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A possible role for long non-coding RNA in modulating signaling pathways.

机译:长的非编码RNA在调节信号通路中的可能作用。

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Signaling proteins often engage in multiple protein-protein interactions that are dependent upon cellular context. Little is known about how signaling proteins select their interacting targets. The Ras GTPase is an example of a protein that can activate a large number of distinct and interconnected downstream signaling pathways. Hyperactive forms of Ras are commonly found in a variety of different cancers, often due to somatic mutations within the RAS gene. Despite extensive studies to identify Ras-regulated pathways, it is still not known exactly which pathways might be activated by hyperactive Ras in a given cellular and disease context. Long non-coding RNAs (lncRNAs) are RNA transcripts longer than 200 bp exhibiting spatially and temporally-regulated expression patterns. LncRNAs have been shown to harbor biological activities but the functions of the great majority of lncRNAs are not known. We hypothesize that long non-coding RNAs serve as signaling modulators linking Ras and potentially other signaling proteins to their specific downstream targets and may therefore play a key role in how signals are propagated in a specific cellular environment. In support of our hypothesis we argue that lncRNAs have been shown to bind and regulate protein complexes targeting their enzymatic activity towards specific substrates. It has also been demonstrated that specific lncRNAs are expressed in particular types of cancers where they may influence tumor progression. Studies suggest that lncRNAs have evolved to help regulate complex biological processes that require the ability to stringently discriminate between a large number of potential effectors. If our hypothesis is correct, we envision that it will be possible to predict the target pathway of a mutant protein based on the lncRNA profile in a specific cancer. More generally, this will expand our understanding of how signal transduction networks are wired within a given biological context.
机译:信号蛋白经常参与多种依赖细胞背景的蛋白相互作用。关于信号蛋白如何选择其相互作用靶点,人们所知甚少。 Ras GTPase是可以激活大量不同且相互连接的下游信号通路的蛋白质的一个例子。过度活跃的Ras常见于多种不同的癌症中,通常是由于RAS基因内的体细胞突变所致。尽管进行了广泛的研究来确定Ras调控的途径,但仍不清楚在给定的细胞和疾病情况下,过度活跃的Ras可能激活哪些途径。长的非编码RNA(lncRNA)是长于200 bp的RNA转录本,表现出时空调控的表达模式。 LncRNA已被证明具有生物活性,但大多数lncRNA的功能尚不清楚。我们假设长的非编码RNA充当将Ras和潜在的其他信号蛋白连接到其特定下游靶标的信号调节剂,因此可能在信号在特定细胞环境中的传播中起关键作用。为了支持我们的假设,我们认为lncRNA已显示出结合并调节针对其特定底物的酶活性的蛋白质复合物。还已经证明,特定的lncRNA在特定类型的癌症中表达,它们可能影响肿瘤的进展。研究表明,lncRNA已经进化为有助于调节复杂的生物学过程,这些过程需要能够严格区分大量潜在效应子。如果我们的假设是正确的,那么我们将可以基于特定癌症中的lncRNA图谱预测突变蛋白的靶途径。更一般而言,这将扩大我们对信号转导网络如何在给定生物学环境中进行连接的理解。

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