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Modulation of gene-specific epigenetic states and transcription by non-coding RNAs

机译:非编码RNA调节基因特异性表观遗传状态和转录

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Emerging evidence points to a role for long non-coding RNAs in the modulation of epigenetic states and transcription in human cells. New insights, using various forms of small non-coding RNAs, suggest that a mechanism of action is operative in human cells, which utilizes non-coding RNAs to direct epigenetic marks to homology containing loci resulting ultimately in the epigenetic-based modulation of gene transcription. Importantly, insights into this mechanism of action have allowed for certain target sequences, which are either actively involved in RNA mediated epigenetic regulation or targets for non-coding RNA based epigenetic regulation, to be selected. As such, it is now feasible to utilize small antisense RNAs to either epigenetically silence a gene expression or remove epigenetic silencing of endogenous non-coding RNAs and essentially turn on a gene expression. Knowledge of this emerging RNA-based epigenetic regulatory network and our ability to cognitively control gene expression has deep implications in the development of an entirely new area of pharmacopeia.
机译:新兴证据表明长非编码RNA在人类细胞表观遗传状态和转录调控中的作用。使用各种形式的小型非编码RNA的新见解表明,一种作用机制在人类细胞中起作用,该机制利用非编码RNA将表观遗传标记引导至含有同源基因的同源基因,最终导致基于表观遗传的基因转录调控。重要的是,对这种作用机制的见解允许选择某些靶序列,这些靶序列要么积极参与RNA介导的表观遗传调控,要么选择基于非编码RNA的表观遗传调控的靶。因此,利用小型反义RNA来表观遗传沉默基因表达或消除内源性非编码RNA的表观遗传沉默并实质上开启基因表达是可行的。对这种新兴的基于RNA的表观遗传调控网络的了解以及我们认知控制基因表达的能力,对药典全新领域的发展产生了深远的影响。

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