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Current development of targeted oligonucleotide-based cancer therapies: Perspective on HER2-positive breast cancer treatment

机译:靶向寡核苷酸为基础的癌症治疗的最新进展:HER2阳性乳腺癌治疗的前景

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摘要

This Review discusses the various types of non-coding oligonucleotides, which have garnered extensive interest as new alternatives for targeted cancer therapies over small molecule inhibitors and monoclonal antibodies. These oligonucleotides can target any hallmark of cancer, no longer limited to so-called “druggable” targets. Thus, any identified gene that plays a key role in cancer progression or drug resistance can be exploited with oligonucleotides. Among them, small-interfering RNAs (siRNAs) are frequently utilized for gene silencing due to the robust and well established mechanism of RNA interference. Despite promising advantages, clinical translation of siRNAs is hindered by the lack of effective delivery platforms. This Review provides general criteria and consideration of nanoparticle development for systemic siRNA delivery. Different classes of nanoparticle candidates for siRNA delivery are discussed, and the progress in clinical trials for systemic cancer treatment is reviewed. Lastly, this Review presents HER2 (human epidermal growth factor receptor type 2)-positive breast cancer as one example that could benefit significantly from siRNA technology. How siRNA-based therapeutics can overcome cancer resistance to such therapies is discussed.
机译:这篇综述讨论了各种类型的非编码寡核苷酸,它们作为靶向治疗的新替代方法已经引起了人们的广泛关注,这些替代方法比小分子抑制剂和单克隆抗体更具优势。这些寡核苷酸可以靶向任何癌症标志物,而不再局限于所谓的“可吸收”靶标。因此,任何鉴定出的在癌症进展或耐药性中起关键作用的基因都可被寡核苷酸利用。其中,由于RNA干扰的牢固和完善的机制,小干扰RNA(siRNA)经常用于基因沉默。尽管有前景可观的优势,但缺乏有效的递送平台仍阻碍了siRNA的临床翻译。这篇综述提供了用于系统性siRNA递送的纳米粒子发展的一般标准和考虑。讨论了用于siRNA递送的不同类别的纳米粒子候选物,并综述了系统性癌症治疗的临床试验进展。最后,本综述提出了HER2(人类表皮生长因子受体2型)阳性乳腺癌的例子,可以从siRNA技术中受益匪浅。讨论了基于siRNA的疗法如何克服癌症对此类疗法的耐药性。

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