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Strong antitumor efficacy of a pancreatic tumor-targeting oncolytic adenovirus for neuroendocrine tumors

机译:靶向胰腺肿瘤的溶瘤腺病毒对神经内分泌肿瘤的强抗肿瘤功效

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Abstract Although oncolytic adenoviruses are promising cancer therapy agents, for effective oncolytic activity, viruses need to specifically infect and effectively replicate in cancer cells but not in normal cells. We have previously identified a pancreatic cancer-targeting ligand, SYENFSA (SYE), by screening an adenovirus library displaying random peptides against human pancreatic cancer cells and reported that a survivin promoter-regulated adenovirus, displaying the SYE ligand (AdSur-SYE), provided effective oncolysis of pancreatic ductal adenocarcinoma (PDAC) in a preclinical study. As we examined the infectivity of AdSur-SYE in human surgical specimens of various pancreatic tumors, we unexpectedly found that AdSur-SYE showed high gene transduction efficiency for pancreatic neuroendocrine tumors (PNETs) as well as for PDAC, 9.1- and 6.2-fold, respectively, compared to that of the nontargeting virus (AdSur). The infectivity of both vectors was almost the same in other cancers and organs such as the pancreas. Immunostaining indicated that the cells infected with AdSur-SYE were PNET cells but not stromal cells. AdSur-SYE showed a significantly higher oncolytic potency than that of AdSur in human PNET cell lines, and intratumoral infection with AdSur-SYE completely diminished subcutaneous tumors in a murine model, in which AdSur-SYE effectively proliferated and spread. AdSur-SYE exerted a stronger oncolytic effect in primary PNET cells cocultured with mouse embryonic fibroblasts than AdSur did. Thus, AdSur-SYE shows promise as a next-generation therapy for PNET.
机译:摘要尽管溶瘤腺病毒是有前途的癌症治疗剂,但为了有效的溶瘤活性,病毒需要特异性感染并在癌细胞中有效复制,而不能在正常细胞中复制。我们以前通过筛选展示针对人类胰腺癌细胞的随机肽的腺病毒文库,鉴定了靶向胰腺癌的配体SYENFSA(SYE),并报道了由Survivin启动子调节的腺病毒,展示了SYE配体(AdSur-SYE),在临床前研究中有效治疗胰腺导管腺癌(PDAC)的溶瘤作用。当我们检查AdSur-SYE在各种胰腺肿瘤的人类手术标本中的感染力时,我们意外地发现AdSur-SYE对胰腺神经内分泌肿瘤(PNETs)和PDAC表现出高的基因转导效率,分别是9.1和6.2倍,与非靶向病毒(AdSur)相比。两种载体在其他癌症和器官(例如胰腺)中的感染力几乎相同。免疫染色表明感染AdSur-SYE的细胞是PNET细胞,而不是基质细胞。在人PNET细胞系中,AdSur-SYE的溶瘤效力比AdSur显着高,并且在鼠模型中,AdSur-SYE的肿瘤内感染完全消除了皮下肿瘤,其中AdSur-SYE有效地增殖和扩散。与AdSur相比,AdSur-SYE在与小鼠胚胎成纤维细胞共培养的原PNET细胞中具有更强的溶瘤作用。因此,AdSur-SYE有望成为PNET的下一代疗法。

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