Literature summary for 1.13.11.20 extracted from

Kasperova, A.; Kunert, J.; Raska, M.
The possible role of dermatophyte cysteine dioxygenase in keratin degradation (2013), Med. Mycol., 51, 449-454.

Search for more literature for 1.13.11.20

Natural Substrates/ Products (Substrates)

Natural Substrates	Organism	Comment (Nat. Sub.)	Natural Products	Comment (Nat. Pro.)	Rev.	Reac.
L-cysteine + O2	Mammalia	-	3-sulfinoalanine	-	?
L-cysteine + O2	Bacillus sp. (in: Bacteria)	-	3-sulfinoalanine	-	?
L-cysteine + O2	Candida albicans	-	3-sulfinoalanine	-	?
L-cysteine + O2	Streptomyces sp.	-	3-sulfinoalanine	-	?
L-cysteine + O2	Trichophyton rubrum	-	3-sulfinoalanine	-	?
L-cysteine + O2	Histoplasma capsulatum	-	3-sulfinoalanine	-	?
L-cysteine + O2	Trichophyton mentagrophytes	-	3-sulfinoalanine	-	?

Organism

Organism	UniProt	Comment	Textmining
Bacillus sp. (in: Bacteria)	-	-	-
Candida albicans	-	-	-
Histoplasma capsulatum	-	-	-
Mammalia	-	-	-
Streptomyces sp.	-	-	-
Trichophyton mentagrophytes	-	-	-
Trichophyton rubrum	-	-	-

Source Tissue

Source Tissue	Comment	Organism	Textmining
keratinocyte	-	Mammalia	-
additional information	in Bacillus and Streptomyces spp. CDO is expressed in the vegetative state, and an increase in its activity is detected after the initiation of conidia production	Bacillus sp. (in: Bacteria)	-
mycelium	in Streptomyces spp. CDO is expressed in the vegetative state, and an increase in its activity is detected after the initiation of conidia production	Streptomyces sp.	-
skin	-	Mammalia	-

Substrates and Products (Substrate)

Substrates	Comment Substrates	Organism	Products	Comment (Products)	Rev.	Reac.
L-cysteine + O2	-	Mammalia	3-sulfinoalanine	-	?
L-cysteine + O2	-	Bacillus sp. (in: Bacteria)	3-sulfinoalanine	-	?
L-cysteine + O2	-	Candida albicans	3-sulfinoalanine	-	?
L-cysteine + O2	-	Streptomyces sp.	3-sulfinoalanine	-	?
L-cysteine + O2	-	Trichophyton rubrum	3-sulfinoalanine	-	?
L-cysteine + O2	-	Histoplasma capsulatum	3-sulfinoalanine	-	?
L-cysteine + O2	-	Trichophyton mentagrophytes	3-sulfinoalanine	-	?

Synonyms

Synonyms	Comment	Organism
CDO	-	Mammalia
CDO	-	Bacillus sp. (in: Bacteria)
CDO	-	Candida albicans
CDO	-	Streptomyces sp.
CDO	-	Trichophyton rubrum
CDO	-	Histoplasma capsulatum
CDO	-	Trichophyton mentagrophytes

General Information

General Information	Comment	Organism
metabolism	in mammals, excess cysteine is generally degraded by oxygenation to 3-sulfino-L-alanine. The majority of cysteine sulphinic acid is then deaminated to sulphinylpyruvate, which decomposes spontaneously byreleasing inorganic sulphite. The latter compound is then further oxidized to sulphate, which is excreted for the most part from the cell. In parallel, a variable proportion of cysteine sulphinic acid is decarboxylated to hypotaurine, then further oxidized to taurine. Although cysteine can be catabolized by some non-oxidative pathways, they are of minor importance. CDO activity is regulated by concentration of cysteine, and in mammals, both have been demonstrated to be important vital factors	Mammalia
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels, supplementation of growth medium with L-cystine induces a persistent increase in the CDO mRNA transcript level, whereas the concentration of intracellular CDO protein changes over time. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Trichophyton mentagrophytes
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Mammalia
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Bacillus sp. (in: Bacteria)
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Candida albicans
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Streptomyces sp.
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Trichophyton rubrum
additional information	intracellular CDO concentration is regulated at both transcriptional and posttranslational levels. Mechanism of cysteine oxygenation from iron(II)-superoxo complex, via cis- and trans-sulfoxide structure formation, to iron(IV)-oxo complex and the final product cysteine sulphinic acid	Histoplasma capsulatum
physiological function	CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion	Bacillus sp. (in: Bacteria)
physiological function	CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion	Streptomyces sp.
physiological function	CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion. In dermatophytes, CDO is a virulence factor crucial for keratin degradation, role of cysteine dioxygenase in the degradation of keratinized tissues by dermatophytes, overview	Trichophyton rubrum
physiological function	CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion. In dermatophytes, CDO is a virulence factor crucial for keratin degradation, role of cysteine dioxygenase in the degradation of keratinized tissues by dermatophytes, overview	Trichophyton mentagrophytes
physiological function	CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion. In dermatophytes, CDO is a virulence factor crucial for keratin degradation, role of cysteine dioxygenase in the degradation of keratinized tissues by dermatophytes, overview. In Candida albicans upregulated expression of CDO is detected in the switch from white to opaque phenotypes [18]. In the latter, a reversible transition has been described between smooth white, dome-shaped yeast colonies (white) to circular or irregular-shaped colonies, composed of a mixture of yeast and fi lamentous cells (opaque)	Candida albicans
physiological function	cysteine dioxygenase is a key enzyme involved in the homeostatic regulation of cysteine level and in production of important oxidized metabolites of cysteine such as pyruvate, sulphite, sulphate, hypotaurine, and taurine in all eukaryotic cells, CDO is crucial for oxidation of cysteine to cysteine sulphinic acid and therefore for sulphite production and secretion	Mammalia
physiological function	in Histoplasma capsulatum, the enzyme is a key factor in the transition from the mycelial to yeast phase. CDO is crucial for oxidation of cysteine to cysteine sulfinic acid and therefore for sulfite production and secretion	Histoplasma capsulatum

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Release 2023.1 (January 2023)