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100248 |
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|a Endres, Lauren
|e author
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|a Massachusetts Institute of Technology. Center for Environmental Health Sciences
|e contributor
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|a Massachusetts Institute of Technology. Department of Biological Engineering
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|a Dedon, Peter C.
|e contributor
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|a Dedon, Peter C.
|e contributor
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|a Dedon, Peter C.
|e author
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|a Begley, Thomas J.
|e author
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|a Codon-biased translation can be regulated by wobble-base tRNA modification systems during cellular stress responses
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|b Landes Bioscience,
|c 2015-12-14T22:06:16Z.
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|z Get fulltext
|u http://hdl.handle.net/1721.1/100248
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|a tRNA (tRNA) is a key molecule used for protein synthesis, with multiple points of stress-induced regulation that can include transcription, transcript processing, localization and ribonucleoside base modification. Enzyme-catalyzed modification of tRNA occurs at a number of base and sugar positions and has the potential to influence specific anticodon-codon interactions and regulate translation. Notably, altered tRNA modification has been linked to mitochondrial diseases and cancer progression. In this review, specific to Eukaryotic systems, we discuss how recent systems-level analyses using a bioanalytical platform have revealed that there is extensive reprogramming of tRNA modifications in response to cellular stress and during cell cycle progression. Combined with genome-wide codon bias analytics and gene expression studies, a model emerges in which stress-induced reprogramming of tRNA drives the translational regulation of critical response proteins whose transcripts display a distinct codon bias. Termed Modification Tunable Transcripts (MoTTs), we define them as (1) transcripts that use specific degenerate codons and codon biases to encode critical stress response proteins, and (2) transcripts whose translation is influenced by changes in wobble base tRNA modification. In this review we note that the MoTTs translational model is also applicable to the process of stop-codon recoding for selenocysteine incorporation, as stop-codon recoding involves a selective codon bias and modified tRNA to decode selenocysteine during the translation of a key subset of oxidative stress response proteins. Further, we discuss how in addition to RNA modification analytics, the comprehensive characterization of translational regulation of specific transcripts requires a variety of tools, including high coverage codon-reporters, ribosome profiling and linked genomic and proteomic approaches. Together these tools will yield important new insights into the role of translational elongation in cell stress response.
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|a National Science Foundation (U.S.) (CHE-1308839)
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|a Singapore. National Research Foundation (Singapore-MIT Alliance for Research and Technology Center. Infectious Disease Research Program)
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|a en_US
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|a Article
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|t RNA Biology
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