Branched-chain amino acid catabolism (Homo sapiens)

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2, 2018, 3933, 421134, 442612, 155, 2223, 24461, 2, 20, 254128, 35, 45386-8, 21414, 19, 3213, 319, 10, 27, 29, 403017, 37, 4323, 24143, 16, 3628, 35, 4514mitochondrial matrixcytosol2OGBCAT2 dimerbHIB-CoASUCCAHCO3-HIBADH tetramerGly2MBUT-CoA L-GluACADSB tetramerp-S292-BCKDHB CARKIC PPM1K:Mn2+IVD Fe2+ NADHIVD tetramerH2OBCKDHA FAD HIBADH L-Val DLD L-GluISV-CoAALDH9A1 tetramerTMLYS2OGBCAAsKIC,KMVA,KIVATPH+ALDH9A1 NADHALDH6A1AUH O2lipo-K44-DBT KMVA FADH2BCKDHA TMLHE ISB-CoA lipo-K44-DBT L-Ile bHIBAenoyl-CoA hydratasePiACAT1 tetramerSHMT1 tetramerTEABLMACR-CoAFADBBOX1 2MACA-CoAbMC-CoAFe2+ H2OAUH hexamerBCAT1 dimerPPM1K Btn-MCCC1 ADPNAD+FAD bHMG-CoACO2L-Leu DLD KIV TDP 2MBUT-CoAAc-CoAL-Val CoA-SHKIC CO2FAD NAD+FAD carnitine exporterBCAA-CoAsCoA-SHbMC-CoAMCCC2 CARlipo-BCKDHBBOX1 dimerPXLP-SHMT1 HSD17B10 tetramerPROP-CoACoA-SHCO26x(Btn-MCCC1:MCCC2)H2OFAD NAD+ACAT1(35-427) ADPACAD8 ISV-CoA ATPH+L-Leu TEABTPiLeu, Ile, ValHTMLYSBCKDKO2BCKDHB HSD17B10 SUCCAaMbHBUT-CoAKIV ACADSB(52-432) PXLP-BCAT2 ISB-CoAH2OHIBCHHTMLYSp-BCKDHNADH2OGCO2KMVA NADHNADHH+FADH2Leu, Ile, ValH2OH+PXLP-BCAT1 tiglyl-CoATMLHE dimerCoA-SHNAD+Mn2+ FADACAD8 tetramerNAD+2M3OPROAL-Ile TDP 9, 1012, 151119163112, 15292427, 40143, 164112335, 4593013, 3127, 401434294399, 10946


Description

The branched-chain amino acids, leucine, isoleucine, and valine, are all essential amino acids (i.e., ones required in the diet). They are major constituents of muscle protein. The breakdown of these amino acids starts with two common steps catalyzed by enzymes that act on all three amino acids: reversible transamination by branched-chain amino acid aminotransferase, and irreversible oxidative decarboxylation by the branched-chain ketoacid dehydrogenase complex. Isovaleryl-CoA is produced from leucine by these two reactions, alpha-methylbutyryl-CoA from isoleucine, and isobutyryl-CoA from valine. These acyl-CoA's undergo dehydrogenation, catalyzed by three different but related enzymes, and the breakdown pathways then diverge. Leucine is ultimately converted to acetyl-CoA and acetoacetate; isoleucine to acetyl-CoA and succinyl-CoA; and valine to succinyl-CoA. Under fasting conditions, substantial amounts of all three amino acids are generated by protein breakdown. In muscle, the final products of leucine, isoleucine, and valine catabolism can be fully oxidized via the citric acid cycle; in liver they can be directed toward the synthesis of ketone bodies (acetoacetate and acetyl-CoA) and glucose (succinyl-CoA) (Chuang & Shih 2001, Sweetman & Williams 2001). View original pathway at:Reactome.

Comments

Reactome-Converter 
Pathway is converted from Reactome ID: 70895
Reactome-version 
Reactome version: 66
Reactome Author 
Reactome Author: D'Eustachio, Peter

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Bibliography

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History

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CompareRevisionActionTimeUserComment
114709view16:18, 25 January 2021ReactomeTeamReactome version 75
113154view11:22, 2 November 2020ReactomeTeamReactome version 74
112382view15:31, 9 October 2020ReactomeTeamReactome version 73
101285view11:17, 1 November 2018ReactomeTeamreactome version 66
100822view20:48, 31 October 2018ReactomeTeamreactome version 65
100363view19:23, 31 October 2018ReactomeTeamreactome version 64
99908view16:06, 31 October 2018ReactomeTeamreactome version 63
99464view14:39, 31 October 2018ReactomeTeamreactome version 62 (2nd attempt)
99120view12:40, 31 October 2018ReactomeTeamreactome version 62
93924view13:45, 16 August 2017ReactomeTeamreactome version 61
93505view11:25, 9 August 2017ReactomeTeamreactome version 61
87096view14:29, 18 July 2016MkutmonOntology Term : 'amino acid metabolic pathway' added !
86600view09:21, 11 July 2016ReactomeTeamreactome version 56
83446view12:25, 18 November 2015ReactomeTeamNew pathway

External references

DataNodes

View all...
NameTypeDatabase referenceComment
2M3OPROAMetaboliteCHEBI:16256 (ChEBI)
2MACA-CoAMetaboliteCHEBI:15476 (ChEBI)
2MBUT-CoA MetaboliteCHEBI:15477 (ChEBI)
2MBUT-CoAMetaboliteCHEBI:15477 (ChEBI)
2OGMetaboliteCHEBI:30915 (ChEBI)
6x(Btn-MCCC1:MCCC2)ComplexR-HSA-70770 (Reactome)
ACAD8 ProteinQ9UKU7 (Uniprot-TrEMBL)
ACAD8 tetramerComplexR-HSA-70856 (Reactome)
ACADSB tetramerComplexR-HSA-70797 (Reactome)
ACADSB(52-432) ProteinP45954 (Uniprot-TrEMBL)
ACAT1 tetramerComplexR-HSA-70839 (Reactome)
ACAT1(35-427) ProteinP24752 (Uniprot-TrEMBL)
ADPMetaboliteCHEBI:16761 (ChEBI)
ALDH6A1ProteinQ02252 (Uniprot-TrEMBL)
ALDH9A1 ProteinP49189 (Uniprot-TrEMBL)
ALDH9A1 tetramerComplexR-HSA-71258 (Reactome)
ATPMetaboliteCHEBI:15422 (ChEBI)
AUH ProteinQ13825 (Uniprot-TrEMBL)
AUH hexamerComplexR-HSA-508309 (Reactome)
Ac-CoAMetaboliteCHEBI:15351 (ChEBI)
BBOX1 ProteinO75936 (Uniprot-TrEMBL)
BBOX1 dimerComplexR-HSA-71107 (Reactome)
BCAA-CoAsComplexR-ALL-508261 (Reactome)
BCAAsComplexR-ALL-508181 (Reactome)
BCAT1 dimerComplexR-HSA-70699 (Reactome)
BCAT2 dimerComplexR-HSA-70704 (Reactome)
BCKDHA ProteinP12694 (Uniprot-TrEMBL)
BCKDHB ProteinP21953 (Uniprot-TrEMBL)
BCKDKProteinO14874 (Uniprot-TrEMBL)
Btn-MCCC1 ProteinQ96RQ3 (Uniprot-TrEMBL)
CARMetaboliteCHEBI:17126 (ChEBI)
CO2MetaboliteCHEBI:16526 (ChEBI)
CoA-SHMetaboliteCHEBI:15346 (ChEBI)
DLD ProteinP09622 (Uniprot-TrEMBL)
FAD MetaboliteCHEBI:16238 (ChEBI)
FADMetaboliteCHEBI:16238 (ChEBI)
FADH2MetaboliteCHEBI:17877 (ChEBI)
Fe2+ MetaboliteCHEBI:18248 (ChEBI)
GlyMetaboliteCHEBI:57305 (ChEBI)
H+MetaboliteCHEBI:15378 (ChEBI)
H2OMetaboliteCHEBI:15377 (ChEBI)
HCO3-MetaboliteCHEBI:17544 (ChEBI)
HIBADH ProteinP31937 (Uniprot-TrEMBL)
HIBADH tetramerComplexR-HSA-70883 (Reactome)
HIBCHProteinQ6NVY1 (Uniprot-TrEMBL)
HSD17B10 ProteinQ99714 (Uniprot-TrEMBL)
HSD17B10 tetramerComplexR-HSA-508381 (Reactome)
HTMLYSMetaboliteCHEBI:15786 (ChEBI)
ISB-CoA MetaboliteCHEBI:15479 (ChEBI)
ISB-CoAMetaboliteCHEBI:15479 (ChEBI)
ISV-CoA MetaboliteCHEBI:15487 (ChEBI)
ISV-CoAMetaboliteCHEBI:15487 (ChEBI)
IVD ProteinP26440 (Uniprot-TrEMBL)
IVD tetramerComplexR-HSA-70730 (Reactome)
KIC MetaboliteCHEBI:17865 (ChEBI)
KIC,KMVA,KIVComplexR-ALL-508187 (Reactome)
KIV MetaboliteCHEBI:16530 (ChEBI)
KMVA MetaboliteCHEBI:28654 (ChEBI)
L-GluMetaboliteCHEBI:29985 (ChEBI)
L-Ile MetaboliteCHEBI:58045 (ChEBI)
L-Leu MetaboliteCHEBI:57427 (ChEBI)
L-Val MetaboliteCHEBI:57762 (ChEBI)
Leu, Ile, ValComplexR-ALL-508182 (Reactome)
Leu, Ile, ValComplexR-ALL-508190 (Reactome)
MACR-CoAMetaboliteCHEBI:27754 (ChEBI)
MCCC2 ProteinQ9HCC0 (Uniprot-TrEMBL)
Mn2+ MetaboliteCHEBI:29035 (ChEBI)
NAD+MetaboliteCHEBI:15846 (ChEBI)
NADHMetaboliteCHEBI:16908 (ChEBI)
O2MetaboliteCHEBI:15379 (ChEBI)
PPM1K ProteinQ8N3J5 (Uniprot-TrEMBL)
PPM1K:Mn2+ComplexR-HSA-5693133 (Reactome)
PROP-CoAMetaboliteCHEBI:15539 (ChEBI)
PXLP-BCAT1 ProteinP54687 (Uniprot-TrEMBL)
PXLP-BCAT2 ProteinO15382 (Uniprot-TrEMBL)
PXLP-SHMT1 ProteinP34896 (Uniprot-TrEMBL)
PiMetaboliteCHEBI:18367 (ChEBI)
SHMT1 tetramerComplexR-HSA-71243 (Reactome)
SUCCAMetaboliteCHEBI:15741 (ChEBI)
TDP MetaboliteCHEBI:18290 (ChEBI)
TEABLMetaboliteCHEBI:18020 (ChEBI)
TEABTMetaboliteCHEBI:16244 (ChEBI)
TMLHE ProteinQ9NVH6 (Uniprot-TrEMBL)
TMLHE dimerComplexR-HSA-71098 (Reactome)
TMLYSMetaboliteCHEBI:17311 (ChEBI)
aMbHBUT-CoAMetaboliteCHEBI:15449 (ChEBI)
bHIB-CoAMetaboliteCHEBI:28259 (ChEBI)
bHIBAMetaboliteCHEBI:11805 (ChEBI)
bHMG-CoAMetaboliteCHEBI:15467 (ChEBI)
bMC-CoAMetaboliteCHEBI:15486 (ChEBI)
bMC-CoAMetaboliteCHEBI:15488 (ChEBI)
carnitine exporterR-HSA-165022 (Reactome)
enoyl-CoA hydrataseR-HSA-70827 (Reactome)
lipo-BCKDHComplexR-HSA-70019 (Reactome)
lipo-K44-DBT ProteinP11182 (Uniprot-TrEMBL)
p-BCKDHComplexR-HSA-5693120 (Reactome)
p-S292-BCKDHB ProteinP21953 (Uniprot-TrEMBL)
tiglyl-CoAMetaboliteCHEBI:15478 (ChEBI)

Annotated Interactions

View all...
SourceTargetTypeDatabase referenceComment
2M3OPROAArrowR-HSA-70885 (Reactome)
2M3OPROAR-HSA-508473 (Reactome)
2M3OPROAR-HSA-70893 (Reactome)
2MACA-CoAArrowR-HSA-70837 (Reactome)
2MACA-CoAR-HSA-508369 (Reactome)
2MACA-CoAR-HSA-70844 (Reactome)
2MBUT-CoAR-HSA-70800 (Reactome)
2OGArrowR-HSA-508179 (Reactome)
2OGArrowR-HSA-508189 (Reactome)
2OGR-HSA-70723 (Reactome)
2OGR-HSA-70724 (Reactome)
2OGR-HSA-71241 (Reactome)
2OGR-HSA-71261 (Reactome)
6x(Btn-MCCC1:MCCC2)mim-catalysisR-HSA-508308 (Reactome)
6x(Btn-MCCC1:MCCC2)mim-catalysisR-HSA-70773 (Reactome)
ACAD8 tetramermim-catalysisR-HSA-70859 (Reactome)
ACADSB tetramermim-catalysisR-HSA-70800 (Reactome)
ACAT1 tetramermim-catalysisR-HSA-70844 (Reactome)
ADPArrowR-HSA-5693148 (Reactome)
ADPArrowR-HSA-70773 (Reactome)
ADPR-HSA-508308 (Reactome)
ALDH6A1mim-catalysisR-HSA-70893 (Reactome)
ALDH9A1 tetramermim-catalysisR-HSA-71260 (Reactome)
ATPArrowR-HSA-508308 (Reactome)
ATPR-HSA-5693148 (Reactome)
ATPR-HSA-70773 (Reactome)
AUH hexamermim-catalysisR-HSA-70785 (Reactome)
Ac-CoAArrowR-HSA-70844 (Reactome)
BBOX1 dimermim-catalysisR-HSA-71261 (Reactome)
BCAA-CoAsArrowR-HSA-70713 (Reactome)
BCAAsArrowR-HSA-70724 (Reactome)
BCAAsR-HSA-508179 (Reactome)
BCAAsR-HSA-70713 (Reactome)
BCAT1 dimermim-catalysisR-HSA-508189 (Reactome)
BCAT1 dimermim-catalysisR-HSA-70723 (Reactome)
BCAT2 dimermim-catalysisR-HSA-508179 (Reactome)
BCAT2 dimermim-catalysisR-HSA-70724 (Reactome)
BCKDKmim-catalysisR-HSA-5693148 (Reactome)
CARArrowR-HSA-164967 (Reactome)
CARArrowR-HSA-71261 (Reactome)
CARR-HSA-164967 (Reactome)
CO2ArrowR-HSA-70713 (Reactome)
CO2ArrowR-HSA-70893 (Reactome)
CO2ArrowR-HSA-71241 (Reactome)
CO2ArrowR-HSA-71261 (Reactome)
CoA-SHArrowR-HSA-70881 (Reactome)
CoA-SHR-HSA-70713 (Reactome)
CoA-SHR-HSA-70844 (Reactome)
CoA-SHR-HSA-70893 (Reactome)
FADH2ArrowR-HSA-70745 (Reactome)
FADH2ArrowR-HSA-70800 (Reactome)
FADH2ArrowR-HSA-70859 (Reactome)
FADR-HSA-70745 (Reactome)
FADR-HSA-70800 (Reactome)
FADR-HSA-70859 (Reactome)
GlyArrowR-HSA-71249 (Reactome)
H+ArrowR-HSA-70837 (Reactome)
H+ArrowR-HSA-70885 (Reactome)
H+ArrowR-HSA-70893 (Reactome)
H+ArrowR-HSA-71260 (Reactome)
H+R-HSA-508369 (Reactome)
H+R-HSA-508473 (Reactome)
H2OR-HSA-508308 (Reactome)
H2OR-HSA-5693153 (Reactome)
H2OR-HSA-70785 (Reactome)
H2OR-HSA-70830 (Reactome)
H2OR-HSA-70870 (Reactome)
H2OR-HSA-70881 (Reactome)
H2OR-HSA-71260 (Reactome)
HCO3-ArrowR-HSA-508308 (Reactome)
HCO3-R-HSA-70773 (Reactome)
HIBADH tetramermim-catalysisR-HSA-508473 (Reactome)
HIBADH tetramermim-catalysisR-HSA-70885 (Reactome)
HIBCHmim-catalysisR-HSA-70881 (Reactome)
HSD17B10 tetramermim-catalysisR-HSA-508369 (Reactome)
HSD17B10 tetramermim-catalysisR-HSA-70837 (Reactome)
HTMLYSArrowR-HSA-71241 (Reactome)
HTMLYSArrowR-HSA-8949413 (Reactome)
HTMLYSR-HSA-71249 (Reactome)
HTMLYSR-HSA-8949413 (Reactome)
ISB-CoAR-HSA-70859 (Reactome)
ISV-CoAR-HSA-70745 (Reactome)
IVD tetramermim-catalysisR-HSA-70745 (Reactome)
KIC,KMVA,KIVArrowR-HSA-70723 (Reactome)
KIC,KMVA,KIVR-HSA-508189 (Reactome)
L-GluArrowR-HSA-70723 (Reactome)
L-GluArrowR-HSA-70724 (Reactome)
L-GluR-HSA-508179 (Reactome)
L-GluR-HSA-508189 (Reactome)
Leu, Ile, ValArrowR-HSA-508179 (Reactome)
Leu, Ile, ValArrowR-HSA-508189 (Reactome)
Leu, Ile, ValR-HSA-70723 (Reactome)
Leu, Ile, ValR-HSA-70724 (Reactome)
MACR-CoAArrowR-HSA-70859 (Reactome)
MACR-CoAR-HSA-70870 (Reactome)
NAD+ArrowR-HSA-508369 (Reactome)
NAD+ArrowR-HSA-508473 (Reactome)
NAD+R-HSA-70713 (Reactome)
NAD+R-HSA-70837 (Reactome)
NAD+R-HSA-70885 (Reactome)
NAD+R-HSA-70893 (Reactome)
NAD+R-HSA-71260 (Reactome)
NADHArrowR-HSA-70713 (Reactome)
NADHArrowR-HSA-70837 (Reactome)
NADHArrowR-HSA-70885 (Reactome)
NADHArrowR-HSA-70893 (Reactome)
NADHArrowR-HSA-71260 (Reactome)
NADHR-HSA-508369 (Reactome)
NADHR-HSA-508473 (Reactome)
O2R-HSA-71241 (Reactome)
O2R-HSA-71261 (Reactome)
PPM1K:Mn2+mim-catalysisR-HSA-5693153 (Reactome)
PROP-CoAArrowR-HSA-70844 (Reactome)
PROP-CoAArrowR-HSA-70893 (Reactome)
PiArrowR-HSA-5693153 (Reactome)
PiArrowR-HSA-70773 (Reactome)
PiR-HSA-508308 (Reactome)
R-HSA-164967 (Reactome) Studies of carnitine (CAR) export from intact rat liver indicate that this process is mediated by a specific, saturable transporter molecule (Sandor et al. 1985). The transporter itself has not been identified, but its properties are distinct from those of OCTN2, the major transport protein responsible for carnitine uptake (Kispal et al. 1987). The existence of a human transport reaction (again without an identified transporter) is inferred from the rat one.
R-HSA-508179 (Reactome) Mitochondrial branched-chain-amino-acid aminotransferase (BCAT2) catalyzes the reversible reactions of alpha-ketoisocaproate, alpha-keto-beta-methylvalerate, or a-ketoisovalerate with glutamate to form leucine, isoleucine, or valine, respectively, and alpha-ketoglutarate (Bledsoe et al. 1997). The active enzyme is a homodimer (Yennawar et al. 2001, 2002). In the body, this enzyme is widely expressed but is especially abundant in muscle tissue.
R-HSA-508189 (Reactome) Cytosolic branched-chain-amino-acid aminotransferase (BCAT1) catalyzes the reversible reactions of alpha-ketoisocaproate, alpha-keto-beta-methylvalerate, or a-ketoisovalerate with glutamate to form leucine, isoleucine, or valine, respectively, and alpha-ketoglutarate (2-oxoglutarate). The active enzyme is a homodimer (Goto et al. 2005).
R-HSA-508308 (Reactome) Methylcrotonyl CoA carboxylase (MCCA) catalyzes the reversible reaction of beta-methylglutaconyl-CoA, ADP, orthophosphate, and H2O to form beta-methylcrotonyl-CoA, ATP, and CO2. Active MCCA is composed of two polypeptides, MCCA1 and MCCA2 (Baumgartner et al. 2001; Holzinger et al. 2001). The enzyme has been purified from fibroblast mitochondria. By analogy to the more thoroughly studied bovine homologue, MCCA is thought to be a hexamer of six MCCA1:MCCA2 dimers, and the MCCA1 polypeptides are thought to have biotin moieties covalently bound to a lysine residue at position 681 in the polypeptide chain. Mitochondrial import of MCCA1 and 2 is associated with removal of aminoterminal mitochondrial targeting sequences but the exact lengths of these sequences have not been determined.
R-HSA-508369 (Reactome) Mitochondrial 3-hydroxyacyl-CoA dehydrogenase type-2 (HSD17B10; HADH2) catalyzes the reversible reaction of alpha-methylacetoacetyl-CoA and NADH + H+ to form alpha-methyl-beta-hydroxybutyryl-CoA and NAD+ (Ofman et al. 2003). Crystallographic data indicate that the enzyme is a homotetramer (Kissinger et al. 2004).
R-HSA-508473 (Reactome) Mitochondrial 3-hydroxyisobutyrate dehydrogenase (HIBADH) catalyzes the reversible reaction of methylmalonyl semialdehyde and NADH + H+ to form beta-hydroxyisobutyrate and NAD+. The biochemical properties of human HIBADH are inferred from those of its better-studied porcine homologue (Robinson and Coon 1957). Unpublished crystallographic studies (PDB 2GF2) have shown the active enzyme to be a tetramer of HIBADH polypeptides whose aminoterminal 40 residues, a mitochondrial targeting sequence, have been removed.
R-HSA-5693148 (Reactome) Mitochondrial 3-methyl-2-oxobutanoate dehydrogenase (lipoamide) kinase (BCKDK) catalyses the phosphorylation and inactivation of the branched-chain alpha-ketoacid dehydrogenase (BCKDH) complex, the key regulatory enzyme of the valine, leucine and isoleucine catabolic pathways (Li et al. 2004, Wynn et al. 2004). BCKDH occupies a strategic point in the branched-chain amino acid (BCAA) catabolic pathway, and careful regulation of its activity is essential for correct BCAA metabolism. The overall activity of the BCKDH complex is controlled by the phosphorylation (inactivation)/dephosphorylation (activation) cycle.
Defects in BCKDK can cause branched-chain ketoacid dehydrogenase kinase deficiency (BCKDKD; MIM:614923), a metabolic disorder characterised by autism, epilepsy, intellectual disability, and reduced BCAAs (Novarino et al. 2012, Garcia-Cazorla et al. 2014).
R-HSA-5693153 (Reactome) The branched-chain alpha-ketoacid dehydrogenase (BCKDH) complex occupies a strategic point in the branched-chain amino acid (BCAA) catabolic pathway, and careful regulation of its activity is essential for correct BCAA metabolism. The overall activity of the BCKDH complex is controlled by the phosphorylation (inactivation)/dephosphorylation (activation) cycle. Mitochondrial protein phosphatase 1K (PPM1K) dephosphorylates the E1 beta subunit of BCKDH therby regaining its active state. PPM1K requires Mn2+ as a cofactor for phosphatase activity (Wynn et al. 2012).
R-HSA-70713 (Reactome) The mitochondrial branched-chain alpha-ketoacid dehydrogenase (BKCDH) complex catalyzes the reactions of alpha-ketoisocaproate, alpha-keto beta-methylvalerate, or alpha-ketoisovalerate with CoA and NAD+ to form isovaleryl-CoA, a-methylbutyryl-CoA, or isobuyryl-CoA, respectively, and CO2 and NADH (Chuang and Shih 2001). While bovine and microbial BCKD complexes have been characterized most extensively (Reed and Hackert 1990), structural studies of individual components and subcomplexes of human BKCD have confirmed their structures and roles in the overall oxidative carboxylation process, and have related these features to the disruptive effects of mutations on branched-chain amino acid metabolism in vivo: E1a and E1b components - AEvarsson et al. 2000; E2 - Chang et al. 2002; E3- Brautigam et al. 2005. In addition, structural studies have confirmed the lipoylation of lysine residue 44 in E2 protein (Chang et al. 2002) and the loss of an aminoterminal mitochondrial transport sequence from mature E3 protein (Bruatigam et al. 2005). Loss of mitochondrial transport sequences from proteins E1a, E1b, and E2 has been domstrated by sequence analysis (Wynn et al. 1999).
R-HSA-70723 (Reactome) Cytosolic branched-chain-amino-acid aminotransferase (BCAT1) catalyzes the reversible reactions of leucine, isoleucine, or valine with alpha-ketoglutarate (2-oxoglutarate) to form alpha-ketoisocaproate, alpha-keto-beta-methylvalerate, or a-ketoisovalerate, respectively, and glutamate. The active enzyme is a homodimer. Hutson and colleagues have argues that cytosolic BCAT1 plays a major role in the generation of glutamate involved in synaptic transmission in neural tissue (Goto et al. 2005).
R-HSA-70724 (Reactome) Mitochondrial branched-chain-amino-acid aminotransferase (BCAT2) catalyzes the reversible reactions of leucine, isoleucine, or valine with alpha-ketoglutarate (2-oxoglutarate) to form alpha-ketoisocaproate, alpha-keto-beta-methylvalerate, or a-ketoisovalerate, respectively, and glutamate (Bledsoe et al. 1997). The active enzyme is a homodimer (Yennawar et al. 2001, 2002). In the body, this enzyme is widely expressed but is especially abundant in muscle tissue.
R-HSA-70745 (Reactome) Mitochondrial isovaleryl dehydrogenase (IVD) catalyzes the reaction of isovaleryl-CoA and FAD to form beta-methylcrotonyl-CoA and FADH2 (Finocchiaro et al. 1978; Rhead and Tanaka 1980). Crystallographic studies demonstrated the existene of a tetramer of IVD polypeptides lacking an aminoterminal mitochondrial targeting sequence (Tiffany et al. 1997).
R-HSA-70773 (Reactome) Methylcrotonyl CoA carboxylase (MCCA) catalyzes the reversible reaction of beta-methylcrotonyl-CoA, ATP, and CO2 to form beta-methylglutaconyl-CoA, ADP, orthophosphate, and H2O. Active MCCA is composed of two polypeptides, MCCA1 and MCCA2 (Baumgartner et al. 2001; Holzinger et al. 2001). The enzyme has been purified from fibroblast mitochondria. By analogy to the more thoroughly studied bovine homologue, MCCA is thought to be a hexamer of six MCCA1:MCCA2 dimers, and the MCCA1 polypeptide is thought to have a biotin moiety covalently bound to lysine residue 681. Localization of the complex to the mitochondrial inner membrane is inferred from studies of the bovine homologue (Hector et al. 1980). Mitochondrial import of MCCA1 and 2 is associated with removal of aminoterminal mitochondrial targeting sequences (Stadler et al. 2005).
R-HSA-70785 (Reactome) Mitochondrial ethylglutaconyl-CoA hydratase (AUH) catalyzes the hydrolysis of beta-methylglutaconyl-CoA to yield beta-hydroxy-beta-methylglutaryl-CoA (IJlst et al. 2002; Narisawa et al. 1986). Crystallographic studies have shown the active enzyme to be a hexamer of AUH polypeptides whose aminoterminal 67 residues, a mitochondrial targeting sequence, have been removed ((Kurimoto et al. 2001).
R-HSA-70800 (Reactome) Mitochondrial 2-methyl branched chain acyl-CoA dehydrogenase (ACADSB) catalyzes the reaction of alpha-methylbutyryl-CoA and FAD to form 'tiglyl-CoA and FADH2 (Andresen et al. 2000; Gibson et al. 2000). Unpublished crystallographic data (PDB 2JIF) indicate that the enzyme is a tetramer of ACADSB polypeptides whose aminoterminal 51 residues, a mitochondrial targeting sequence, have been removed.
R-HSA-70830 (Reactome) Mitochondrial tiglyl-CoA is hydrolyzed to form alpha-methyl-beta-hydroxybutyryl-CoA. While crude extracts of human liver cells have been shown to catalyze the reaction, the specific enzyme responsible for it has not been identified (Sweetman and Williams 2001).
R-HSA-70837 (Reactome) Mitochondrial 3-hydroxyacyl-CoA dehydrogenase type-2 (HSD17B10; HADH2) catalyzes the reversible reaction of alpha-methyl-beta-hydroxybutyryl-CoA and NAD+ to form alpha-methylacetoacetyl-CoA and NADH + H+ (Ofman et al. 2003). Crystallographic data indicate that the enzyme is a homotetramer (Kissinger et al. 2004).
R-HSA-70844 (Reactome) Mitochondrial acetyl-CoA acetyltransferase (ACAT1) catalyzes the reaction of alpha-methyl-acetoacetyl-CoA and CoA to form propionyl-CoA and acetyl-CoA. Structural studies have shown the active enzyme to be a tetramer of ACAT1 polypeptides whose aminoterminal 34 residues, a mitochondrial targeting sequence, have been removed (Haapalainen et al. 2007).
R-HSA-70859 (Reactome) Mitochondrial isobutyryl-CoA dehydrogenase (ACAD8) catalyzes the reaction of isobutyryl-CoA and FAD to form methacrylyl-CoA and FADH2 (Roe et al. 1999; Nguyen et al. 2002). Crystallographic studies have shown the active enzyme to be a tetramer of ACAD8 polypeptides whose aminoterminal 23 residues, a mitochondrial targeting sequence, have been removed (Bataille et al. 2004).
R-HSA-70870 (Reactome) The reversible reaction of methacrylyl-CoA and water to form beta-hydroxybutyryl-CoA takes place in the mitochondrial matrix. While crude extracts of human fibroblasts and liver cells have been shown to catalyze the reaction, the specific human enzyme responsible for it has not been identified.
R-HSA-70881 (Reactome) Mitochondrial 3-hydroxyisobutyryl-CoA hydrolase (HIBCH) catalyzes the hydrolysis of beta-hydroxyisobutyryl-CoA to form beta-hydroxyisobutyrate (3-hydroxy-2-methylpropanoate) and CoA (Hawes et al. 1996).
R-HSA-70885 (Reactome) Mitochondrial 3-hydroxyisobutyrate dehydrogenase (HIBADH) catalyzes the reversible reaction of beta-hydroxyisobutyrate and NAD+ to form methylmalonyl semialdehyde and NADH + H+. The biochemical properties of human HIBADH are inferred from those of its better-studied porcine homologue (Robinson and Coon 1957). Unpublished crystallographic studies (PDB 2GF2) have shown the active enzyme to be a tetramer of HIBADH polypeptides whose aminoterminal 40 residues, a mitochondrial targeting sequence, have been removed.
R-HSA-70893 (Reactome) Mitochondrial methylmalonate semialdehyde dehydrogenase (ALDH6A1) catalyzes the reaction of methylmalonate semialdehyde, NAD+, and CoA to form propionyl-CoA, CO2, and NADH + H+. A human ALDH6A1 gene has been cloned. Its sequence is closely homologous to that of the better-characterized rat enzyme (Kedishvili et al. 1992) and a missense mutation in a normally well-conserved codon has been found in the allele of the gene from a patient with a defect in methylmalonic semialdehyde dehydrogenase activity (Chambliss et al. 2000).
R-HSA-71241 (Reactome) Trimethyllysine dioxygenase (TMLHE) dimer in the mitochondrial matrix catalyzes the reaction of oxygen, 2-oxoglutarate (2OG), and N6,N6,N6-trimethyl-L-lysine (TMLYS) to form CO2, 3-hydroxy-N6,N6,N6-trimethyl-L-lysine (HTMLYS), and succinate (SUCCA) (Vaz et al. 2001).
R-HSA-71249 (Reactome) Cytosolic serine hydroxymethyltransferase tetramer (SHMT1) catalyzes the reaction of 3-Hydroxy-N6,N6,N6-trimethyl-L-lysine (NTMLYS) to form glycine (Gly) and 4-trimethylammoniobutanal (TEABL) in vitro (Hulse et al. 1978). The possibility that an additional enzyme may catalyze this reaction in vivo has not been excluded (Bremer 1983).
R-HSA-71260 (Reactome) Cytosolic 4-trimethylaminobutyraldehyde dehydrogenase (ALDH9A1) tetramer catalyzes the reaction of NAD+ and 4-trimethylammoniobutanal (TEABL) to form 4-trimethylammoniobutanoate (TEABT) and NADH + H+ (Kurys et al. 1989; Vaz et al. 2000).
R-HSA-71261 (Reactome) Cytosolic gamma-butyrobetaine hydroxylase dimer (BBOX1), a dioxygenase, catalyzes the reaction of oxygen, 4-trimethylammoniobutanoate (TEABT), and 2-oxoglutarate (2OG)to form CO2, succinate (SUCCA), and carnitine (CAR) (Lindstedt and Nordin 1984; Vaz et al. 1998).
R-HSA-8949413 (Reactome) HTMLYS (3-Hydroxy-N6,N6,N6-trimethyl-L-lysine) moves from the mitochondrial matrix to the cytosol (Longo et al. 2016). The molecular mechanism for this translocation is unknown.
SHMT1 tetramermim-catalysisR-HSA-71249 (Reactome)
SUCCAArrowR-HSA-71241 (Reactome)
SUCCAArrowR-HSA-71261 (Reactome)
TEABLArrowR-HSA-71249 (Reactome)
TEABLR-HSA-71260 (Reactome)
TEABTArrowR-HSA-71260 (Reactome)
TEABTR-HSA-71261 (Reactome)
TMLHE dimermim-catalysisR-HSA-71241 (Reactome)
TMLYSR-HSA-71241 (Reactome)
aMbHBUT-CoAArrowR-HSA-508369 (Reactome)
aMbHBUT-CoAArrowR-HSA-70830 (Reactome)
aMbHBUT-CoAR-HSA-70837 (Reactome)
bHIB-CoAArrowR-HSA-70870 (Reactome)
bHIB-CoAR-HSA-70881 (Reactome)
bHIBAArrowR-HSA-508473 (Reactome)
bHIBAArrowR-HSA-70881 (Reactome)
bHIBAR-HSA-70885 (Reactome)
bHMG-CoAArrowR-HSA-70785 (Reactome)
bMC-CoAArrowR-HSA-508308 (Reactome)
bMC-CoAArrowR-HSA-70745 (Reactome)
bMC-CoAArrowR-HSA-70773 (Reactome)
bMC-CoAR-HSA-508308 (Reactome)
bMC-CoAR-HSA-70773 (Reactome)
bMC-CoAR-HSA-70785 (Reactome)
carnitine exportermim-catalysisR-HSA-164967 (Reactome)
enoyl-CoA hydratasemim-catalysisR-HSA-70830 (Reactome)
enoyl-CoA hydratasemim-catalysisR-HSA-70870 (Reactome)
lipo-BCKDHArrowR-HSA-5693153 (Reactome)
lipo-BCKDHR-HSA-5693148 (Reactome)
lipo-BCKDHmim-catalysisR-HSA-70713 (Reactome)
p-BCKDHArrowR-HSA-5693148 (Reactome)
p-BCKDHR-HSA-5693153 (Reactome)
tiglyl-CoAArrowR-HSA-70800 (Reactome)
tiglyl-CoAR-HSA-70830 (Reactome)
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