胎盘发育和疾病中的长非编码RNA

T. Basak, R. Ain
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引用次数: 14

摘要

为了重新定义表转录组学,长非编码RNA(lncRNA)正在成为刻板生物科学范式转变的未来前沿。长非编码RNA(lncRNA)代表一类内源性RNA分子,其长度大于200个核苷酸,但不超过100千碱基,不编码蛋白质,但由RNA聚合酶II转录并多腺苷酸化。与蛋白质编码基因不同,它们表现出较差的种间保守性。然而,缺乏序列守恒并不意味着缺乏功能。事实上,这种进化保守性的缺乏对lncRNA的功能研究提出了挑战。lncRNA研究的最新进展表明,它们以前被表征为普遍转录的产物,是转录和转录后水平上基因调控的必要介质。越来越多的RNA测序数据正在扩大lncRNA的库存,以从根本上剖析真核生物复杂性的结构。在过去的二十年里,一系列研究发现了相当多的胎盘lncRNA。然而,鉴于胎盘发育的复杂性,人们对其生物学功能提出了许多问题。尽管如此,在整个妊娠期间,在母体循环中鉴定胎盘来源的lncRNA,提高了lncRNA被评估为导致不良妊娠结果的滋养层相关疾病的预后生物标志物的前景。在这篇综述中,我们总结了胎儿-母体器官-胎盘发育过程中lncRNA研究的最新进展,以及作为胎盘相关妊娠并发症主要决定因素的lncRNA功能失调的关键发现。
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Long non-coding RNAs in placental development and disease
To reconceptualize epitranscriptomics, long non-coding RNAs (lncRNAs) are emerging as future frontiers in the paradigm shift of stereotyped biological science. Long non-coding RNAs (lncRNA) represent a class of endogenous RNA molecules with length greater than 200 nucleotides but not exceeding 100 kilobases that do not encode proteins, yet transcribed by RNA Polymerase II and are poly-adenylated. Unlike protein-coding genes, they exhibit poor interspecies conservation. However, lack of sequence conservation does not imply the lack of function. Indeed, this dearth in evolutionary conservation challenges the functional investigation of lncRNAs. Previously characterized as products of pervasive transcription, recent advances in lncRNA research proposes them as imperative mediators of gene regulation at the transcription and post-transcriptional level. Ever-increasing amount of RNA sequencing data is expanding the lncRNA inventory to fundamentally dissect the architecture of eukaryotic complexity. Over the last two decades a flurry of studies identified quite a few placental lncRNAs. However, given the complexity of placental development, many questions have been raised regarding their biological function. Nonetheless, identification of lncRNAs of placental origin in the maternal circulation throughout pregnancy raised the prospect of lncRNAs being evaluated as prognostic biomarker of trophoblast associated disorders leading to adverse pregnancy outcome. In this review, we summarize key findings on the recent advances in lncRNA research during the development of the feto-maternal organ placenta and dys-regulations of lncRNA functionalities as prime determinants of placenta associated pregnancy complications.
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