacked cancer cells [ 23 ].…”

Section: Discussionmentioning

confidence: 99%

“…However, ZD55 lacks the targeting ability for specific tumor type such as liver cancer. Thus, to improve the specific killing effect of oncolytic adenovirus on one type of cancer, one common strategy to design oncolytic adenoviruses is to use cancer or tissue-specific promoter to control the expression of viral essential gene for replication, which is the transcriptional targeted strategy [ 13 , 14 ]. It causes the viral gene selectively expression in tumor cells, then the virus could only replicate in and kill tumor cells [ 7 , 15 ].…”

Section: Introductionmentioning

confidence: 99%

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A novel Golgi protein (GOLPH2)-regulated oncolytic adenovirus exhibits potent antitumor efficacy in hepatocellular carcinoma

et al. 2015

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Golgi apparatus is the organelle mainly functioning as protein processing and secretion. GOLPH2 is a resident Golgi glycoprotein, usually called GP73. Recent data displayed that GOLPH2 is a superb hepatocellular carcinoma (HCC) marker candidate, and even its specificity is better than liver cancer marker AFP. Oncolytic adenoviruses are broadly used for targeting cancer therapy due to their selective tumor-killing effect. However, it was reported that traditionally oncolytic adenovirus lack the HCC specificity. In this study, a novel dual-regulated oncolytic adenovirus GD55 targeting HCC was first constructed based on our cancer targeted gene-viral therapeutic strategy. To verify the targeting and effectiveness of GOLPH2-regulated oncolytic adenovirus GD55 in HCC, the anticancer capacity was investigated in HCC cell lines and animal model. The results proved that the novel GOLPH2-regulated GD55 conferred higher adenovirus replication and infectivity for liver cancer cells than oncolytic adenovirus ZD55. The GOLPH2-regulated GD55 exerted a significant grow-suppressing effect on HCC cells in vitro but little damage to normal liver cells. In animal experiment, antitumor effect of GD55 was more effective in HCC xenograft of nude mice than that of ZD55. Thus GOLPH2-regulated GD55 may be a promising oncolytic virus agent for future liver cancer treatment.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A novel Golgi protein (GOLPH2)-regulated oncolytic adenovirus exhibits potent antitumor efficacy in hepatocellular carcinoma

et al. 2015

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“…Cell Adhesion Molecule 1 is a protein that has been found to be strongly expressed in neurons, [71][72][73][74][75] spermatogenic cells, [52,[76][77][78] immune cells, [79][80][81][82][83][84][85][86][87] and endothelial cells [88,89]. Functionally, CADM1 has been shown to participate in homophilic binding, and paradoxically, tumor suppression.…”

Section: Cadm1: An Additional Role For a Versatile Protein?mentioning

confidence: 99%

Tumor Necrosis Factor α Regulates Endothelial Progenitor Cell Migration via CADM1 and NF-kB

et al. 2016

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Shortly after the discovery of endothelial progenitor cells (EPCs) in 1997, many clinical trials were conducted using EPCs as a cellular based therapy with the goal of restoring damaged organ function by inducing growth of new blood vessels (angiogenesis). Results were disappointing, largely because the cellular and molecular mechanisms of EPC-induced angiogenesis were not clearly understood. Following injection, EPCs must migrate to the target tissue and engraft prior to induction of angiogenesis. In this study EPC migration was investigated in response to tumor necrosis factor α (TNFα), a pro-inflammatory cytokine, to test the hypothesis that organ damage observed in ischemic diseases induces an inflammatory signal that is important for EPC homing. In this study, EPC migration and incorporation were modeled in vitro using a co-culture assay where TNFα treated EPCs were tracked while migrating towards vessel-like structures. It was found that TNFα treatment of EPCs increased migration and incorporation into vessel-like structures. Using a combination of genomic and proteomic approaches, NF-kB mediated upregulation of CADM1 was identified as a mechanism of TNFα induced migration. Inhibition of NF-kB or CADM1 significantly decreased migration of EPCs in vitro suggesting a role for TNFα signaling in EPC homing during tissue repair.

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“…Other than E1B detection, another common mutant of adenoviruses is the 24 bp deletion of the E1A retinoblastoma (Rb) binding site (∆24). Mutant adenoviruses show obvious tumor selectivity because viral replication is promoted in tumor cells with a defective Rb/p16 pathway and abolished in normal cells with intact Rb/p16[ 37 ]. Most cancer cells and CSCs harbor defects in the Rb and/or p53 pathway, which makes it possible to use OncoAd to eradicate the gastrointestinal cancer cells.…”

Section: Oncolytic Virotherapymentioning

confidence: 99%

Oncolytic viruses against cancer stem cells: A promising approach for gastrointestinal cancer

Huang

Wang

et al. 2016

WJG

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Gastrointestinal cancer has been one of the five most commonly diagnosed and leading causes of cancer mortality over the past few decades. Great progress in traditional therapies has been made, which prolonged survival in patients with early cancer, yet tumor relapse and drug resistance still occurred, which is explained by the cancer stem cell (CSC) theory. Oncolytic virotherapy has attracted increasing interest in cancer because of its ability to infect and lyse CSCs. This paper reviews the basic knowledge, CSC markers and therapeutics of gastrointestinal cancer (liver, gastric, colon and pancreatic cancer), as well as research advances and possible molecular mechanisms of various oncolytic viruses against gastrointestinal CSCs. This paper also summarizes the existing obstacles to oncolytic virotherapy and proposes several alternative suggestions to overcome the therapeutic limitations.

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Tumor suppressor in lung cancer-1 (TSLC1) mediated by dual-regulated oncolytic adenovirus exerts specific antitumor actions in a mouse model

Cited by 21 publications

References 39 publications

A novel Golgi protein (GOLPH2)-regulated oncolytic adenovirus exhibits potent antitumor efficacy in hepatocellular carcinoma

A novel Golgi protein (GOLPH2)-regulated oncolytic adenovirus exhibits potent antitumor efficacy in hepatocellular carcinoma

Tumor Necrosis Factor α Regulates Endothelial Progenitor Cell Migration via CADM1 and NF-kB

Oncolytic viruses against cancer stem cells: A promising approach for gastrointestinal cancer

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