WordNet

any of the enzymes that catalyze biological oxidation

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出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2015/06/30 16:11:20」(JST)

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Sulfite oxidase (EC 1.8.3.1) is an enzyme in the mitochondria of all eukaryotes.^{[citation needed]} It oxidizes sulfite to sulfate and, via cytochrome c, transfers the electrons produced to the electron transport chain, allowing generation of ATP in oxidative phosphorylation.^[1]^[2]^[3] This is the last step in the metabolism of sulfur-containing compounds and the sulfate is excreted.

Sulfite oxidase is a metallo-enzyme that utilizes a molybdopterin cofactor and a heme group. It is one of the cytochromes b₅ and belongs to the enzyme super-family of molybdenum oxotransferases that also includes DMSO reductase, xanthine oxidase, and nitrite reductase.

In mammals, the expression levels of sulfite oxidase is high in the liver, kidney, and heart, and very low in spleen, brain, skeletal muscle, and blood.

Structure

As a homodimer, sulfite oxidase contains two identical subunits with an N-terminal domain and a C-terminal domain. These two domains are connected by ten amino acids forming a loop. The N-terminal domain has a heme cofactor with three adjacent antiparallel beta sheets and five alpha helices. The C-terminal domain hosts a molybdopterin cofactor that is surrounded by thirteen beta sheets and three alpha helices. The molybdopterin cofactor has a Mo(VI) center, which is bonded to a sulfur from cysteine, an ene-dithiolate from pyranopterin, and two terminal oxygens. It is at this molybdenum center that the catalytic oxidation of sulfite takes place.

Active site and mechanism

A proposed mechanism of the oxidation of sulfite to sulfate by sulfite oxidase.

The active site of sulfite oxidase contains the molybdopterin cofactor and supports molybdenum in its highest oxidation state, +6 (Mo^VI). In the enzyme's oxidized state, molybdenum is coordinated by a cysteine thiolate, the dithiolene group of molybdopterin, and two terminal oxygen atoms (oxos). Upon reacting with sulfite, one oxygen atom is transferred to sulfite to produce sulfate, and the molybdenum center is reduced by two electrons to Mo^IV. Water then displaces sulfate, and the removal of two protons (H⁺) and two electrons (e⁻) returns the active site to its original state. A key feature of this oxygen atom transfer enzyme is that the oxygen atom being transferred arises from water, not from dioxygen (O₂).

Deficiency

Sulfite oxidase is required to metabolize the sulfur-containing amino acids cysteine and methionine in foods. Lack of functional sulfite oxidase causes a disease known as sulfite oxidase deficiency. This rare but fatal disease causes neurological disorders, mental retardation, physical deformities, the degradation of the brain, and death. Reasons for the lack of functional sulfite oxidase include a genetic defect that leads to the absence of a molybdopterin cofactor and point mutations in the enzyme.^[4] A G473D mutation impairs dimerization and catalysis in human sulfite oxidase.^[5]^[6]

References

^ D'Errico G, Di Salle A, La Cara F, Rossi M, Cannio R (January 2006). "Identification and characterization of a novel bacterial sulfite oxidase with no heme binding domain from Deinococcus radiodurans". J. Bacteriol. 188 (2): 694–701. doi:10.1128/JB.188.2.694-701.2006. PMC 1347283. PMID 16385059.
^ Tan WH, Eichler FS, Hoda S, Lee MS, Baris H, Hanley CA, Grant PE, Krishnamoorthy KS, Shih VE (September 2005). "Isolated sulfite oxidase deficiency: a case report with a novel mutation and review of the literature". Pediatrics 116 (3): 757–66. doi:10.1542/peds.2004-1897. PMID 16140720.
^ Cohen HJ, Betcher-Lange S, Kessler DL, Rajagopalan KV (December 1972). "Hepatic sulfite oxidase. Congruency in mitochondria of prosthetic groups and activity". J. Biol. Chem. 247 (23): 7759–66. PMID 4344230.
^ Karakas E, Kisker C (November 2005). "Structural analysis of missense mutations causing isolated sulfite oxidase deficiency". Dalton Transactions (21): 3459–63. doi:10.1039/b505789m. PMID 16234925.
^ Wilson HL, Wilkinson SR, Rajagopalan KV (February 2006). "The G473D mutation impairs dimerization and catalysis in human sulfite oxidase". Biochemistry 45 (7): 2149–60. doi:10.1021/bi051609l. PMID 16475804.
^ Feng C, Tollin G, Enemark JH (May 2007). "Sulfite oxidizing enzymes". Biochim. Biophys. Acta 1774 (5): 527–39. doi:10.1016/j.bbapap.2007.03.006. PMC 1993547. PMID 17459792.

External links

Sulfite oxidase at the US National Library of Medicine Medical Subject Headings (MeSH)
Research Activity of Sarkar Group

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5. 先天性代謝異常：個々の障害の発見 inborn errors of metabolism identifying the specific disorder

English Journal

Hydrogen sulfide in pharmacology and medicine - An update.

Bełtowski J1.
Pharmacological reports : PR.Pharmacol Rep.2015 Jun;67(3):647-658. doi: 10.1016/j.pharep.2015.01.005. Epub 2015 Jan 22.
Hydrogen sulfide (H2S) is the endogenously produced gasotransmitter involved in the regulation of nervous system, cardiovascular functions, inflammatory response, gastrointestinal system and renal function. Together with nitric oxide and carbon monoxide, H2S belongs to a family of gasotransmitters.
PMID 25933982

Low molybdenum state induced by tungsten as a model of molybdenum deficiency in rats.

Yoshida M1, Nakagawa M, Hosomi R, Nishiyama T, Fukunaga K.
Biological trace element research.Biol Trace Elem Res.2015 May;165(1):75-80. doi: 10.1007/s12011-015-0239-1. Epub 2015 Jan 28.
Organ molybdenum (Mo) concentration and the activity of hepatic sulfite oxidase and xanthine oxidase were compared in tungsten-administered rats as well as rats fed with a low Mo diet to evaluate the use of tungsten-administered rats as a model of Mo deficiency. Twenty-four male 6-week-old Wistar ra
PMID 25627419

In vitro evidence that sulfite impairs glutamatergic neurotransmission and inhibits glutathione metabolism-related enzymes in rat cerebral cortex.

Parmeggiani B1, Moura AP1, Grings M1, Bumbel AP1, de Moura Alvorcem L1, Tauana Pletsch J1, Fernandes CG1, Wyse ATs1, Wajner M2, Leipnitz G3.
International journal of developmental neuroscience : the official journal of the International Society for Developmental Neuroscience.Int J Dev Neurosci.2015 May;42:68-75. doi: 10.1016/j.ijdevneu.2015.03.005. Epub 2015 Mar 13.
Sulfite oxidase (SOX) deficiency is an inherited neurometabolic disorder biochemically characterized by tissue accumulation and high urinary excretion of sulfite and thiosulfate. Affected patients present severe neurological dysfunction accompanied by seizures, whose pathophysiology is poorly known.
PMID 25777939

Japanese Journal

Sulfite Oxidation Catalyzed by aa_3-Type Cytochrome c Oxidase in Acidithiobacillus ferrooxidans

SUGIO Tsuyoshi,AKO Ami,TAKEUCHI Fumiaki
Bioscience, biotechnology, and biochemistry 74(11), 2242-2247, 2010-11-23
… Sulfite is produced as a toxic intermediate during Acidithiobacillus ferrooxidans … D3-2, which posseses the highest copper bioleaching activity, is more resistant to sulfite than other A. … When sulfite oxidase was purified homogeneously from strain D3-2, the oxidized and reduced forms of the purified sulfite oxidase absorption spectra corresponded to those of A. …
NAID 10027561458

Functional deficiencies of sulfite oxidase : Differential diagnoses in neonates presenting with intractable seizures and cystic encephalomalacia

SASS Jorn Oliver,GUNDUZ Aysegul,FUNAYAMA Carolina Araujo Rodrigues,KORKMAZ Baris,PINTO Kylvia Giselle Dantas,TUYSUZ Beyhan,SANTOS Leticia Yanasse Dos,TASKIRAN Emine,DE FATIMA TURCATO Marlene,LAM Ching-Wan,REISS Jochen,WALTER Melanie,YALCINKAYA Cengiz,JUNIOR Jose Simon Camelo
Brain & development 32(7), 544-549, 2010-08-01
NAID 10027491957

Isolation and Characterization of Acidithiobacillus ferrooxidans Strain D3-2 Active in Copper Bioleaching from a Copper Mine in Chile

SUGIO Tsuyoshi,WAKABAYASHI Masanori,KANAO Tadayoshi,TAKEUCHI Fumiaki
Bioscience, biotechnology, and biochemistry 72(4), 998-1004, 2008-04-23
… The iron oxidase activities of D3-2, D3-6, and ATCC 23270 were 11.7, 13.2, and 27.9 μl O2 … In contrast, the sulfite oxidase activities of strains D3-2, D3-6, and ATCC 23270 were 5.8, 2.9, and 1.0 μl O2 … The sulfite oxidase of strain D3-2 was much more resistant to sulfite ion than that of strain ATCC 23270. …
NAID 10027526575

Related Pictures

★リンクテーブル★

リンク元	「亜硫酸酸化酵素」「sulfite dehydrogenase」「sulfite reductase」「亜硫酸オキシダーゼ」
関連記事	「sulfite」

「亜硫酸酸化酵素」

Sulfite oxidase
	PDB rendering based on 1mj4.
Available structures
PDB	Ortholog search: PDBe, RCSB
List of PDB id codes
	1MJ4
Identifiers
Symbol	SUOX
External IDs	OMIM: 606887 MGI: 2446117 HomoloGene: 394 GeneCards: SUOX Gene
EC number	1.8.3.1
Gene ontology
Molecular function	• sulfite oxidase activity; • electron carrier activity; • heme binding; • molybdenum ion binding; • molybdopterin cofactor binding;
Cellular component	• mitochondrial intermembrane space; • mitochondrial matrix;
Biological process	• sulfur amino acid metabolic process; • sulfur amino acid catabolic process; • cellular nitrogen compound metabolic process; • small molecule metabolic process; • sulfide oxidation, using sulfide:quinone oxidoreductase;
	Sources: Amigo / QuickGO
Orthologs
	v; t; e;

Search
PMC	articles
PubMed	articles
NCBI	proteins

sulfite oxidase
	Sulfite oxidase catalyses the oxidation-reduction reaction of sulfite and water, yielding sulfate.
Identifiers
EC number	1.8.3.1
CAS number	9029-38-3
Databases
IntEnz	IntEnz view
BRENDA	BRENDA entry
ExPASy	NiceZyme view
KEGG	KEGG entry
MetaCyc	metabolic pathway
PRIAM	profile
PDB structures	RCSB PDB PDBe PDBsum
Gene Ontology	AmiGO / EGO
Search
PMC	articles
PubMed	articles
NCBI	proteins