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溶瘤病毒作为治疗剂。

Oncolytic viruses as therapeutic agents.

作者信息

Wildner O

机构信息

Humboldt-Universität zu Berlin, Labor für Gentherapie, Germany.

出版信息

Ann Med. 2001 Jul;33(5):291-304. doi: 10.3109/07853890109002081.

Abstract

The concept of using viruses as oncolytic agents has a long history. However, relatively new developments are the use of these viruses as gene delivery vehicles and the restriction of viral replication and lysis to tumour cells. The latter is attempted by the use of tumour-specific promoters, which transcriptionally target viral genes involved in replication, or by deletion of viral functions dispensable for replication in tumour cells but essential for productive infection of normal cells. In addition, retargeting of the viral tropism towards tumours by capsid modifications has been examined. Although much progress has been made in developing oncolytic vectors for clinical use, there is still a long way to go to determine which combinations of virus, gene therapy, surgery, radiation, and/or chemotherapy will provide improved therapy for the control and eradication of a variety of human cancers. First controlled clinical trials with an oncolytic adenovirus in combination with chemotherapy have shown encouraging antineoplastic activity. For future vector developments it will be crucial to achieve maximum vector distribution and transgene expression within tumours, to trigger a specific systemic immune effector response against treated and untreated lesions, and to modulate the immune system to avoid immune-mediated inactivation or destruction of the virus. In the context of replication-competent vectors, suicide genes might be used as fail-safe mechanism in the case of a runaway infection.

摘要

将病毒用作溶瘤剂的概念由来已久。然而,相对较新的进展是将这些病毒用作基因传递载体,并将病毒复制和裂解限制在肿瘤细胞内。后者可通过使用肿瘤特异性启动子来实现,该启动子可转录靶向参与复制的病毒基因,或者通过缺失在肿瘤细胞中复制所必需但对正常细胞有效感染必不可少的病毒功能来实现。此外,还研究了通过衣壳修饰将病毒嗜性重新靶向肿瘤的方法。尽管在开发用于临床的溶瘤载体方面已经取得了很大进展,但要确定病毒、基因治疗、手术、放疗和/或化疗的哪些组合将为控制和根除各种人类癌症提供更好的治疗方法,仍有很长的路要走。首次使用溶瘤腺病毒联合化疗的对照临床试验已显示出令人鼓舞的抗肿瘤活性。对于未来的载体开发,关键在于在肿瘤内实现最大程度的载体分布和转基因表达,引发针对已治疗和未治疗病变的特异性全身免疫效应反应,并调节免疫系统以避免免疫介导的病毒失活或破坏。在具有复制能力的载体的背景下,自杀基因可在感染失控时用作故障安全机制。

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