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首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >Brothers in arms: DNA enzymes, short interfering RNA, and the emerging wave of small-molecule nucleic acid-based gene-silencing strategies.
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Brothers in arms: DNA enzymes, short interfering RNA, and the emerging wave of small-molecule nucleic acid-based gene-silencing strategies.

机译:兄弟般的兄弟:DNA酶,短干扰RNA和新兴的基于小分子核酸的基因沉默策略浪潮。

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摘要

The past decade has seen the rapid evolution of small-molecule gene-silencing strategies, driven largely by enhanced understanding of gene function in the pathogenesis of disease. Over this time, many genes have been targeted by specifically engineered agents from different classes of nucleic acid-based drugs in experimental models of disease to probe, dissect, and characterize further the complex processes that underpin molecular signaling. Arising from this, a number of molecules have been examined in the setting of clinical trials, and several have recently made the successful transition from the bench to the clinic, heralding an exciting era of gene-specific treatments. This is particularly important because clear inadequacies in present therapies account for significant morbidity, mortality, and cost. The broad umbrella of gene-silencing therapeutics encompasses a range of agents that include DNA enzymes, short interfering RNA, antisense oligonucleotides, decoys, ribozymes, and aptamers. This review tracks current movements in these technologies, focusing mainly on DNA enzymes and short interfering RNA, because these are poised to play an integral role in antigene therapies in the future.
机译:在过去的十年中,小分子基因沉默策略的快速发展,很大程度上是由于人们对疾病发病机理中基因功能的增强理解。在这段时间里,许多基因已被疾病实验模型中来自不同类别基于核酸的药物的专门工程化试剂靶向,以进一步探查,解剖和表征支持分子信号传导的复杂过程。因此,已经在临床试验中检查了许多分子,最近一些分子已成功地从实验台过渡到临床,预示着基因特异性治疗的激动人心的时代。这一点特别重要,因为当前疗法中明显的不足之处导致了很大的发病率,死亡率和成本。基因沉默治疗剂的广泛范围涵盖了一系列试剂,包括DNA酶,短干扰RNA,反义寡核苷酸,诱饵,核酶和适体。这篇综述跟踪了这些技术的当前发展,主要集中在DNA酶和短干扰RNA,因为它们准备在将来的抗原疗法中发挥不可或缺的作用。

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