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首页> 外文期刊>Annals of the New York Academy of Sciences >Small molecule targeting of RNA structures in neurological disorders
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Small molecule targeting of RNA structures in neurological disorders

机译:神经障碍RNA结构的小分子靶向

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摘要

Aberrant RNA structure and function operate in neurological disease progression and severity. As RNA contributes to disease pathology in a complex fashion, that is, via various mechanisms, it has become an attractive therapeutic target for small molecules and oligonucleotides. In this review, we discuss the identification of RNA structures that cause or contribute to neurological diseases as well as recent progress toward the development of small molecules that target them, including small molecule modulators of pre-mRNA splicing and RNA repeat expansions that cause microsatellite disorders such as Huntington's disease and amyotrophic lateral sclerosis. The use of oligonucleotide-based modalities is also discussed. There are key differences between small molecule and oligonucleotide targeting of RNA. The former targets RNA structure, while the latter prefers unstructured regions. Thus, some targets will be preferentially targeted by oligonucleotides and others by small molecules.
机译:异常RNA结构和功能在神经疾病进展和严重程度下运行。随着RNA以复杂的方式促进疾病病理,即通过各种机制,它已成为小分子和寡核苷酸的有吸引力的治疗靶标。在本次综述中,我们讨论了导致或有助于神经疾病的RNA结构的鉴定以及最近朝着靶向它们的小分子的进展,包括引起微卫星障碍的前mRNA剪接和RNA重复膨胀的小分子调节剂如亨廷顿的疾病和肌萎缩的外侧硬化。还讨论了使用寡核苷酸的方式。在RNA的小分子和寡核苷酸靶向之间存在关键差异。前者靶向RNA结构,而后者更喜欢非结构化的地区。因此,一些靶标的通过小分子优先由寡核苷酸和其他靶向靶向。

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