Fructose metabolism (Homo sapiens)

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13. O'Brien MM, Schofield PJ, Edwards MR.; ''Polyol-pathway enzymes of human brain. Partial purification and properties of sorbitol dehydrogenase.''; PubMed Europe PMC Scholia
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28. Beutler E, Guinto E.; ''Dihydroxyacetone metabolism by human erythrocytes: demonstration of triokinase activity and its characterization.''; PubMed Europe PMC Scholia
29. Xu MY, Jia XF, Qu Y, Zheng RD, Yuan ZH, Weng HL, Dooley S, Wang XP, Zhang LJ, Lu LG.; ''Serum dihydroxyacetone kinase peptide m/z 520.3 as predictor of disease severity in patients with compensated chronic hepatitis B.''; PubMed Europe PMC Scholia
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31. Sass JO, Fischer K, Wang R, Christensen E, Scholl-Bürgi S, Chang R, Kapelari K, Walter M.; ''D-glyceric aciduria is caused by genetic deficiency of D-glycerate kinase (GLYCTK).''; PubMed Europe PMC Scholia
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33. Schapira F.; ''Kinetic and immunological abnormalities of aldolase B in herediatry fructose intolerance.''; PubMed Europe PMC Scholia
34. Van Schaftingen E.; ''D-glycerate kinase deficiency as a cause of D-glyceric aciduria.''; PubMed Europe PMC Scholia
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History

External references

DataNodes

Name	Type	Database reference	Comment
3PDGA	Metabolite	CHEBI:58272 (ChEBI)
ADP	Metabolite	CHEBI:456216 (ChEBI)
AKR1B1	Protein	P15121 (Uniprot-TrEMBL)
ALDH1A1	Protein	P00352 (Uniprot-TrEMBL)
ALDH1A1 tetramer	Complex	R-HSA-71689 (Reactome)
ALDOB	Protein	P05062 (Uniprot-TrEMBL)
ALDOB tetramer	Complex	R-HSA-70340 (Reactome)
ATP	Metabolite	CHEBI:30616 (ChEBI)
D-sorbitol	Metabolite	CHEBI:17924 (ChEBI)
DGA	Metabolite	CHEBI:32398 (ChEBI)
DHAP	Metabolite	CHEBI:57642 (ChEBI)
Fru 1-P	Metabolite	CHEBI:18105 (ChEBI)
Fru	Metabolite	CHEBI:15824 (ChEBI)
GA3P	Metabolite	CHEBI:59776 (ChEBI)
GA	Metabolite	CHEBI:17378 (ChEBI)
GLYCTK	Protein	Q8IVS8 (Uniprot-TrEMBL)
Glc	Metabolite	CHEBI:17925 (ChEBI)
H+	Metabolite	CHEBI:15378 (ChEBI)
H2O	Metabolite	CHEBI:15377 (ChEBI)
K+	Metabolite	CHEBI:29103 (ChEBI)
KHK	Protein	P50053 (Uniprot-TrEMBL)
KHK dimer	Complex	R-HSA-3006523 (Reactome)
Mg2+	Metabolite	CHEBI:18420 (ChEBI)
NAD+	Metabolite	CHEBI:57540 (ChEBI)
NADH	Metabolite	CHEBI:57945 (ChEBI)
NADP+	Metabolite	CHEBI:18009 (ChEBI)
NADPH	Metabolite	CHEBI:16474 (ChEBI)
SORD	Protein	Q00796 (Uniprot-TrEMBL)
SORD tetramer	Complex	R-HSA-5652211 (Reactome)
TKFC	Protein	Q3LXA3 (Uniprot-TrEMBL)
TKFC:2Mg2+ dimer	Complex	R-HSA-5652070 (Reactome)
Vitamin D (calciferol) metabolism	Pathway	R-HSA-196791 (Reactome)	Vitamin D3 (VD3, cholecalciferol) is a steroid hormone that principally plays roles in regulating intestinal calcium absorption and in bone metabolism. It is obtained from the diet and produced in the skin by photolysis of 7-dehydrocholesterol and released into the bloodstream. Very few foods (eg. oily fish, mushrooms exposed to sunlight and cod liver oil) are natural sources of vitamin D. A small number of countries in the world artificially fortify a few foods with vitamin D. The metabolites of vitamin D are carried in the circulation bound to a plasma protein called vitamin D binding protein (GC) (for review see Delanghe et al. 2015, Chun 2012). Vitamin D undergoes two subsequent hydroxylations to form the active form of the vitamin, 1-alpha, 25-dihydroxyvitamin D (1,25(OH)2D). The first hydroxylation takes place in the liver followed by subsequent transport to the kidney where the second hydroxylation takes place. 1,25(OH)2D acts by binding to nuclear vitamin D receptors (Neme et al. 2017) and it has been estimated that upwards of 2000 genes are directly or indirectly regulated which are involved in calcium homeostasis, immune responses, cellular growth, differentiation and apoptosis (Hossein-nezhad et al. 2013, Hossein-nezhad & Holick 2013). Inactivation of 1,25(OH)2D occurs via C23/C24 oxidation catalysed by cytochrome CYP24A1 enzyme (Christakos et al. 2016).
Zn2+	Metabolite	CHEBI:29105 (ChEBI)

Annotated Interactions

Source	Target	Type	Database reference	Comment
	3PDGA	Arrow	R-HSA-6799495 (Reactome)
	ADP	Arrow	R-HSA-6799495 (Reactome)
	ADP	Arrow	R-HSA-70333 (Reactome)
	ADP	Arrow	R-HSA-70349 (Reactome)
ADP		TBar	R-HSA-70333 (Reactome)
AKR1B1		mim-catalysis	R-HSA-5652172 (Reactome)
ALDH1A1 tetramer		mim-catalysis	R-HSA-6813749 (Reactome)
ALDOB tetramer		mim-catalysis	R-HSA-70342 (Reactome)
ATP			R-HSA-6799495 (Reactome)
ATP			R-HSA-70333 (Reactome)
ATP			R-HSA-70349 (Reactome)
	D-sorbitol	Arrow	R-HSA-5652172 (Reactome)
D-sorbitol			R-HSA-5652195 (Reactome)
	DGA	Arrow	R-HSA-6813749 (Reactome)
DGA			R-HSA-6799495 (Reactome)
	DHAP	Arrow	R-HSA-70342 (Reactome)
	Fru 1-P	Arrow	R-HSA-70333 (Reactome)
Fru 1-P			R-HSA-70342 (Reactome)
	Fru	Arrow	R-HSA-5652195 (Reactome)
Fru			R-HSA-70333 (Reactome)
	GA3P	Arrow	R-HSA-70349 (Reactome)
	GA	Arrow	R-HSA-70342 (Reactome)
GA			R-HSA-6813749 (Reactome)
GA			R-HSA-70349 (Reactome)
GLYCTK		mim-catalysis	R-HSA-6799495 (Reactome)
Glc			R-HSA-5652172 (Reactome)
	H+	Arrow	R-HSA-5652195 (Reactome)
	H+	Arrow	R-HSA-6799495 (Reactome)
	H+	Arrow	R-HSA-6813749 (Reactome)
H+			R-HSA-5652172 (Reactome)
H2O			R-HSA-6813749 (Reactome)
K+		Arrow	R-HSA-70333 (Reactome)
KHK dimer		mim-catalysis	R-HSA-70333 (Reactome)
NAD+			R-HSA-5652195 (Reactome)
NAD+			R-HSA-6813749 (Reactome)
	NADH	Arrow	R-HSA-5652195 (Reactome)
	NADH	Arrow	R-HSA-6813749 (Reactome)
	NADP+	Arrow	R-HSA-5652172 (Reactome)
NADPH			R-HSA-5652172 (Reactome)
			R-HSA-5652172 (Reactome)	Cytosolic AKR1B1 (aldose reductase) catalyzes the reaction of glucose (Glc) and NADPH + H+ to form D-sorbitol and NADP+. This reaction was first described by Hers (1960) in sheep seminal vesicles; the human enzyme was identified by Nishimura et al. (1990) and is a potential target for treatment of diabetic neuropathy (Oates, 2008). The active enzyme is a monomer (Ruiz et al. 2004) whose amino-terminal methionine residue has been removed (Jacquinod et al. 1993). Under physiological conditions, formation of D-sorbitol is strongly favored (Grimshaw 1992).
			R-HSA-5652195 (Reactome)	Cytosolic SORD (sorbitol dehydrogenase) catalyzes the reaction of D-sorbitol and NAD+ to form fructose (Fru) and NADH + H+. This reaction was first described by Hers (1960) in sheep seminal vesicles; the human enzyme was identified by O'Brien et al. (1983). The active enzyme is a tetramer with four associated Zn2+ ions (Pauly et al. 2003) whose amino-terminal methionine residue has been removed (Karlsson et al. 1989).
			R-HSA-6799495 (Reactome)	D-glyceric acid (DGA) is an intermediate of serine catabolism and of a minor pathway of fructose metabolism. The only known fate of DGA is phosphorylation to 3-phospho-D-glyceric acid (3PDGA) by cytosolic glycerate kinase (GLYCTK) (Gou et al. 2006). Defects in GLYCTK can cause D-glyceric aciduria (D-GA; MIM:220120), a rare inborn error of serine and fructose metabolism where DGA is excreted in large amounts in the urine. A variable phenotype is observed, ranging from severe mental retardation and death to milder speech delays and normal development (Van Schaftingen 1989, Sass et al. 2010).
			R-HSA-6813749 (Reactome)	Retinal dehydrogenase 1 (ALDH1A1 tetramer) is a cytosolic aldehyde dehydrogenase that can oxidise glyceraldehyde (GA) to D-glycerate (DGA) (Yoval-Sanchez et al. 2013). DGA is a metabolite in a minor pathway of fructose catabolism and serine catabolism.
			R-HSA-70333 (Reactome)	Cytosolic ketohexokinase (KHK, also known as fructokinase) catalyzes the reaction of D-fructose (Fru) and ATP to form D-fructose 1-phosphate (Fru 1-P) and ADP. Two isoforms of the enzyme, A and C, are encoded by alternatively spliced forms of the gene; both form catalytically active dimers. The C isoform is predominant in liver and kidney tissues, has high affinity for fructose, and is probably responsible for the bulk of fructose phosphorylation in vivo (Asipu et al. 2003; Trinh et al. 2009). The A isoform is found in lower levels in many other tissues and may serve a role in fructose metabolism outside of liver and kidney (Funari et al. 2005). The physiological role of KHK has been established from metabolic and DNA sequencing studies of patients with essential fructosuria (Bonthron et al. 1994) and in mouse models for this disease (Diggle et al. 2010; Ishimoto et al. 2012).
			R-HSA-70342 (Reactome)	Cytosolic aldolase B (ALDOB) catalyzes the reaction of D-fructose 1-phosphate (Fru 1-P) to form dihydroxyacetone phosphate (DHAP) and D-glyceraldehyde (GA) (Hers & Kusaka 1953; Schapira 1975). The active form of the enzyme is a tetramer (Dalby et al. 2001). Deficiencies in the enzyme are associated with hereditary fructose intolerance in vivo (e.g., Tolan 1995; Ali et al. 1998). ALDOB is the same aldolase isoform that catalyzes the reversible cleavage of fructose-1,6-bisphosphate in glycolysis. This isoform, found in liver, kidney, and intestine, is approximately equally active with fructose 1 phosphate and fructose 1,6 bisphosphate as substrates at saturating concentrations, while the muscle and brain isoforms (ALDOA and ALDOC, respectively), have little activity with fructose-1-phosphate (Lebherz & Rutter 1969; Penhoet et el. 1969).
			R-HSA-70349 (Reactome)	Cytosolic dihydroxyacetone kinase (DAK) catalyzes the reaction of ATP and D-glyceraldehyde (GA) to form ADP and D-glyceraldehyde 3-phosphate (GA3P). This reaction was originally characterized in studies of guinea pig liver and human erythrocytes (Hers & Kusaka 1953; Beutler & Guinto 1973). The human enzyme has been cloned and studied (Cabezas et al. 2005; Rodrigues et al. 2014). DAK/TKFC also catalyzes the phosphorylation of dihydroxyacetone (DHA) to dihydroxyacetone phosphate (DHAP), not a necessary step in fructose catabolism, but possibly functional on exogenous DHA. Triokinase activities on GA and DHA require homodimeric enzyme formed by two-domain subunits, where triose binds to one subunit and ATP to the other, each in a different domain. DAK/TKFC is a bifunctional enzyme which, besides the ATP/Mg-dependent phosphorylation of GA and DHA, also catalyses, in presence of Mn2+, a unisubstrate reaction splitting flavin-adenine dinucleotide (FAD) into riboflavin cyclic 4',5'-phosphate (cyclic FMN) and AMP (Cabezas et al. 2005; Rodrigues et al. 2014). In addition, DAK/TKFC protein binds to MDA5 and acts as a negative regulator of MDA5-mediated induction of IFN-alpha/beta pathways (Diao et al. 2007). Potentially related to this TKFC effect are the observations that hepatic DAK/TKFC levels correlate with outcome in chronic hepatitis C patients treated with interferon (Perdomo et al. 2012), and that a DAK/TKFC serum peptide is a predictor of disease severity in hepatitis B patients (Xu et al. 2013).
SORD tetramer		mim-catalysis	R-HSA-5652195 (Reactome)
TKFC:2Mg2+ dimer		mim-catalysis	R-HSA-70349 (Reactome)