National Institute of Pharmaceutical Education and Research (NIPER), Department of Biotechnology , Sector 67, S.A.S. Nagar, Punjab 160 062 , India
Expert Opin Drug Discov. 2011 May;6(5):507-26. doi: 10.1517/17460441.2011.565744. Epub 2011 Mar 16.
Antisense oligonucleotides (ASOs) are short synthetic single-stranded DNA sequences that bind to and induce the cleavage of homologous stretches of mRNA sequences. These result in targeted destruction of mRNA and correction of genetic aberrations. ASOs thus can act as drug molecules and potentially rectify many disease conditions. The broad range of applications reported in the literature highlights the advances in the field.
This review covers different areas in which use of ASOs has been shown to have therapeutic effects. Some drugs in different stages of preclinical and clinical trials are discussed in detail. The problems faced and the strategies to surmount them are also described. The readers will gain an understanding of the recent developments in the field of ASOs with emphasis on their therapeutic applications. They will also become aware of the different strategies used for targeted delivery of ASOs and their stabilization, which may be useful for their work in this field, or in the area of nucleic acid therapeutics in general.
The design and application of ASOs for recognition of target mRNA sequences have become a fairly straightforward protocol. The main problem lies in designing ASOs which are stable in in vivo milieu. The delivery and bioavailability of the oligonucleotide to the site of action continue to be hurdles in the development of ASOs and therapeutic molecules.
反义寡核苷酸(ASO)是短链合成单链 DNA 序列,可与同源 mRNA 序列结合并诱导其切割。这导致靶向破坏 mRNA 和纠正遗传异常。因此,ASO 可以作为药物分子,并有可能纠正许多疾病状况。文献中报道的广泛应用突出了该领域的进展。
本综述涵盖了 ASO 已显示出治疗效果的不同领域。详细讨论了不同临床前和临床试验阶段的一些药物。还描述了所面临的问题和克服这些问题的策略。读者将了解 ASO 领域的最新发展,并重点了解其治疗应用。他们还将意识到用于靶向递送 ASO 及其稳定化的不同策略,这对于他们在该领域或一般核酸治疗领域的工作可能是有用的。
设计和应用 ASO 来识别靶 mRNA 序列已成为相当简单的方案。主要问题在于设计在体内环境中稳定的 ASO。寡核苷酸递送至作用部位的传递和生物利用度仍然是 ASO 开发和治疗分子的障碍。
