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Multiple phosphorylation sites regulate the activity of the repressor Mig1 in Candida albicans .

Bernardo Ramírez-ZavalaDarina BetsovaSonja SchwanfelderInes KrügerAustin MottolaThomas KruegerOlaf KniemeyerAxel A BrakhageJoachim Morschhäuser
Published in: mSphere (2023)
. However, so far, it has remained elusive how SNF1 controls the activity of one of its main effectors, the repressor protein Mig1 that inhibits the expression of genes required for the utilization of alternative carbon sources when glucose is available. In this study, we have identified multiple phosphorylation sites in Mig1 that contribute to its inactivation. Mutation of these sites strongly increased Mig1 repressor activity in the absence of SNF1, but SNF1 could still sufficiently inhibit the hyperactive Mig1 to enable growth on alternative carbon sources. These findings reveal features of Mig1 that are important for controlling its repressor activity. Furthermore, they demonstrate that both SNF1 and additional protein kinases regulate Mig1 in this pathogenic yeast.
Keyphrases
  • candida albicans
  • genome wide
  • metabolic syndrome
  • biofilm formation
  • gene expression
  • amino acid
  • escherichia coli
  • staphylococcus aureus
  • protein kinase
  • long non coding rna
  • small molecule