Regulation of Peroxisome Homeostasis by Post-Translational Modification in the Methylotrophic Yeast .

Front Cell Dev Biol

Division of Applied Life Sciences, Graduate School of Agriculture, Kyoto University, Kyoto, Japan.

Published: April 2022

AI Article Synopsis

  • Methylotrophic yeast can utilize methanol for growth, stimulating peroxisome proliferation and activating a series of transcription factors that induce methanol-metabolizing enzymes.
  • The presence of ethanol represses this methanol-induced gene expression through the action of acetyl-CoA, which inactivates key transcription factor Mxr1 by phosphorylation.
  • Pexophagy, the degradation of peroxisomes when methanol is depleted, is regulated by phosphorylation events, where methanol signals inhibit pexophagy while its absence activates it.

Article Abstract

The methylotrophic yeast can grow on methanol with an associated proliferation of peroxisomes, which are subsequently degraded by pexophagy upon depletion of methanol. Two cell wall integrity and stress response component (WSC) family proteins (Wsc1 and Wsc3) sense the extracellular methanol concentration and transmit the methanol signal to Rom2. This stimulates the activation of transcription factors (Mxr1, Trm1, and Mit1 etc.), leading to the induction of methanol-metabolizing enzymes (methanol-induced gene expression) and synthesis of huge peroxisomes. Methanol-induced gene expression is repressed by the addition of ethanol (ethanol repression). This repression is not conducted directly by ethanol but rather by acetyl-CoA synthesized from ethanol by sequential reactions, including alcohol and aldehyde dehydrogenases, and acetyl-CoA synthetase. During ethanol repression, Mxr1 is inactivated by phosphorylation. Peroxisomes are degraded by pexophagy on depletion of methanol and this event is triggered by phosphorylation of Atg30 located at the peroxisome membrane. In the presence of methanol, Wsc1 and Wsc3 repress pexophagy by transmitting the methanol signal the MAPK cascade to the transcription factor Rlm1, which induces phosphatases involved in dephosphorylation of Atg30. Upon methanol consumption, repression of Atg30 phosphorylation is released, resulting in initiation of pexophagy. Physiological significance of these machineries involved in peroxisome homeostasis and their post-translational modification is also discussed in association with the lifestyle of methylotrophic yeast in the phyllosphere.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9061947PMC
http://dx.doi.org/10.3389/fcell.2022.887806DOI Listing

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