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Amino acid metabolites that regulate G protein signaling during osmotic stress
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نویسنده
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shellhammer j.p. ,morin-kensicki e. ,matson j.p. ,yin g. ,isom d.g. ,campbell s.l. ,mohney r.p. ,dohlman h.g.
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منبع
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plos genetics - 2017 - دوره : 13 - شماره : 5
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چکیده
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All cells respond to osmotic stress by implementing molecular signaling events to protect the organism. failure to properly adapt can lead to pathologies such as hypertension and ischemia-reperfusion injury. mitogen-activated protein kinases (mapks) are activated in response to osmotic stress,as well as by signals acting through g protein-coupled receptors (gpcrs). for proper adaptation,the action of these kinases must be coordinated. to identify second messengers of stress adaptation,we conducted a mass spectrometry-based global metabolomics profiling analysis,quantifying nearly 300 metabolites in the yeast s. cerevisiae. we show that three branched-chain amino acid (bcaa) metabolites increase in response to osmotic stress and require the mapk hog1. ectopic addition of these bcaa derivatives promotes phosphorylation of the g protein α subunit and dampens g protein-dependent transcription,similar to that seen in response to osmotic stress. conversely,genetic ablation of hog1 activity or the bcaa-regulatory enzymes leads to diminished phosphorylation of gα and increased transcription. taken together,our results define a new class of candidate second messengers that mediate cross talk between osmotic stress and gpcr signaling pathways. © 2017 shellhammer et al.
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آدرس
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department of pharmacology,university of north carolina at chapel hill,chapel hill,nc, United States, metabolon,inc,research triangle park,nc,united states,attain,llc,morrisville,nc, United States, department of biochemistry and biophysics,university of north carolina at chapel hill,chapel hill,nc, United States, department of biochemistry and biophysics,university of north carolina at chapel hill,chapel hill,nc, United States, the university of miami miller school of medicine,miami,fl, United States, department of biochemistry and biophysics,university of north carolina at chapel hill,chapel hill,nc, United States, metabolon,inc,research triangle park,nc, United States, department of pharmacology,university of north carolina at chapel hill,chapel hill,nc,united states,department of biochemistry and biophysics,university of north carolina at chapel hill,chapel hill,nc, United States
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Authors
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