Grim-19 expressed by recombinant adenovirus for esophageal neoplasm target therapy.
[No authors listed]
摘要
Esophageal squamous cell carcinoma (ESCC) and esophageal adenocarcinoma (EA) are the two most common types of esophageal cancer, which is the sixth highest cause of cancerâassociated mortality and the eighth most common cancer worldwide. Gene associated with retinoidâinterferon (IFN)âinduced mortalityâ19 (Grimâ19) is reported to be a cell death activator that may be used to define mechanisms involved in IFNâβâ and retinoic acidâinduced cell death and apoptosis in a number of tumor cell lines. The present study constructed a recombinant adenovirus expressing Grimâ19 (rAdâGrimâ19) and investigated its therapeutic outcomes in ESCC cells and tumorâbearing mice. Grimâ19 expression was detected in ECâ109 (ESCC) cells by reverse transcriptionâquantitative polymerase chain reaction and western blot analysis. Tumor cell death and apoptosis induced by rAdâGrimâ19 in ECâ109 cells were analyzed by flow cytometry. The inhibitory effects of rAdâGrimâ19 on ECâ109 growth were determined by MTT assays. Furthermore, the therapeutic effects of rAdâGrimâ19 were investigated in ECâ109âbearing mice. The results demonstrated that Grimâ19 mRNA and protein expression was downregulated in ECâ109 esophageal carcinoma cells compared with Hetâ1A normal esophageal epithelial cells. In addition, ECâ109 cells exhibited a significant reduction in tumor cell growth in the rAdâGrimâ19 group compared with the control groups. Furthermore, rAdâGrimâ19 increased ECâ109 cell apoptosis compared with the control group. These results indicated that rAd-Grim-19 may regulate tumor cell growth and apoptosis. Additionally, the results demonstrated that rAdâGrimâ19 led to beneficial outcomes and prolonged the survival of esophageal tumorâbearing mice. In conclusion, the present study demonstrated that rAdâGrimâ19 may have potential as an antitumor agent for esophageal neoplasms and may therefore be beneficial for patients with esophageal neoplasms.
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基因功能
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原始数据
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文献解读
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