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Long Non-Coding RNA Targeting and Transcriptional De-Repression

机译:长时间非编码RNA靶向和转录抑制。

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摘要

Our current understanding of the molecular events that functionally characterize cellular biology continues to be revised. Recent observations find that the vast majority of the human genome is transcribed and may be functionally relevant. Many of these previously unrecognized transcripts, both short and long non-coding RNAs, have been found to be active modulators of protein coding gene function. While such observations were in the past relegated to imprinted genes, it is now becoming apparent that several different genes in differentiated cells may be under some form of non-coding RNA based regulatory control. Emerging evidence suggests that some of these long non-coding RNAs are functional in controlling gene transcription by the targeted recruitment of epigenetic silencing complexes to homology-containing loci in the genome. Most notably when these repressor non-coding RNAs are targeted using small RNA-based inhibitors (such as with RNA interference), a de-repression of the targeted gene can occur resulting in activation of gene expression. Knowledge of this emerging RNA based epigenetic regulatory network has implications not only in cellular evolution but also for the development of an entirely new area of pharmacology.
机译:我们目前对功能上表征细胞生物学的分子事件的理解仍在不断修订。最近的观察发现,人类基因组的绝大多数被转录并且可能在功能上相关。已经发现许多这些先前未被识别的转录本,短和长的非编码RNA,都是蛋白质编码基因功能的活性调节剂。尽管这些观察过去只限于印迹基因,但现在变得明显的是,分化细胞中的几种不同基因可能处于某种形式的基于非编码RNA的调控控制之下。新兴证据表明,这些长链非编码RNA中的某些在通过将表观遗传沉默复合体靶向募集到基因组中包含同源性的基因座中而控制基因转录的功能中。最值得注意的是,当使用基于RNA的小型抑制剂(例如受RNA干扰)靶向这些阻遏物非编码RNA时,会发生靶基因的抑制,导致基因表达激活。对这种新兴的基于RNA的表观遗传调控网络的了解不仅对细胞进化有影响,而且对药理学一个全新领域的发展也有影响。

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