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Combination of the tumor angiogenesis inhibitor bevacizumab and intratumoral oncolytic herpes virus injections as a treatment strategy for human gastric cancers

机译:肿瘤血管生成抑制剂贝伐单抗和肿瘤内溶瘤性疱疹病毒注射剂的结合作为人类胃癌的治疗策略

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Background/Aims: Advanced gastric cancer is difficult to treat due to the frequency of liver metastases and peritoneal dissemination. A combination of two new strategies, including the anti-angiogenesis inhibitor Bevacizumab and an oncolytic herpes virus is a promising treatment for advanced cancer. Methodology: The effects of Bevacizumab on oncolytic herpes virus replication and viral cytotoxicity were examined at varying Bevacizumab concentrations and viral titers. In addition, the ability of these two new promising anticancer agents to inhibit tumor growth was studied. Histological examinations of CD31 and LacZ were used to assess angiogenesis and virus distribution within the tumor, respectively. Results: Bevacizumab did not affect viral replication or viral cytotoxicity in vitro. The combination of Bevacizumab and the oncolytic herpes virus hrR3 significantly reduced tumor growth in vivo in an experimental gastric cancer model. Bevacizumab inhibited angiogenesis caused by local injection of hrR3 and induced virus spread. Bevacizumab increased the distribution of the intratumorally injected oncolytic herpes virus within the tumor. Conclusions: Combination therapy consisting of Bevacizumab and an oncolytic herpes virus is a promising new treatment strategy for gastric cancer.
机译:背景/目的:由于肝转移和腹膜扩散的频率,晚期胃癌难以治疗。包括抗血管生成抑制剂贝伐单抗和溶瘤性疱疹病毒在内的两种新策略的组合是治疗晚期癌症的有希望的方法。方法:在不同的贝伐单抗浓度和病毒滴度下,检查了贝伐单抗对溶瘤性疱疹病毒复制和病毒细胞毒性的影响。另外,研究了这两种新的有希望的抗癌剂抑制肿瘤生长的能力。 CD31和LacZ的组织学检查分别用于评估肿瘤内的血管生成和病毒分布。结果:贝伐单抗在体外不影响病毒复制或病毒细胞毒性。贝伐单抗和溶瘤性疱疹病毒hrR3的组合在实验性胃癌模型中显着降低了体内肿瘤的生长。贝伐单抗抑制由hrR3的局部注射引起的血管生成并诱导病毒传播。贝伐单抗增加了肿瘤内注射溶瘤性疱疹病毒在肿瘤内的分布。结论:由贝伐单抗和溶瘤性疱疹病毒组成的联合治疗是胃癌的一种有希望的新治疗策略。

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