通过溶瘤病毒治疗靶向肿瘤血管:最新进展。

IF 6.7 Oncolytic Virotherapy Pub Date : 2015-11-11 eCollection Date: 2015-01-01 DOI:10.2147/OV.S66045
Marcela Toro Bejarano, Jaime R Merchan
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引用次数: 25

摘要

溶瘤病毒治疗领域在过去十年中取得了重大进展,早期和后期临床试验数量迅速增加,其中一些显示出安全性和有希望的治疗效果。溶瘤病毒(OVs)靶向肿瘤血管系统是一种有吸引力的策略,与非靶向病毒相比,它具有许多优点,包括改善肿瘤病毒进入、直接抗血管作用和增强抗肿瘤疗效。目前对肿瘤新生血管的生物学机制、新的血管靶点和耐药机制的了解,使得设计靶向肿瘤新生血管的溶瘤病毒载体得以发展。虽然一些ov病毒(如牛痘病毒和水疱性口炎病毒)可以内在地靶向肿瘤血管系统并诱导血管破坏,但大多数已报道的血管靶向病毒是其病毒基因组遗传操作的结果。这些策略包括转录或转导内皮靶向,能够下调血管生成因子的“武装”病毒,或表达抗血管生成分子。上述策略无论是单独使用,还是与标准药物或靶向药物联合使用,均显示出临床前安全性和抗肿瘤疗效的提高。本文综述了近年来血管靶向OVs治疗癌症的研究进展,并为未来开发新一代人类癌症生物制剂提供了一个转化/临床前景。
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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Targeting tumor vasculature through oncolytic virotherapy: recent advances.

The oncolytic virotherapy field has made significant advances in the last decade, with a rapidly increasing number of early- and late-stage clinical trials, some of them showing safety and promising therapeutic efficacy. Targeting tumor vasculature by oncolytic viruses (OVs) is an attractive strategy that offers several advantages over nontargeted viruses, including improved tumor viral entry, direct antivascular effects, and enhanced antitumor efficacy. Current understanding of the biological mechanisms of tumor neovascularization, novel vascular targets, and mechanisms of resistance has allowed the development of oncolytic viral vectors designed to target tumor neovessels. While some OVs (such as vaccinia and vesicular stomatitis virus) can intrinsically target tumor vasculature and induce vascular disruption, the majority of reported vascular-targeted viruses are the result of genetic manipulation of their viral genomes. Such strategies include transcriptional or transductional endothelial targeting, "armed" viruses able to downregulate angiogenic factors, or to express antiangiogenic molecules. The above strategies have shown preclinical safety and improved antitumor efficacy, either alone, or in combination with standard or targeted agents. This review focuses on the recent efforts toward the development of vascular-targeted OVs for cancer treatment and provides a translational/clinical perspective into the future development of new generation biological agents for human cancers.

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