Literature DB >> 22836135

The ribosome profiling strategy for monitoring translation in vivo by deep sequencing of ribosome-protected mRNA fragments.

Nicholas T Ingolia1, Gloria A Brar, Silvia Rouskin, Anna M McGeachy, Jonathan S Weissman.   

Abstract

Recent studies highlight the importance of translational control in determining protein abundance, underscoring the value of measuring gene expression at the level of translation. We present a protocol for genome-wide, quantitative analysis of in vivo translation by deep sequencing. This ribosome profiling approach maps the exact positions of ribosomes on transcripts by nuclease footprinting. The nuclease-protected mRNA fragments are converted into a DNA library suitable for deep sequencing using a strategy that minimizes bias. The abundance of different footprint fragments in deep sequencing data reports on the amount of translation of a gene. In addition, footprints reveal the exact regions of the transcriptome that are translated. To better define translated reading frames, we describe an adaptation that reveals the sites of translation initiation by pretreating cells with harringtonine to immobilize initiating ribosomes. The protocol we describe requires 5-7 days to generate a completed ribosome profiling sequencing library. Sequencing and data analysis require a further 4-5 days.

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Year:  2012        PMID: 22836135      PMCID: PMC3535016          DOI: 10.1038/nprot.2012.086

Source DB:  PubMed          Journal:  Nat Protoc        ISSN: 1750-2799            Impact factor:   13.491


  49 in total

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Review 2.  Computational methods for transcriptome annotation and quantification using RNA-seq.

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Review 9.  Differentiating protein-coding and noncoding RNA: challenges and ambiguities.

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Authors:  David J Young; Nicholas R Guydosh; Fan Zhang; Alan G Hinnebusch; Rachel Green
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3.  Ras Suppresses TXNIP Expression by Restricting Ribosome Translocation.

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Journal:  Cell       Date:  2014-02-27       Impact factor: 41.582

5.  Spliceosome Profiling Visualizes Operations of a Dynamic RNP at Nucleotide Resolution.

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6.  A bicistronic MAVS transcript highlights a class of truncated variants in antiviral immunity.

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Review 7.  RNA-binding proteins in neurodegeneration: Seq and you shall receive.

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Review 8.  The Growing Toolbox for Protein Synthesis Studies.

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9.  Native elongating transcript sequencing reveals human transcriptional activity at nucleotide resolution.

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10.  RIPiT-Seq: a high-throughput approach for footprinting RNA:protein complexes.

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