Methylglyoxal-Scavenging Enzyme Activities Trigger Erythroascorbate Peroxidase and Cytochrome c Peroxidase in Glutathione-Depleted Candida albicans
γ-Glutamylcysteine synthetase (Gcs1) and glutathione reductase (Glr1) activity maintains minimal levels of cellular methylglyoxal in . In glutathione-depleted , we previously saw that NAD(H)-linked methylglyoxal oxidoreductase (Mgd1) and alcohol dehydrogenase (Adh1) are the most active methylglyoxal...
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Veröffentlicht in: | Journal of microbiology and biotechnology 2021, 31(1), , pp.79-91 |
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Sprache: | eng |
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Zusammenfassung: | γ-Glutamylcysteine synthetase (Gcs1) and glutathione reductase (Glr1) activity maintains minimal levels of cellular methylglyoxal in
. In glutathione-depleted
, we previously saw that NAD(H)-linked methylglyoxal oxidoreductase (Mgd1) and alcohol dehydrogenase (Adh1) are the most active methylglyoxal scavengers. With methylglyoxal accumulation, disruptants lacking
or
exhibit a poor redox state. However, there is little convincing evidence for a reciprocal relationship between methylglyoxal scavenger genes-disrupted mutants and changes in glutathione-(in)dependent redox regulation. Herein, we attempt to demonstrate a functional role for methylglyoxal scavengers, modeled on a triple disruptant (
/
/
), to link between antioxidative enzyme activities and their metabolites in glutathione-depleted conditions. Despite seeing elevated methylglyoxal in all of the disruptants, the result saw a decrease in pyruvate content in
/
/
which was not observed in double gene-disrupted strains such as
/
and
/
. Interestingly,
/
/
exhibited a significantly decrease in H
O
and superoxide which was also unobserved in
/
and
/
. The activities of the antioxidative enzymes erythroascorbate peroxidase and cytochrome c peroxidase were noticeably higher in
/
/
than in the other disruptants. Meanwhile, Glr1 activity severely diminished in
/
/
. Monitoring complementary gene transcripts between double gene-disrupted
/
and
/
supported the concept of an unbalanced redox state independent of the Glr1 activity for
/
/
. Our data demonstrate the reciprocal use of Eapx1 and Ccp1 in the absence of both methylglyoxal scavengers; that being pivotal for viability in non-filamentous budding yeast. |
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ISSN: | 1017-7825 1738-8872 |
DOI: | 10.4014/JMB.2010.10057 |