AI Article Synopsis

  • Glucose starvation is a significant stress that affects cell survival and triggers changes in the transcription of mRNA and noncoding RNA (ncRNA).
  • Researchers found that glucose deficiency leads to increased transcription of long ncRNA (lncRNA) related to the gluconeogenesis gene (fbp1+), which modifies chromatin structure and promotes gene activation.
  • The study utilized RNA sequencing and ChIP-seq to identify different early, middle, and late responses to glucose starvation, revealing that the transcription changes are mainly driven by the transcription factor Atf1, suggesting a coordinated response involving both mRNA and lncRNA in cellular adaptation.

Article Abstract

Shortage of glucose, the primary energy source for all organisms, is one of the most critical stresses influencing cell viability. Glucose starvation promptly induces changes in mRNA and noncoding RNA (ncRNA) transcription. We previously reported that glucose starvation induces long ncRNA (lncRNA) transcription in the 5' segment of a fission yeast gluconeogenesis gene (fbp1+), which leads to stepwise chromatin alteration around the fbp1+ promoter and to subsequent robust gene activation. Here, we analyzed genomewide transcription by strand-specific RNA sequencing, together with chromatin landscape by immunoprecipitation sequencing (ChIP-seq). Clustering analysis showed that distinct mRNAs and ncRNAs are induced at the early, middle and later stages of cellular response to glucose starvation. The starvation-induced transcription depends substantially on the stress-responsive transcription factor Atf1. Using a new computer program that examines dynamic changes in expression patterns, we identified ncRNAs with similar behavior to the fbp1+ lncRNA. We confirmed that there are continuous lncRNAs associated with local reduction of histone density. Overlapping with the regions for transcription of these lncRNAs, antisense RNAs are antagonistically transcribed under glucose-rich conditions. These results suggest that Atf1-dependent integrated networks of mRNA and lncRNA govern drastic changes in cell physiology in response to glucose starvation.

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Source
http://dx.doi.org/10.1111/gtc.12229DOI Listing

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