Literature DB >> 25132067

RNA structural analysis by evolving SHAPE chemistry.

Robert C Spitale1, Ryan A Flynn, Eduardo A Torre, Eric T Kool, Howard Y Chang.   

Abstract

RNA is central to the flow of biological information. From transcription to splicing, RNA localization, translation, and decay, RNA is intimately involved in regulating every step of the gene expression program, and is thus essential for health and understanding disease. RNA has the unique ability to base-pair with itself and other nucleic acids to form complex structures. Hence the information content in RNA is not simply its linear sequence of bases, but is also encoded in complex folding of RNA molecules. A general chemical functionality that all RNAs have is a 2'-hydroxyl group in the ribose ring, and the reactivity of the 2'-hydroxyl in RNA is gated by local nucleotide flexibility. In other words, the 2'-hydroxyl is reactive at single-stranded and conformationally flexible positions but is unreactive at nucleotides constrained by base-pairing. Recent efforts have been focused on developing reagents that modify RNA as a function of RNA 2' hydroxyl group reactivity. Such RNA structure probing techniques can be read out by primer extension in experiments termed RNA SHAPE (selective 2'- hydroxyl acylation and primer extension). Herein, we describe the efforts devoted to the design and utilization of SHAPE probes for characterizing RNA structure. We also describe current technological advances that are being applied to utilize SHAPE chemistry with deep sequencing to probe many RNAs in parallel. The merging of chemistry with genomics is sure to open the door to genome-wide exploration of RNA structure and function.
© 2014 John Wiley & Sons, Ltd.

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Year:  2014        PMID: 25132067      PMCID: PMC5592018          DOI: 10.1002/wrna.1253

Source DB:  PubMed          Journal:  Wiley Interdiscip Rev RNA        ISSN: 1757-7004            Impact factor:   9.957


  64 in total

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  26 in total

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5.  Simple alkanoyl acylating agents for reversible RNA functionalization and control.

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6.  Metrics for rapid quality control in RNA structure probing experiments.

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7.  Studying RNA Homology and Conservation with Infernal: From Single Sequences to RNA Families.

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Review 8.  Using Genome Sequence to Enable the Design of Medicines and Chemical Probes.

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