Literature DB >> 16155006

HuR stabilizes vacuolar H+-translocating ATPase mRNA during cellular energy depletion.

Selvi Jeyaraj1, Duaa Dakhlallah, Stephanie R Hill, Beth S Lee.   

Abstract

V-ATPases are multisubunit membrane proteins that use ATP binding and hydrolysis to transport protons across membranes against a concentration gradient. Although some cell types express plasma membrane forms of these transporters, all eukaryotes require V-ATPases to maintain an acidic pH in membrane-bound compartments of endocytic and secretory networks to facilitate protein trafficking and processing. Mammalian cells that completely lack V-ATPases are not viable; yet, the abundance of V-ATPases can differ among cell types by an order of magnitude or more, requiring precise control of their expression. We previously showed that mRNA stability appears to play a major role in regulating overall abundance of V-ATPases. In this report, we demonstrate that the stability of V-ATPase mRNA is regulated through AU-rich elements in 3'-untranslated regions. Unlike some mRNAs that are short-lived due to the presence of these elements, V-ATPase mRNAs have half-lives of hours to days. However, during stress induced by ATP depletion, AU-rich elements are necessary to maintain stability of these transcripts and their presence in the cytoplasm. HuR, an RNA-binding protein that interacts with and stabilizes AU-rich mRNAs, shows increased binding to some V-ATPase mRNAs during ATP depletion. siRNA-mediated knockdown of HuR results in diminished V-ATPase expression. These results indicate that AU-rich elements and associated proteins can play a role in regulation of even very stable mRNAs by protecting against loss during cellular stress.

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Year:  2005        PMID: 16155006      PMCID: PMC1351387          DOI: 10.1074/jbc.M502883200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  65 in total

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4.  Interaction between aldolase and vacuolar H+-ATPase: evidence for direct coupling of glycolysis to the ATP-hydrolyzing proton pump.

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Journal:  Oncogene       Date:  2005-01-13       Impact factor: 9.867

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  17 in total

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7.  Krüppel -like factor 8 is a stress-responsive transcription factor that regulates expression of HuR.

Authors:  Suman Govindaraju; Beth S Lee
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8.  Transcriptional control of human antigen R by bone morphogenetic protein.

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10.  Expression of the RNA-stabilizing protein HuR in ischemia-reperfusion injury of rat kidney.

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