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Group B adenovirus enadenotucirev infects polarised colorectal cancer cells efficiently from the basolateral surface expected to be encountered during intravenous delivery to treat disseminated cancer

机译:B组Adenovirus Enadenotucirev通过预期的基础外侧表面感染偏振结直肠癌细胞,在静脉内递送期间遇到静脉分娩以治疗散发癌症

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摘要

Enadenotucirev (EnAd) is a group B oncolytic adenovirus developed for systemic delivery and currently undergoing clinical evaluation for advanced cancer therapy. For differentiated carcinomas, systemic delivery would likely expose virus particles to the basolateral surface of cancer cells rather than the apical surface encountered during natural infection. Here, we compare the ability of EnAd and adenovirus type-5 (Ad5) to infect polarised colorectal carcinoma cells from the apical or basolateral surfaces. Whereas Ad5 infection was more efficient via the apical than basolateral surface, EnAd readily infected cells from either surface. Progeny particles from EnAd were released preferentially via the apical surface for all cell lines and routes of infection. These data further support the utility of group B adenoviruses for systemic delivery and suggest that progeny virus are more likely to be released into the tumour rather than back through the basolateral surface into the blood stream.
机译:Enadenotucirev(ENAD)是B组氯霉素腺病毒,用于全身递送,目前正在接受晚期癌症治疗的临床评价。对于分化的癌,系统递送可能将病毒颗粒暴露于癌细胞的基外侧表面,而不是在自然感染期间遇到的顶端表面。在这里,我们比较eNAD和腺病毒类型-5(AD5)从顶端或基石表面感染偏振结直肠癌细胞的能力。虽然Ad5感染通过顶部的基础表面更有效,但eNAD容易受到任何表面的感染细胞。 eNAD的后代颗粒优先通过顶端表面释放,用于所有细胞系和感染途径。这些数据进一步支持B组腺病毒进行全身递送的效用,并表明后代病毒更容易被释放到肿瘤中,而不是通过基石表面释放到血流中。

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