Your search keyword '"Gao Pegn"' showing total 2 results

1. Potent anti-tumor effects of a dual specific oncolytic adenovirus expressing apoptin in vitro and in vivo

Author

Wang Yu-hang, Jin Ning-yi, Jin KuoShi, Sun Lili, Gao Pegn, Wang Zhuo-yue, Liu Yan, Kan Shifu, Yang Encheng, Xu Xiaohong, Lu HuiJun, Li Xiao, Wen Zhongmei, Tian MingYao, and Li Chang

Subjects

Oncolytic adenovirus, Cancer Research, Lung Neoplasms, DNA, Recombinant, Gene Expression, Antineoplastic Agents, Apoptosis, Biology, medicine.disease_cause, lcsh:RC254-282, Adenoviridae, Mice, chemistry.chemical_compound, Subcutaneous Tissue, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Transgenes, Melanoma, Telomerase, Cell Proliferation, Oncolytic Virotherapy, Research, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Survival Analysis, Primary tumor, Oncolytic virus, chemistry, Oncology, Organ Specificity, Cancer cell, Cancer research, Molecular Medicine, Adenovirus E1A Proteins, Growth inhibition, Apoptosis Regulatory Proteins

Abstract

Background Oncolytic virotherapy is an attractive drug platform of cancer gene therapy, but efficacy and specificity are important prerequisites for success of such strategies. Previous studies determined that Apoptin is a p53 independent, bcl-2 insensitive apoptotic protein with the ability to specifically induce apoptosis in tumor cells. Here, we generated a conditional replication-competent adenovirus (CRCA), designated Ad-hTERT-E1a-Apoptin, and investigated the effectiveness of the CRCA a gene therapy agent for further clinical trials. Results The observation that infection with Ad-hTERT-E1a-Apoptin significantly inhibited growth of the melanoma cells, protecting normal human epidermal melanocytes from growth inhibition confirmed cancer cell selective adenoviral replication, growth inhibition, and apoptosis induction of this therapeutic approach. The in vivo assays performed by using C57BL/6 mice containing established primary or metastatic tumors expanded the in vitro studies. When treated with Ad-hTERT-E1a-Apoptin, the subcutaneous primary tumor volume reduction was not only observed in intratumoral injection group but in systemic delivery mice. In the lung metastasis model, Ad-hTERT-E1a-Apoptin effectively suppressed pulmonary metastatic lesions. Furthermore, treatment of primary and metastatic models with Ad-hTERT-E1a-Apoptin increased mice survival. Conclusions These data further reinforce the previously research showing that an adenovirus expressing Apoptin is more effective and advocate the potential applications of Ad-hTERT-E1a-Apoptin in the treatment of neoplastic diseases in future clinical trials.

Published

2010

2. Potent anti-tumor effects of a dual specific oncolytic adenovirus expressing apoptin in vitro and in vivo.

Author

Li Xiao, Liu Yan, Wen Zhongmei, Li Chang, Lu Huijun, Tian Mingyao, Jin Kuoshi, Sun Lili, Gao Pegn, Yang Encheng, Xu Xiaohong, Kan Shifu, Wang Zhuoyue, Wang Yuhang, and Jin Ningyi

Subjects

GENE therapy, CANCER treatment, CANCER genetics, APOPTOSIS, CANCER cells, MELANOMA, LABORATORY mice

Abstract

Background: Oncolytic virotherapy is an attractive drug platform of cancer gene therapy, but efficacy and specificity are important prerequisites for success of such strategies. Previous studies determined that Apoptin is a p53 independent, bcl-2 insensitive apoptotic protein with the ability to specifically induce apoptosis in tumor cells. Here, we generated a conditional replication-competent adenovirus (CRCA), designated Ad-hTERT-E1a-Apoptin, and investigated the effectiveness of the CRCA a gene therapy agent for further clinical trials. Results: The observation that infection with Ad-hTERT-E1a-Apoptin significantly inhibited growth of the melanoma cells, protecting normal human epidermal melanocytes from growth inhibition confirmed cancer cell selective adenoviral replication, growth inhibition, and apoptosis induction of this therapeutic approach. The in vivo assays performed by using C57BL/6 mice containing established primary or metastatic tumors expanded the in vitro studies. When treated with Ad-hTERT-E1a-Apoptin, the subcutaneous primary tumor volume reduction was not only observed in intratumoral injection group but in systemic delivery mice. In the lung metastasis model, AdhTERT- E1a-Apoptin effectively suppressed pulmonary metastatic lesions. Furthermore, treatment of primary and metastatic models with Ad-hTERT-E1a-Apoptin increased mice survival. Conclusions: These data further reinforce the previously research showing that an adenovirus expressing Apoptin is more effective and advocate the potential applications of Ad-hTERT-E1a-Apoptin in the treatment of neoplastic diseases in future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2010