Bimodal expression of PHO84 is modulated by early termination of antisense transcription

Castelnuovo, Manuele; Rahman, Shadab A.; Guffanti, Elisa; Infantino, Valentina; Stutz, Françoise; Zenklusen, Daniel

doi:10.1038/nsmb.2598

Cited by 124 publications

(153 citation statements)

References 55 publications

(86 reference statements)

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“…If this were the case, the HXT lncRNAs may function similarly to PHO84 lncRNA that functions as a "bimodal" switch to promote different cell fates within a genetically identical population (Castelnuovo et al 2013). A third possibility is that the antisense HXT transcripts function in the cytoplasm, controlling translational efficiency to stability of the corresponding sense mRNA (Carrieri et al 2012;Pelechano and Steinmetz 2013;Wang et al 2013).…”

Section: Discussionmentioning

confidence: 99%

Regulation of Glucose-Dependent Gene Expression by the RNA Helicase Dbp2 in Saccharomyces cerevisiae

et al. 2014

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Cellular homeostasis requires a fine balance between energy uptake, utilization, and growth. Dbp2 is a member of the DEAD-box protein family in Saccharomyces cerevisiae with characterized ATPase and helicase activity in vitro. DEAD-box RNA helicases are a class of enzymes that utilize ATP hydrolysis to remodel RNA and/or RNA-protein (RNP) composition. Dbp2 has been proposed to utilize its helicase activity in vivo to promote RNA-protein complex assembly of both messenger (m)RNAs and long noncoding (lnc)RNAs. Previous work from our laboratory demonstrated that loss of DBP2 enhances the lncRNA-dependent transcriptional induction of the GAL genes by abolishing glucose-dependent repression. Herein, we report that either a carbon source switch or glucose deprivation results in rapid export of Dbp2 to the cytoplasm. Genome-wide RNA sequencing identified a new class of antisense hexose transporter transcripts that are specifically upregulated upon loss of DBP2. Further investigation revealed that both sense and antisense hexose transporter (HXT) transcripts are aberrantly expressed in DBP2-deficient cells and that this expression pathway can be partially mimicked in wild-type cells by glucose depletion. We also find that Dbp2 promotes ribosome biogenesis and represses alternative ATP-producing pathways, as loss of DBP2 alters the transcript levels of ribosome biosynthesis (snoRNAs and associated proteins) and respiration gene products. This suggests that Dbp2 is a key integrator of nutritional status and gene expression programs required for energy homeostasis.

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Section: Discussionmentioning

confidence: 99%

Regulation of Glucose-Dependent Gene Expression by the RNA Helicase Dbp2 in Saccharomyces cerevisiae

et al. 2014

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“…Finally, as more efforts are put forth to decipher the role of the non-coding genome, it must be emphasized that some of these long non-coding RNAs have been detected with translating ribosomes. 88 Although no examples of lncRNAs that produce functional peptides have been documented to date, we should continue to view the term 29 Promotes induction MMF1 Mitochondrial protein YES ASP3 lncRNA 98 Upregulation ASP3 Asparagine catabolism YES PHO84 AS RNA [99][100][101] Repression PHO84 Phosphate metabolism YES SRG1 28,50,51 Repression SER3 Serine / glycine biogenesis YES PHO5 AS RNA 102 Promotes induction PHO5 Phosphate metabolism YES usURA2. 103 Repression URA2 Pyrimidine biogenesis YES usDCI1.…”

mentioning

confidence: 99%

LncRNAs: Bridging environmental sensing and gene expression

2016

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The survival of all organisms is dependent on complex, coordinated responses to environmental cues. Non-coding RNAs have been identified as major players in regulation of gene expression, with recent evidence supporting roles for long non-coding (lnc)RNAs in both transcriptional and post-transcriptional control. Evidence from our laboratory shows that lncRNAs have the ability to form hybridized structures called R-loops with specific DNA target sequences in S. cerevisiae, thereby modulating gene expression. In this Point of View, we provide an overview of the nature of lncRNA-mediated control of gene expression in the context of our studies using the GAL gene cluster as a model for controlling the timing of transcription.

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“…10,11 It is perhaps also due to the pleasing notion that an antisense-transcribing polymerase complex might collide with and disrupt either the sense-transcribing polymerase, or else the pre-initiation complex on the sense promoter. However, Hongay et al 12 found that antisense transcription did not occur at the same time as sense transcription within the same cells, while Castelnuovo et al 13 and Nguyen et al…”

Section: Antisense Transcription Is Not a Universal Repressor Of Sensmentioning

confidence: 99%

Using both strands: The fundamental nature of antisense transcription

Murray¹,

Mellor

2016

BioArchitecture

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ABSTRACT. Non-coding transcription across the antisense strands of genes is an abundant, pervasive process in eukaryotes from yeast to humans, however its biological function remains elusive. Here, we provide commentary on a recent study of ours, which demonstrates a genome-wide role for antisense transcription: establishing a unique, dynamic chromatin architecture over genes. Antisense transcription increases the level of nucleosome occupancy and histone acetylation at the promoter and body of genes, without necessarily modulating the level of protein-coding sense transcription. It is also associated with high levels of histone turnover. By allowing genes to sample a wider range of chromatin configurations, antisense transcription could serve to make genes more sensitive to changing signals, priming them for responses to developmental programs or stressful cellular environments. Given the abundance of antisense transcription and the breadth of these chromatin changes, we propose that antisense transcription represents a fundamental, canonical feature of eukaryotic genes.

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Bimodal expression of PHO84 is modulated by early termination of antisense transcription

Cited by 124 publications

References 55 publications

Regulation of Glucose-Dependent Gene Expression by the RNA Helicase Dbp2 in Saccharomyces cerevisiae

Regulation of Glucose-Dependent Gene Expression by the RNA Helicase Dbp2 in Saccharomyces cerevisiae

LncRNAs: Bridging environmental sensing and gene expression

Using both strands: The fundamental nature of antisense transcription

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