肿瘤缺氧与靶向基因治疗。

Olga Greco, Simon Scott
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引用次数: 13

摘要

缺氧是肿瘤微环境的一个整体特征,主要是由于伴随肿瘤加速生长的微血管缺陷。肿瘤缺氧区域的存在与放疗、化疗和手术后的负面结果相关,因为缺氧不仅提供了直接促进化疗和放射耐药的环境,而且还促进了表型变化的进化,从而导致对治疗的永久耐药和转移性扩散。因此,成功治疗缺氧细胞不仅可以改善局部控制,还可以影响患者的整体生存。基因治疗的所有三个步骤都可以实现对缺氧肿瘤区域的特异性和选择性靶向:将治疗基因传递到肿瘤,调节基因表达和治疗效果。本文就低氧靶向基因治疗的最新进展和创新进行了综述。特别是,诸如缺氧条件复制病毒、细胞载体和基因治疗手段等方法可以破坏缺氧诱导因子(HIF)信号。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tumor hypoxia and targeted gene therapy.

Hypoxia is an integral characteristic of the tumor microenvironment, primarily due to the microvascular defects that accompany the accelerated neoplastic growth. The presence of tumor hypoxic areas correlates with negative outcome after radiotherapy, chemotherapy, and surgery, as hypoxia not only provides an environment directly facilitating chemo- and radio-resistance, but also encourages the evolution of phenotypic changes inducing permanent resistance to treatment and metastatic spread. Therefore, successful treatment of hypoxic cells has the potential to not only improve local control but also impact overall patient survival. Specific and selective targeting of hypoxic tumor areas can be achieved at all three steps of a gene therapy treatment: delivery of the therapeutic gene to the tumor, regulation of gene expression, and therapeutic efficacy. In this review the latest developments and innovations in hypoxia-targeted gene therapy are discussed. In particular, approaches such as hypoxia-conditionally replicating viruses, cellular vehicles, and gene therapy means to disrupt the hypoxia-inducible factor (HIF) signaling are outlined.

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