Overcoming the limitations of locally administered oncolytic virotherapy.

BMC biomedical engineering Pub Date : 2019-07-01 eCollection Date: 2019-01-01 DOI:10.1186/s42490-019-0016-x
JinWoo Hong, Chae-Ok Yun
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引用次数: 23

Abstract

Adenovirus (Ad) has been most extensively evaluated gene transfer vector in clinical trials due to facile production in high viral titer, highly efficient transduction, and proven safety record. Similarly, an oncolytic Ad, which replicates selectively in cancer cells through genetic modifications, is actively being evaluated in various phases of clinical trials as a promising next generation therapeutic against cancer. Most of these trials with oncolytic Ads to date have employed intratumoral injection as the standard administration route. Although these locally administered oncolytic Ads have shown promising outcomes, the therapeutic efficacy is not yet optimal due to poor intratumoral virion retention, nonspecific shedding of virion to normal organs, variable infection efficacy due to heterogeneity of tumor cells, adverse antiviral immune response, and short biological activity of oncolytic viruses in situ. These inherent problems associated with locally administered Ad also holds true for other oncolytic viral vectors. Thus, this review will aim to discuss various nanomaterial-based delivery strategies to improve the intratumoral administration efficacy of oncolytic Ad as well as other types of oncolytic viruses.

克服局部给药溶瘤病毒治疗的局限性。
腺病毒(Ad)由于其易于生产、高病毒滴度、高效转导和已证实的安全记录,在临床试验中被广泛评价为基因转移载体。同样,一种溶瘤性Ad,通过基因修饰在癌细胞中选择性复制,正在临床试验的各个阶段被积极评估为有希望的下一代癌症治疗方法。迄今为止,大多数溶瘤性广告的试验都采用肿瘤内注射作为标准给药途径。尽管这些局部给药的溶瘤病毒已显示出良好的效果,但由于肿瘤内病毒粒子潴留差、病毒粒子向正常器官的非特异性脱落、肿瘤细胞异质性导致的感染效果不稳定、抗病毒免疫反应不良以及溶瘤病毒在原位的生物活性短,治疗效果尚不理想。这些与局部给药Ad相关的固有问题也适用于其他溶瘤病毒载体。因此,本综述旨在讨论各种基于纳米材料的递送策略,以提高溶瘤性Ad和其他类型溶瘤病毒的肿瘤内给药效果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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