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Optimizing targeted gene delivery: Chemical modification of viral vectors and synthesis of artificial virus vector systems

机译:优化靶向基因的传递:病毒载体的化学修饰和人工病毒载体系统的合成

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摘要

In comparison to classical medicines, gene therapy has the potential to mediate the highest possible level of therapeutic specificity. Every normal or diseased cell can switch on or off a gene expression cassette in a tissue-, disease-, and time-dependent fashion, by use of specific transcription factors that are active only in a given unique situation. In practice, we face the problem in realizing the concept: the delivery of nucleic acids into target cells is very ineffective and presents a formidable challenge. Key issues for future developments include improved targeting, enhanced intracellular uptake, and reduced toxicity of gene vectors. The currently used classes of vectors have complementary characteristics, such as high intracellular efficiency of viral vectors on the one hand and low immunogenicity and greater flexibility of nonviral vectors on the other hand. The merge of viral and nonviral vector technologies is highlighted as an encouraging strategy for the future; concepts include chemically modified viral vectors (“chemo-viruses”) and synthesis of virus-like systems (“synthetic viruses”). Examples for the development of vectors toward artificial synthetic viruses are presented.
机译:与经典药物相比,基因治疗有可能介导最高水平的治疗特异性。通过使用仅在给定的独特情况下才有活性的特定转录因子,每个正常或患病的细胞都可以以组织,疾病和时间依赖的方式打开或关闭基因表达盒。在实践中,我们在实现这一概念时面临问题:将核酸输送至靶细胞非常无效,并且提出了严峻的挑战。未来发展的关键问题包括改善靶向性,增强细胞内摄取以及降低基因载体的毒性。当前使用的载体类别具有互补的特征,例如一方面病毒载体的细胞内效率高,另一方面免疫原性低,并且非病毒载体的灵活性更高。病毒和非病毒载体技术的融合被强调为对未来的鼓励策略。概念包括化学修饰的病毒载体(“化学病毒”)和病毒样系统的合成(“合成病毒”)。提出了向人工合成病毒开发载体的实例。

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