Literature DB >> 23045643

Genome-wide ribosome profiling reveals complex translational regulation in response to oxidative stress.

Maxim V Gerashchenko1, Alexei V Lobanov, Vadim N Gladyshev.   

Abstract

Information on unique and coordinated regulation of transcription and translation in response to stress is central to the understanding of cellular homeostasis. Here we used ribosome profiling coupled with next-generation sequencing to examine the interplay between transcription and translation under conditions of hydrogen peroxide treatment in Saccharomyces cerevisiae. Hydrogen peroxide treatment led to a massive and rapid increase in ribosome occupancy of short upstream ORFs, including those with non-AUG translational starts, and of the N-terminal regions of ORFs that preceded the transcriptional response. In addition, this treatment induced the synthesis of N-terminally extended proteins and elevated stop codon read-through and frameshift events. It also increased ribosome occupancy at the beginning of ORFs and potentially the duration of the elongation step. We identified proteins whose synthesis was regulated rapidly by hydrogen peroxide posttranscriptionally; however, for the majority of genes increased protein synthesis followed transcriptional regulation. These data define the landscape of genome-wide regulation of translation in response to hydrogen peroxide and suggest that potentiation (coregulation of the transcript level and translation) is a feature of oxidative stress.

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Year:  2012        PMID: 23045643      PMCID: PMC3491468          DOI: 10.1073/pnas.1120799109

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  33 in total

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  143 in total

Review 1.  Hydroxylation and translational adaptation to stress: some answers lie beyond the STOP codon.

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8.  Site-Specific K63 Ubiquitinomics Provides Insights into Translation Regulation under Stress.

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9.  Widespread Accumulation of Ribosome-Associated Isolated 3' UTRs in Neuronal Cell Populations of the Aging Brain.

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