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Oncolytic Virus with Attributes of Vesicular Stomatitis Virus and Measles Virus in Hepatobiliary and Pancreatic Cancers

机译:具有肝胆道和胰腺癌症的囊泡口炎病毒和麻疹病毒的溶瘤病毒

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摘要

Recombinant vesicular stomatitis virus (VSV)-fusion and hemagglutinin (FH) was developed by substituting the promiscuous VSV-G glycoprotein (G) gene in the backbone of VSV with genes encoding for the measles virus envelope proteins F and H. Hybrid VSV-FH exhibited a multifaceted mechanism of cancer-cell killing and improved neurotolerability over parental VSV in preclinical studies. In this study, we evaluated VSV-FH in vitro and in vivo in models of hepatobiliary and pancreatic cancers. Our results indicate that high intrahepatic doses of VSV-FH did not result in any significant toxicity and were well tolerated by transgenic mice expressing the measles virus receptor CD46. Furthermore, a single intratumoral treatment with VSV-FH yielded improved survival and complete tumor regressions in a proportion of mice in the Hep3B hepatocellular carcinoma model but not in mice xenografted with BxPC-3 pancreatic cancer cells. Our preliminary findings indicate that VSV-FH can induce potent oncolysis in hepatocellular and pancreatic cancer cell lines with concordant results in vivo in hepatocellular cancer and discordant in pancreatic cancer without the VSV-mediated toxic effects previously observed in laboratory animals. Further study of VSV-FH as an oncolytic virotherapy is warranted in hepatocellular carcinoma and pancreatic cancer to understand broader applicability and mechanisms of sensitivity and resistance.
机译:通过在VSV的骨干中用编码麻疹病毒包膜蛋白F和H. Hybrid VSV-FH的基因代替VSV中的混合物VSV-G糖蛋白(G)基因来开发重组膜气炎病毒(VSV) - 熔融和血凝素(FH)。在临床前研究中表现出癌细胞杀伤和改善神经核细胞的多方核细胞性能。在这项研究中,我们在肝胆和胰腺癌模型中进行了体外和体内的VSV-FH。我们的结果表明,高肝内剂量的VSV-FH不会导致任何显着的毒性,并通过表达麻疹病毒受体CD46的转基因小鼠耐受良好耐受。此外,用VSV-FH的单一肿瘤内处理在HEP3B肝细胞癌模型中的一部分小鼠中产生了改善的存活和完全肿瘤回归,但不含BxPC-3胰腺癌细胞的小鼠异种移植物。我们的初步发现表明,VSV-FH可以在肝细胞癌和胰腺癌细胞系中诱导有效的溶解,并在肝细胞癌中体内导致肝细胞癌和在胰腺癌中不和谐而在实验动物中以前观察到的VSV介导的毒性作用。在肝细胞癌和胰腺癌中有必要进一步研究VSV-FH,以了解更广泛的适用性和敏感性和抗性机制。

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