SMPDB

Pathway Description

Pyruvaldehyde Degradation

Homo sapiens

Metabolic Pathway

Created: 2013-08-01

Last Updated: 2025-01-23

This Pyruvaldehyde degradation pathway (Methylglyoxal degradation;2-oxopropanal degradation), also known as the glyoxalase system, is probably the most common pathway for the degradation of pyruvaldehyde (methylglyoxal), a potentially toxic metabolite due to its interaction with nucleic acids and other proteins. Pyruvaldehyde is formed in low concentrations by glycolysis, fatty acid metabolism and protein metabolism. Pyruvaldehyde is catalyzed by the glyoxylase system, composed of the enzymes lactoylglutathione lyase (glyoxalase I) and glyoxylase II. Glyoxalase I catalyes the isomerization of the spontaneously formed hemithioacetal adduct between glutathione and pyruvaldehyde into S-lactoylglutathione. S-lactoylglutathione is then catalyzed by glyoxalase II into D-lactic acid and glutathione. D-lactic acid is then catalyzed by an unknown quinol in the membrane to pyruvic acid, which then enters pyruvate metabolism.

References

Pyruvaldehyde Degradation References

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Pubmed: 7684374

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Pubmed: 8449929

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Pubmed: 8670058

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Pubmed: 12127981

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	D-Lactic acid
	FAD
	Glutathione
	Hydrogen Ion
	Pyruvaldehyde
	Pyruvic acid
	S-Lactoylglutathione
	Water
	Zinc (II) ion

		D-Lactic acid
		FAD
		Glutathione
		Hydrogen Ion
		Pyruvaldehyde
		Pyruvic acid
		S-Lactoylglutathione
		Water
		Zinc (II) ion

	Hydroxyacylglutathione hydrolase, mitochondrial
	Lactoylglutathione lyase
	Probable D-lactate dehydrogenase, mitochondrial

		Hydroxyacylglutathione hydrolase, mitochondrial
		Lactoylglutathione lyase
		Probable D-lactate dehydrogenase, mitochondrial

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Pyruvaldehyde Degradation

Pyruvaldehyde Degradation References