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Stimulation of -1 programmed ribosomal frameshifting by a metabolite-responsive RNA pseudoknot.

机译:代谢物反应性RNA假结刺激-1程序化的核糖体移码。

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Specific recognition of metabolites by functional RNA motifs within mRNAs has emerged as a crucial regulatory strategy for feedback control of biochemical reactions. Such riboswitches have been demonstrated to regulate different gene expression processes, including transcriptional termination and translational initiation in prokaryotic cells, as well as splicing in eukaryotic cells. The regulatory process is usually mediated by modulating the accessibility of specific sequence information of the expression platforms via metabolite-induced RNA conformational rearrangement. In eukaryotic systems, viral and the more limited number of cellular decoding -1 programmed ribosomal frameshifting (PRF) are commonly promoted by a 3' mRNA pseudoknot. In addition, such -1 PRF is generally constitutive rather than being regulatory, and usually results in a fixed ratio of products. We report here an RNA pseudoknot capable of stimulating -1 PRF whose efficiency can be tuned in response to the concentration of S-adenosylhomocysteine (SAH), and the improvement of its frameshifting efficiency by RNA engineering. In addition to providing an alternative approach for small-molecule regulation of gene expression in eukaryotic cells, such a metabolite-responsive pseudoknot suggests a plausible mechanism for metabolite-driven translational regulation of gene expression in eukaryotic systems.
机译:通过mRNA中功能性RNA基序对代谢物的特异性识别已成为生化反应反馈控制的关键调控策略。已经证明这种核糖开关调节不同的基因表达过程,包括原核细胞中的转录终止和翻译起始以及真核细胞中的剪接。调节过程通常通过经由代谢物诱导的RNA构象重排调节表达平台的特定序列信息的可及性来介导。在真核系统中,病毒和数量有限的细胞解码-1程序化核糖体移码(PRF)通常由3'mRNA假结促进。此外,这种-1 PRF通常是组成性的,而不是可调节的,通常会导致固定比例的产品。我们在这里报告了一种能够刺激-1 PRF的RNA假结,其效率可以根据S-腺苷同型半胱氨酸(SAH)的浓度进行调节,并通过RNA工程提高其移码效率。除了提供用于在真核细胞中小分子调节基因表达的替代方法之外,这种代谢物响应性假结还提出了由代谢物驱动的真核系统中基因表达的翻译调节的合理机制。

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