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Non-viral gene delivery using nanoparticles.

机译:使用纳米颗粒的非病毒基因递送。

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摘要

Although the potential benefits of gene therapy for the treatment of acquired and inherited genetic diseases have been demonstrated through preclinical studies, the results of human gene therapy trials have been disappointing. Recombinant viruses are the primary vectors of choice because of their ability to protect genetic materials, cross cellular membranes, escape from endosomes and transport their genetic materials into the nucleus. Unfortunately, viral vectors have been unable to gain widespread clinical application because of their toxicity and immunogenicity. Consequently, the need for safer alternatives has led to the development of liposomes, cationic polyplexes, microparticles and nanoparticles. Although these alternative vectors have shown promise, degradable nanoparticles are the only non-viral vectors that can provide a targeted intracellular delivery with controlled release properties. Furthermore, the potential advantage of degradable nanoparticles over their non-degradable counterparts is the reduced toxicity and the avoidance of accumulation within the target tissue after repeated administration. In this article, current non-viral gene delivery devices are reviewed with a special emphasis on nanoparticle gene delivery systems. Also, the authors highlight their philosophy and efforts on the development of l-tyrosine-based polyphosphate nanoparticle-based non-viral gene delivery systems and assess the potential benefits and shortcomings of their approach.
机译:尽管通过临床前研究已经证明了基因疗法在治疗获得性和遗传性遗传疾病方面的潜在益处,但人类基因疗法的试验结果却令人失望。重组病毒是首选的主要载体,因为它们能够保护遗传物质,穿越细胞膜,逃脱内体并将其遗传物质转运到细胞核中。不幸的是,由于其毒性和免疫原性,病毒载体无法获得广泛的临床应用。因此,对更安全替代品的需求导致了脂质体,阳离子多聚体,微粒和纳米颗粒的发展。尽管这些替代载体已显示出希望,但可降解的纳米颗粒是唯一可以提供具有控制释放特性的靶向细胞内递送的非病毒载体。此外,可降解纳米粒子相对于其不可降解对应物的潜在优势是毒性降低,并且避免了重复给药后靶组织内的积累。在本文中,对当前的非病毒基因递送设备进行了综述,其中特别强调了纳米颗粒基因递送系统。此外,作者强调了他们在基于酪氨酸的聚磷酸盐纳米颗粒非病毒基因递送系统的开发上的理念和努力,并评估了其方法的潜在优势和不足。

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