Citric acid cycle and respiratory electron transport (Homo sapiens)

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4, 5, 10, 33, 4930, 369, 7925, 7021, 42376719, 24, 623223, 63, 718, 12, 14, 43, 58...11, 39, 59, 6550, 805325, 7016, 28, 38, 55, 57...536, 18, 26, 762234, 35, 40, 4513, 15, 23, 54223, 20, 5216, 28, 38, 55, 57...34, 35, 45-47, 6917, 51, 61, 74488, 12, 14, 27, 58...31, 607321, 4229, 44, 777, 68, 7041, 7866, 7548mitochondrial matrixmitochondrial intermembrane spacecytosolLDHB LIPAM NADHNNT Co2+SUCC-CoAPDK2(?-407)SUCLG1:SUCLG2glyoxylateIDH3G PDP1 Mn2+Lipo-K110-DLST NAD+H2OFAD NADHPDK2(?-407) ADPNADHMg2+ CO2LDHA HBUTSLC16A1 MALCS dimerRXRA:PPARD:atRAH+PDK1 GSTZ1 FAHD1 Zn2+ MPC1 NADHLDHAL6BH+PYRPYRFAD IDH2 LACTCoA-SHCO2IDH2 dimerFH ME3:Mg2+ tetramerMn2+ ATPNADP+PDPNADP+NNT dimerPDK2(?-407) CO2H+IDH3B CO2ME2 ATPNADHFH tetramerNADP+TDP TDP SUCLG2 BSG:MCTsPDHA2 GLO1 dimer:2xZn2+H+H+SUCLG1 SUCLA2:SUCLG1SDHB LDH tetramerPiSUCCAAc-CoAGSHTDP Zn2+NADHZn2+ H+PDHA1 GLO1 SUCLG1 PDK isoformsMg2+ MDH2 H2OGTP(R)-S-LGSHHClRespiratory electrontransport, ATPsynthesis bychemiosmoticcoupling, and heatproduction byuncouplingproteins.NAD+ADPSDHC GSTZ1 dimerHAGH-2 GSHME2:Mg2+ tetramerCoA-SHBSG NAD+MGXLLDHAL6A H+PDHX NADHFUMACITCoA-SHDCAlipo-PDHMPC2 PDPR IDH3 complexNADPHMg2+ lipo-K132,K259-DLAT MPC1:MPC2LACTlipo-K132,K259-DLAT FADH2PDK3(?-406) FAD p-lipo-PDH2HGNADPHPDP2 CO2ISCITNADPHME1 ME3 L2HGDHMg2+DCA:PDK2IDH3A LACTIron Sulphur Cluster CS Mn2+ NAD+H+2OGSUCCSAPDHB ATPFADH2OH+Mg2+ ADPSDH complex (ox.)PDHA1 CO2FAD H+OAAFAHD1:Mg2+ dimerPDHA2 PPARD PDHX SDHA RXRA NAD+H+SUCLA2 D2HGDHADHFE1(1-?)NAD+H2OGSH CoA-SHPDHB MALlipo-aKGDHMDH2 dimerME1:Mg2+ tetramerGDPH+SLC16A3 LDHC DLD OGDH DLD NAD+FAD HAGH-2:2xZn2+PiACO2atRA DLD SLC16A8 2HGSDHD NADHPYRNAD+PDK4(?-411) VDAC13424347631, 60761, 2, 35, 45761, 2, 35, 4540, 45761, 255381, 23456


Description

The metabolism of pyruvate provides one source of acetyl-CoA which enters the citric acid (TCA, tricarboxylic acid) cycle to generate energy and the reducing equivalent NADH. These reducing equivalents are re-oxidized back to NAD+ in the electron transport chain (ETC), coupling this process with the export of protons across the inner mitochondrial membrane. The chemiosmotic gradient created is used to drive ATP synthesis. View original pathway at:Reactome.

Comments

Reactome-Converter 
Pathway is converted from Reactome ID: 1428517
Reactome-version 
Reactome version: 65
Reactome Author 
Reactome Author: Birney, Ewan, D'Eustachio, Peter, Schmidt, Esther

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Bibliography

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History

View all...
CompareRevisionActionTimeUserComment
123311view07:12, 15 July 2022EgonwTyped a datanode (and added missing label)
116655view11:45, 9 May 2021EweitzModified title
101141view21:32, 31 October 2018ReactomeTeamreactome version 65
100669view20:06, 31 October 2018ReactomeTeamreactome version 64
100219view16:51, 31 October 2018ReactomeTeamreactome version 63
99770view15:17, 31 October 2018ReactomeTeamreactome version 62 (2nd attempt)
99328view12:47, 31 October 2018ReactomeTeamreactome version 62
93815view13:38, 16 August 2017ReactomeTeamreactome version 61
93361view11:21, 9 August 2017ReactomeTeamreactome version 61
87138view18:51, 18 July 2016EgonwOntology Term : 'classic metabolic pathway' added !
87136view18:51, 18 July 2016EgonwOntology Term : 'citric acid cycle pathway' added !
86443view09:18, 11 July 2016ReactomeTeamreactome version 56
83385view11:04, 18 November 2015ReactomeTeamVersion54
81567view13:06, 21 August 2015ReactomeTeamVersion53
77032view08:33, 17 July 2014ReactomeTeamFixed remaining interactions
76737view12:10, 16 July 2014ReactomeTeamFixed remaining interactions
76062view10:12, 11 June 2014ReactomeTeamRe-fixing comment source
75772view11:28, 10 June 2014ReactomeTeamReactome 48 Update
75122view14:07, 8 May 2014AnweshaFixing comment source for displaying WikiPathways description
74769view08:51, 30 April 2014ReactomeTeamNew pathway

External references

DataNodes

View all...
NameTypeDatabase referenceComment
(R)-S-LGSHMetaboliteCHEBI:15694 (ChEBI)
2HGMetaboliteCHEBI:32796 (ChEBI)
2HGMetaboliteCHEBI:32797 (ChEBI)
2OGMetaboliteCHEBI:30915 (ChEBI)
ACO2ProteinQ99798 (Uniprot-TrEMBL)
ADHFE1(1-?)ProteinQ8IWW8 (Uniprot-TrEMBL)
ADPMetaboliteCHEBI:16761 (ChEBI)
ATPMetaboliteCHEBI:15422 (ChEBI)
Ac-CoAMetaboliteCHEBI:15351 (ChEBI)
BSG ProteinP35613 (Uniprot-TrEMBL)
BSG:MCTsComplexR-HSA-204396 (Reactome)
CHEBI:28240 (ChEBI)
CITMetaboliteCHEBI:30769 (ChEBI)
CO2MetaboliteCHEBI:16526 (ChEBI)
CS ProteinO75390 (Uniprot-TrEMBL)
CS dimerComplexR-HSA-70973 (Reactome)
Co2+MetaboliteCHEBI:27638 (ChEBI)
CoA-SHMetaboliteCHEBI:15346 (ChEBI)
D2HGDHProteinQ8N465 (Uniprot-TrEMBL)
DCA:PDK2ComplexR-HSA-9011531 (Reactome)
DCAMetaboliteCHEBI:28240 (ChEBI)
DLD ProteinP09622 (Uniprot-TrEMBL)
FAD MetaboliteCHEBI:16238 (ChEBI)
FADMetaboliteCHEBI:16238 (ChEBI)
FADH2MetaboliteCHEBI:17877 (ChEBI)
FAHD1 ProteinQ6P587 (Uniprot-TrEMBL)
FAHD1:Mg2+ dimerComplexR-HSA-9012057 (Reactome)
FH ProteinP07954 (Uniprot-TrEMBL)
FH tetramerComplexR-HSA-451041 (Reactome)
FUMAMetaboliteCHEBI:18012 (ChEBI)
GDPMetaboliteCHEBI:17552 (ChEBI)
GLO1 ProteinQ04760 (Uniprot-TrEMBL)
GLO1 dimer:2xZn2+ComplexR-HSA-5694123 (Reactome)
GSH MetaboliteCHEBI:16856 (ChEBI)
GSHMetaboliteCHEBI:16856 (ChEBI)
GSTZ1 ProteinO43708 (Uniprot-TrEMBL)
GSTZ1 dimerComplexR-HSA-9011584 (Reactome)
GTPMetaboliteCHEBI:15996 (ChEBI)
H+MetaboliteCHEBI:15378 (ChEBI)
H2OMetaboliteCHEBI:15377 (ChEBI)
HAGH-2 ProteinQ16775-2 (Uniprot-TrEMBL)
HAGH-2:2xZn2+ComplexR-HSA-6783206 (Reactome)
HBUTMetaboliteCHEBI:16724 (ChEBI)
HClMetaboliteCHEBI:17883 (ChEBI)
IDH2 ProteinP48735 (Uniprot-TrEMBL)
IDH2 dimerComplexR-HSA-450982 (Reactome)
IDH3 complexComplexR-HSA-70965 (Reactome)
IDH3A ProteinP50213 (Uniprot-TrEMBL)
IDH3B ProteinO43837 (Uniprot-TrEMBL)
IDH3G ProteinP51553 (Uniprot-TrEMBL)
ISCITMetaboliteCHEBI:151 (ChEBI)
Iron Sulphur Cluster R-ALL-113591 (Reactome)
L2HGDHProteinQ9H9P8 (Uniprot-TrEMBL)
LACTMetaboliteCHEBI:422 (ChEBI)
LDH tetramerComplexR-HSA-184549 (Reactome)
LDHA ProteinP00338 (Uniprot-TrEMBL)
LDHAL6A ProteinQ6ZMR3 (Uniprot-TrEMBL)
LDHAL6BProteinQ9BYZ2 (Uniprot-TrEMBL)
LDHB ProteinP07195 (Uniprot-TrEMBL)
LDHC ProteinP07864 (Uniprot-TrEMBL)
LIPAM MetaboliteCHEBI:17460 (ChEBI)
Lipo-K110-DLST ProteinP36957 (Uniprot-TrEMBL)
MALMetaboliteCHEBI:30797 (ChEBI)
MDH2 ProteinP40926 (Uniprot-TrEMBL)
MDH2 dimerComplexR-HSA-198511 (Reactome)
ME1 ProteinP48163 (Uniprot-TrEMBL)
ME1:Mg2+ tetramerComplexR-HSA-9012061 (Reactome)
ME2 ProteinP23368 (Uniprot-TrEMBL)
ME2:Mg2+ tetramerComplexR-HSA-9012264 (Reactome)
ME3 ProteinQ16798 (Uniprot-TrEMBL)
ME3:Mg2+ tetramerComplexR-HSA-9012356 (Reactome)
MGXLMetaboliteCHEBI:17158 (ChEBI)
MPC1 ProteinQ9Y5U8 (Uniprot-TrEMBL)
MPC1:MPC2ComplexR-HSA-2512902 (Reactome)
MPC2 ProteinO95563 (Uniprot-TrEMBL)
Mg2+ MetaboliteCHEBI:18420 (ChEBI)
Mg2+MetaboliteCHEBI:18420 (ChEBI)
Mn2+ MetaboliteCHEBI:29035 (ChEBI)
Mn2+MetaboliteCHEBI:29035 (ChEBI)
NAD+MetaboliteCHEBI:15846 (ChEBI)
NADHMetaboliteCHEBI:16908 (ChEBI)
NADP+MetaboliteCHEBI:18009 (ChEBI)
NADPHMetaboliteCHEBI:16474 (ChEBI)
NNT ProteinQ13423 (Uniprot-TrEMBL)
NNT dimerComplexR-HSA-451008 (Reactome)
OAAMetaboliteCHEBI:30744 (ChEBI)
OGDH ProteinQ02218 (Uniprot-TrEMBL)
PDHA1 ProteinP08559 (Uniprot-TrEMBL)
PDHA2 ProteinP29803 (Uniprot-TrEMBL)
PDHB ProteinP11177 (Uniprot-TrEMBL)
PDHX ProteinO00330 (Uniprot-TrEMBL)
PDK isoformsComplexR-HSA-203947 (Reactome)
PDK1 ProteinQ15118 (Uniprot-TrEMBL)
PDK2(?-407) ProteinQ15119 (Uniprot-TrEMBL)
PDK2(?-407)ProteinQ15119 (Uniprot-TrEMBL)
PDK3(?-406) ProteinQ15120 (Uniprot-TrEMBL)
PDK4(?-411) ProteinQ16654 (Uniprot-TrEMBL)
PDP1 ProteinQ9P0J1 (Uniprot-TrEMBL)
PDP2 ProteinQ9P2J9 (Uniprot-TrEMBL)
PDPR ProteinQ8NCN5 (Uniprot-TrEMBL)
PDPComplexR-HSA-204219 (Reactome)
PPARD ProteinQ03181 (Uniprot-TrEMBL)
PYRMetaboliteCHEBI:32816 (ChEBI)
PiMetaboliteCHEBI:18367 (ChEBI)
RXRA ProteinP19793 (Uniprot-TrEMBL)
RXRA:PPARD:atRAComplexR-HSA-5634107 (Reactome)
Respiratory electron

transport, ATP synthesis by chemiosmotic coupling, and heat production by uncoupling

proteins.
PathwayR-HSA-163200 (Reactome) Oxidation of fatty acids and pyruvate in the mitochondrial matrix yield large amounts of NADH. The respiratory electron transport chain couples the re-oxidation of this NADH to NAD+ to the export of protons from the mitochonrial matrix, generating a chemiosmotic gradient across the inner mitochondrial membrane. This gradient is used to drive the synthesis of ATP; it can also be bypassed by uncoupling proteins to generate heat, a reaction in brown fat that may be important in regulation of body temperature in newborn children.
SDH complex (ox.)ComplexR-HSA-70990 (Reactome)
SDHA ProteinP31040 (Uniprot-TrEMBL)
SDHB ProteinP21912 (Uniprot-TrEMBL)
SDHC ProteinQ99643 (Uniprot-TrEMBL)
SDHD ProteinO14521 (Uniprot-TrEMBL)
SLC16A1 ProteinP53985 (Uniprot-TrEMBL)
SLC16A3 ProteinO15427 (Uniprot-TrEMBL)
SLC16A8 ProteinO95907 (Uniprot-TrEMBL)
SUCC-CoAMetaboliteCHEBI:15380 (ChEBI)
SUCCAMetaboliteCHEBI:15741 (ChEBI)
SUCCSAMetaboliteCHEBI:16265 (ChEBI)
SUCLA2 ProteinQ9P2R7 (Uniprot-TrEMBL)
SUCLA2:SUCLG1ComplexR-HSA-156625 (Reactome)
SUCLG1 ProteinP53597 (Uniprot-TrEMBL)
SUCLG1:SUCLG2ComplexR-HSA-156627 (Reactome)
SUCLG2 ProteinQ96I99 (Uniprot-TrEMBL)
TDP MetaboliteCHEBI:18290 (ChEBI)
VDAC1ProteinP21796 (Uniprot-TrEMBL)
Zn2+ MetaboliteCHEBI:29105 (ChEBI)
Zn2+MetaboliteCHEBI:29105 (ChEBI)
atRA MetaboliteCHEBI:15367 (ChEBI)
glyoxylateMetaboliteCHEBI:16891 (ChEBI)
lipo-K132,K259-DLAT ProteinP10515 (Uniprot-TrEMBL)
lipo-PDHComplexR-HSA-70070 (Reactome)
lipo-aKGDHComplexR-HSA-69996 (Reactome)
p-lipo-PDHComplexR-HSA-210342 (Reactome)

Annotated Interactions

View all...
SourceTargetTypeDatabase referenceComment
(R)-S-LGSHArrowR-HSA-5694071 (Reactome)
(R)-S-LGSHR-HSA-6783221 (Reactome)
2HGArrowR-HSA-880033 (Reactome)
2HGR-HSA-880002 (Reactome)
2HGR-HSA-880007 (Reactome)
2HGR-HSA-880050 (Reactome)
2OGArrowR-HSA-450984 (Reactome)
2OGArrowR-HSA-70967 (Reactome)
2OGArrowR-HSA-880002 (Reactome)
2OGArrowR-HSA-880007 (Reactome)
2OGArrowR-HSA-880050 (Reactome)
2OGR-HSA-71401 (Reactome)
2OGR-HSA-880033 (Reactome)
ACO2mim-catalysisR-HSA-450975 (Reactome)
ACO2mim-catalysisR-HSA-70971 (Reactome)
ADHFE1(1-?)mim-catalysisR-HSA-880002 (Reactome)
ADHFE1(1-?)mim-catalysisR-HSA-880033 (Reactome)
ADPArrowR-HSA-203946 (Reactome)
ADPArrowR-HSA-70967 (Reactome)
ADPR-HSA-70997 (Reactome)
ATPArrowR-HSA-70997 (Reactome)
ATPR-HSA-203946 (Reactome)
ATPTBarR-HSA-9012268 (Reactome)
Ac-CoAArrowR-HSA-203946 (Reactome)
Ac-CoAArrowR-HSA-71397 (Reactome)
Ac-CoAR-HSA-70975 (Reactome)
BSG:MCTsmim-catalysisR-HSA-373867 (Reactome)
BSG:MCTsmim-catalysisR-HSA-373875 (Reactome)
CITArrowR-HSA-450975 (Reactome)
CITArrowR-HSA-70975 (Reactome)
CITR-HSA-70971 (Reactome)
CO2ArrowR-HSA-450984 (Reactome)
CO2ArrowR-HSA-70967 (Reactome)
CO2ArrowR-HSA-71397 (Reactome)
CO2ArrowR-HSA-71401 (Reactome)
CO2ArrowR-HSA-9012016 (Reactome)
CO2ArrowR-HSA-9012036 (Reactome)
CO2ArrowR-HSA-9012268 (Reactome)
CO2ArrowR-HSA-9012349 (Reactome)
CS dimermim-catalysisR-HSA-70975 (Reactome)
Co2+ArrowR-HSA-880007 (Reactome)
CoA-SHArrowR-HSA-70975 (Reactome)
CoA-SHArrowR-HSA-70997 (Reactome)
CoA-SHArrowR-HSA-71775 (Reactome)
CoA-SHR-HSA-71397 (Reactome)
CoA-SHR-HSA-71401 (Reactome)
D2HGDHmim-catalysisR-HSA-880007 (Reactome)
DCA:PDK2ArrowR-HSA-9011543 (Reactome)
DCA:PDK2TBarR-HSA-203946 (Reactome)
DCAR-HSA-9011543 (Reactome)
DCAR-HSA-9011595 (Reactome)
DCATBarR-HSA-9011595 (Reactome)
FADH2ArrowR-HSA-880007 (Reactome)
FADH2ArrowR-HSA-880050 (Reactome)
FADR-HSA-880007 (Reactome)
FADR-HSA-880050 (Reactome)
FAHD1:Mg2+ dimermim-catalysisR-HSA-9012016 (Reactome)
FH tetramermim-catalysisR-HSA-451033 (Reactome)
FH tetramermim-catalysisR-HSA-70982 (Reactome)
FUMAArrowR-HSA-451033 (Reactome)
FUMAArrowR-HSA-70994 (Reactome)
FUMAArrowR-HSA-9012268 (Reactome)
FUMAR-HSA-70982 (Reactome)
GDPR-HSA-71775 (Reactome)
GLO1 dimer:2xZn2+mim-catalysisR-HSA-5694071 (Reactome)
GSHArrowR-HSA-6783221 (Reactome)
GSHArrowR-HSA-9011595 (Reactome)
GSHR-HSA-5694071 (Reactome)
GSTZ1 dimermim-catalysisR-HSA-9011595 (Reactome)
GTPArrowR-HSA-71775 (Reactome)
H+ArrowR-HSA-372342 (Reactome)
H+ArrowR-HSA-373867 (Reactome)
H+ArrowR-HSA-373875 (Reactome)
H+ArrowR-HSA-450971 (Reactome)
H+ArrowR-HSA-450984 (Reactome)
H+ArrowR-HSA-70510 (Reactome)
H+ArrowR-HSA-70967 (Reactome)
H+ArrowR-HSA-70979 (Reactome)
H+ArrowR-HSA-9012036 (Reactome)
H+ArrowR-HSA-9012268 (Reactome)
H+ArrowR-HSA-9012349 (Reactome)
H+R-HSA-372342 (Reactome)
H+R-HSA-373867 (Reactome)
H+R-HSA-373875 (Reactome)
H+R-HSA-450971 (Reactome)
H+R-HSA-6807826 (Reactome)
H+R-HSA-71783 (Reactome)
H+R-HSA-71849 (Reactome)
H2OArrowR-HSA-451033 (Reactome)
H2OR-HSA-204169 (Reactome)
H2OR-HSA-70975 (Reactome)
H2OR-HSA-70982 (Reactome)
H2OR-HSA-9011595 (Reactome)
HAGH-2:2xZn2+mim-catalysisR-HSA-6783221 (Reactome)
HBUTArrowR-HSA-880002 (Reactome)
HBUTR-HSA-880033 (Reactome)
HClArrowR-HSA-9011595 (Reactome)
IDH2 dimermim-catalysisR-HSA-450984 (Reactome)
IDH3 complexmim-catalysisR-HSA-70967 (Reactome)
ISCITArrowR-HSA-70971 (Reactome)
ISCITR-HSA-450975 (Reactome)
ISCITR-HSA-450984 (Reactome)
ISCITR-HSA-70967 (Reactome)
L2HGDHmim-catalysisR-HSA-880050 (Reactome)
LACTArrowR-HSA-373867 (Reactome)
LACTArrowR-HSA-373875 (Reactome)
LACTArrowR-HSA-6783221 (Reactome)
LACTArrowR-HSA-6807826 (Reactome)
LACTArrowR-HSA-71849 (Reactome)
LACTR-HSA-373867 (Reactome)
LACTR-HSA-373875 (Reactome)
LACTR-HSA-70510 (Reactome)
LDH tetramermim-catalysisR-HSA-70510 (Reactome)
LDH tetramermim-catalysisR-HSA-71849 (Reactome)
LDHAL6Bmim-catalysisR-HSA-6807826 (Reactome)
MALArrowR-HSA-70982 (Reactome)
MALArrowR-HSA-71783 (Reactome)
MALR-HSA-451033 (Reactome)
MALR-HSA-70979 (Reactome)
MALR-HSA-9012036 (Reactome)
MALR-HSA-9012268 (Reactome)
MALR-HSA-9012349 (Reactome)
MDH2 dimermim-catalysisR-HSA-70979 (Reactome)
MDH2 dimermim-catalysisR-HSA-71783 (Reactome)
ME1:Mg2+ tetramermim-catalysisR-HSA-9012036 (Reactome)
ME2:Mg2+ tetramermim-catalysisR-HSA-9012268 (Reactome)
ME3:Mg2+ tetramermim-catalysisR-HSA-9012349 (Reactome)
MGXLR-HSA-5694071 (Reactome)
MPC1:MPC2mim-catalysisR-HSA-372342 (Reactome)
Mg2+ArrowR-HSA-204169 (Reactome)
Mn2+ArrowR-HSA-880007 (Reactome)
NAD+ArrowR-HSA-6807826 (Reactome)
NAD+ArrowR-HSA-71783 (Reactome)
NAD+ArrowR-HSA-71849 (Reactome)
NAD+R-HSA-450971 (Reactome)
NAD+R-HSA-70510 (Reactome)
NAD+R-HSA-70967 (Reactome)
NAD+R-HSA-70979 (Reactome)
NAD+R-HSA-71397 (Reactome)
NAD+R-HSA-71401 (Reactome)
NAD+R-HSA-9012268 (Reactome)
NADHArrowR-HSA-203946 (Reactome)
NADHArrowR-HSA-450971 (Reactome)
NADHArrowR-HSA-70510 (Reactome)
NADHArrowR-HSA-70967 (Reactome)
NADHArrowR-HSA-70979 (Reactome)
NADHArrowR-HSA-71397 (Reactome)
NADHArrowR-HSA-71401 (Reactome)
NADHArrowR-HSA-9012268 (Reactome)
NADHR-HSA-6807826 (Reactome)
NADHR-HSA-71783 (Reactome)
NADHR-HSA-71849 (Reactome)
NADP+ArrowR-HSA-450971 (Reactome)
NADP+R-HSA-450984 (Reactome)
NADP+R-HSA-9012036 (Reactome)
NADP+R-HSA-9012349 (Reactome)
NADPHArrowR-HSA-450984 (Reactome)
NADPHArrowR-HSA-9012036 (Reactome)
NADPHArrowR-HSA-9012349 (Reactome)
NADPHR-HSA-450971 (Reactome)
NNT dimermim-catalysisR-HSA-450971 (Reactome)
OAAArrowR-HSA-70979 (Reactome)
OAAR-HSA-70975 (Reactome)
OAAR-HSA-71783 (Reactome)
OAAR-HSA-9012016 (Reactome)
PDK isoformsmim-catalysisR-HSA-203946 (Reactome)
PDK2(?-407)R-HSA-9011543 (Reactome)
PDPmim-catalysisR-HSA-204169 (Reactome)
PYRArrowR-HSA-372342 (Reactome)
PYRArrowR-HSA-70510 (Reactome)
PYRArrowR-HSA-9012016 (Reactome)
PYRArrowR-HSA-9012036 (Reactome)
PYRArrowR-HSA-9012268 (Reactome)
PYRArrowR-HSA-9012349 (Reactome)
PYRArrowR-HSA-9012374 (Reactome)
PYRR-HSA-372342 (Reactome)
PYRR-HSA-6807826 (Reactome)
PYRR-HSA-71397 (Reactome)
PYRR-HSA-71849 (Reactome)
PYRR-HSA-9012374 (Reactome)
PYRTBarR-HSA-203946 (Reactome)
PiArrowR-HSA-204169 (Reactome)
PiR-HSA-70997 (Reactome)
PiR-HSA-71775 (Reactome)
R-HSA-203946 (Reactome) The mitochondrial pyruvate dehydrogenase (PDH) complex (lipo-PDH) irreversibly decarboxylates pyruvate to acetyl CoA, thereby serving to oxidatively remove lactate, which is in equilibrium with pyruvate, and to link glycolysis in the cytosol to the tricarboxylic acid cycle in the mitochondria matrix. Pyruvate Dehydrogenase Kinase (PDK) in the mitochondrial matrix catalyzes the phosphorylation of serine residues of the E1 alpha subunit of the PDH complex, inactivating it. Pyruvate negatively regulates this reaction, and NADH and acetyl CoA positively regulate it (Bao et al. 2004). Four PDK isoforms have been identified and shown to catalyze the phosphorylation of E1 alpha in vitro (Gudi et al. 1995, Kolobova et al. 2001, Rowles et al. 1996). They differ in their expression patterns and quantitative responses to regulatory small molecules. All four isoforms catalyze the phosphorylation of serine residues 293 ("site 1") and 300 ("site 2"); PDK1 can also catalyse the phosphorylation of serine 232 ("site 3"). Phosphorylation of a single site in a single E1 alpha subunit is sufficient for enzyme inactivation (Bowker-Kinley et al. 1998, Gudi et al. 1995, Kolobova et al. 2001, Korotchkina and Patel, 2001).
R-HSA-204169 (Reactome) Pyruvate dehydrogenase phosphatase (PDP) in the mitochondrial matrix catalyzes the hydrolytic removal of phosphate groups from phosphoserine residues in the E1 alpha subunit of the pyruvate dehydrogenase complex. The active form of PDP is a heterodimer of a catalytic subunit and a regulatory one. Two isoforms of the catalytic subunit have been identified and biochemically characterized (Huang et al. 1998) and mutations in PDP1 have been associated with PDP deficiency in vivo (Maj et al. 2005). The properties of the human regulatory subunit have been deduced from those of its bovine homologue (Lawson et al. 1997). The activity of PDP1 is greatly enhanced through Ca2+ -dependent binding of the catalytic subunit (PDP1c) to the L2 (inner lipoyl) domain of dihydrolipoyl acetyltransferase (E2), which is also integrated in the pyruvate dehydrogenase complex. PDP activity requires Mg2+ (Huang et al. 1998).
R-HSA-372342 (Reactome) Pyruvate (PYR) and a proton (H+) are cotransported from the mitochondrial intermembrane space to the mitochondrial matrix, mediated by a complex of mitochondrial pyruvate carriers 1 and 2 (MCP1 and MCP2) located in the inner mitochondrial membrane (McCommis & Finck 2015). The proton gradient across the inner mitochondrial membrane must be maintained for ATP production to occur. Transport of PYR across this membrane would collapse this gradient therefore PYR is cotransported with H+. Studies of pyruvate uptake in rat indicate that it is specific, saturable, and competitively inhibitable, indicating a specific role for a membrane transport protein (Papa et al. 1971, Halestrap & Denton 1974), and the stoichiometry of the human reaction is inferred from this work. MCP1 and MCP2 have been identified as essential components of the transporter based on the observation that expression of both proteins (but not either one alone) restored mitochondrial pyruvate uptake in mutant budding yeast. The proteins form a multimeric complex; its stoichiometry is unknown (Bricker et al. 2012).
R-HSA-373867 (Reactome) The membrane-associated MCT:basigin complex mediates the reversible uptake of extracellular lactate and H+ (Wilson et al. 2005).
R-HSA-373875 (Reactome) The membrane-associated MCT:basigin complex mediates the reversible export of cytosolic lactate and H+ (Wilson et al. 2005).
R-HSA-450971 (Reactome) NNT (nicotinamide nucleotide transhydrogenase) associated with the inner mitochondrial membrane catalyzes the reaction of mitochondrial NADPH and NAD+ to form NADP+ and NADH. The reaction is coupled to the translocation of a proton across the inner mitochondrial membrane into the mitochondrial matrix (White et al, 2000). The active form of NNT is inferred to be a homodimer based on the known structure of its bovine homolog (Yamaguchi and Hatefi 1991).
R-HSA-450975 (Reactome) Mitochondrial aconitase reversibly converts isocitrate to citrate via a cis-aconitate intermediate. Mitochondrial aconitase activity has been demonstrated in diverse human tissue extracts (Slaughter et al. 1975) and a protein homologous to the well-characterized porcine enzyme has been purified from human tissues (Baldwin et al. 1991).
R-HSA-450984 (Reactome) Mitochondrial isocitrate dehydrogenase IDH2 catalyzes the irreversible reaction of isocitrate and NADP+ to form alpha ketoglutarate, CO2, and NADPH + H+ (Hartong et al. 2008). The structure of the active human enzyme has not been determined experimentally, but is inferred to be a homodimer with one Mn++ bound to each subunit based on detailed studies of the homologous pig enzyme (Ceccarelli et al. 2002). NADP-specific IDH2 was the first isocitrate dehydrogenase isoenzyme to be characterized in biochemical studies of the mammalian TCA cycle (Ochoa 1948). Later work with yeast revealed the existence of both NADP-specific (IDH2-homologous) and NAD-specific (IDH3-homologous) enzymes and demonstrated the ADP-dependence of the latter (Kornberg and Pricer 1951), consistent with the now widely accepted view that IDH3 mediates the conversion of isocitrate to alpha-ketoglutarate in the TCA cycle. The physiological function of IDH2 is thus unclear. The recent observation that individuals homozygous for IDH3 mutations that sharply reduce its activity do not show symptoms of deficient energy metabolism in most tissues raises the possibility that the IDH2 reaction may play an accessory role in the TCA cycle (Hartong et al. 2008).
R-HSA-451033 (Reactome) Mitochondrial fumarate hydratase catalyzes the reversible reaction of malate to form fumarate and water (Bourgeron et al. 1994). Unpublished crystallographic data indicate that the protein is a tetramer (PDB 3E04).
R-HSA-5694071 (Reactome) Lactoylglutathione lyase (GLO1) catalyses the transformation of methylglyoxal (MGXL) and glutathione (GSH) to (R)-S-lactoylglutathione ((R)-S-LGSH), an intermediate in pyruvate metabolism. MGXL is a reactive 2-oxoaldehyde byproduct of normal metabolism that is a carcinogen and a mutagen (Ridderstrom et al. 1998). This is the first step in the glyoxalase system, a critical two-step detoxification system for MGXL.
R-HSA-6783221 (Reactome) In the second step of the glyoxalase system, hydroxyacylglutathione hydrolase (HAGH) catalyses the hydrolysis of (R)-S-lactoylglutathione ((R)-S-LGSH) to glutathione (GSH) and lactic acid (LACT) (Ridderstrom et al. 1996). The HAGH gene can produce two forms of the protein, form 1 is mitochondrial whereas form 2 is cytosolic (Cordell et al. 2004). HAGH is monomeric but requires two Zn2+ ions for activity (Cameron et al. 1999). This reaction completes the detoxification of methylglyoxal, a reactive byproduct of pyruvate metabolism.
R-HSA-6807826 (Reactome) LDHAL6B (L-lactate dehydrogenase A-like 6B) catalyzes the reaction of PYR (pyruvate) and NADH + H+ to form LACT (lactate) and NAD+. The LDHAL6B protein is the inferred product of an open reading frame transcribed in the testis (Wang et al. 2005). Its mitochondrial localization is inferred from the presence of a mitochondrial localization sequence at its amino terminus (Holmes and Goldberg 2009). A physiological role for lactate formation from the abundant pyruvate and NADH expected in rapidly respiring mitochondria is not straightforward to imagine, however.
R-HSA-70510 (Reactome) Cytosolic lactate dehydrogenase catalyzes the freely reversible reaction of lactate and NAD+ to form pyruvate and NADH + H+. In liver parenchymal cells, this reaction allows lactate from red blood cells and exercising muscle to be converted to pyruvate which in turn is typically used for gluconeogenesis which also consumes the NADH from the reaction.

Lactate dehydrogenase is active as a tetramer. Two isoforms of lactate dehydrogenase, A and B, are widely expressed in human tissues, and all five tetramers - A4, A3B, A2B2, AB3, and B4 - are found (Read et al. 2001; Sakai et al. 1987; Yu et al. 2001). A third isoform, C, and its tetramer, C4, are found in testis (Millan et al. 1987; LeVan & Goldberg 1991). A fourth isoform, LDHAL6A, is less fully characterized than these others but limited data suggest that it may be testis-specific (Chen et al. 2009).

R-HSA-70967 (Reactome) Mitochondrial isocitrate dehydrogenase IDH3 catalyzes the irreversible reaction of isocitrate and NAD+ to form alpha ketoglutarate, CO2, and NADH + H+. The enzyme is a heteromer containing four polypeptide chains, two IDH3A, one IDH3B, and one IDH3G, and two Mn++ (Dange and Colman 2010). It is activated by ADP (Soundar et al. 2003, 2006; Bzymek and Colman 2007). This is the first of four oxidation reactions in the citric acid cycle, and the first decarboxylation.
R-HSA-70971 (Reactome) Mitochondrial aconitase reversibly converts citrate to isocitrate via a cis-aconitate intermediate. Mitochondrial aconitase activity has been demonstrated in diverse human tissue extracts (Slaughter et al. 1975) and a protein homologous to the well-characterized porcine enzyme has been purified from human tissues (Baldwin et al. 1991).
R-HSA-70975 (Reactome) Mitochondrial citrate synthase dimer catalyzes the irreversible reaction of acetyl-CoA, water, and oxaloacetate to form citrate and coenzyme A. This reaction is the entry point of two-carbon units into the citric acid cycle. The reaction is subject to allosteric regulation. The gene encoding the human enzyme has been cloned (Goldenthal et al. 1998), but the enzyme has not been characterized in detail - its properties are inferred from those of the well-studied homologous pig enzyme (e.g., Morgunov and Srere 1998).
R-HSA-70979 (Reactome) Mitochondrial malate dehydrogenase catalyzes the reversible reaction of malate and NAD+ to form oxaloacetate and NADH + H+ (Luo et al. 2006). This reaction is highly endergonic but is pulled in the direction annotated here when the TCA cycle is operating. Unpublished crystallographic data indicate that the protein is a dimer (PDB 3E04).
R-HSA-70982 (Reactome) Mitochondrial fumarate hydratase catalyzes the reversible reaction of fumarate and water to form malate, the seventh step of the TCA cycle (Bourgeron et al. 1994). Unpublished crystallographic data indicate that the protein is a tetramer (PDB 3E04).
R-HSA-70994 (Reactome) The succinate dehydrogenase complex, associated with the inner mitochondrial membrane, catalyzes the dehydrogenation of succinate to fumarate, reducing the FAD cofactor bound to the enzyme. This redox potential is then used in the electron transfer chain to drive a proton motive force to generate ATP.
R-HSA-70997 (Reactome) Mitochondrial succinate CoA ligase (ADP-forming) catalyzes the reversible conversion of succinyl CoA to succinate plus Coenzyme A, coupled to the conversion of ADP and orthophosphate to ATP. The enzyme is a heterodimer containing SUCLG1 and SUCLA2 monomers.

The enzyme catalyzing the reaction in vertebrates is a heterodimer that occurs in two isoforms. The enzymes have been purified from pigeon and rat tissue and characterized in detail. Both isoforms, an alpha:betaA heterodimer and an alpha:betaG heterodimer, catalyze the reversible conversion of succinyl CoA to succinate plus Coenzyme A. The alpha:betaA heterodimer couples this conversion to the synthesis of ATP from ADP and orthophosphate, while the alpha:betaG heterodimer couples it to the synthesis of GTP from GDP and orthophosphate (Johnson et al. 1998a,b; Lambeth et al. 2004). Consistent with these results in model systems, patients homozygous for a mutant allele of the gene encoding the ADP enzyme beta subunit, SUCLA2, are deficient in succinyl CoA ligase activity (Elpeleg et al. 2005).

Both isoforms are found in vivo, and appear to be expressed at different levels in various tissues. Their relative contributions to the flux of carbon atoms through the TCA cycle are unknown. Genetic and biochemical data suggest that the alpha:betaA isoform may be required to catalyze the reverse reaction, conversion of succinate, Coenzyme A, and ATP to succinyl CoA, ADP, and orthophosphate for heme biosynthesis (Furuyama and Sassa 2000).

R-HSA-71397 (Reactome) The mitochondrial pyruvate dehydrogenase complex catalyzes the reaction of pyruvate, CoASH, and NAD+ to form acetylCoA, CO2, and NADH. The enzyme complex contains multiple copies of three different proteins, E1 alpha, E1 beta, E2, and E3, each with distinct catalytic activities (Reed and Hackert 1990; Zhou et al 2001). The reaction starts with the oxidative decarboxylation of pyruvate catalyzed by E1 alpha and beta (pyruvate dehydrogenase). Lipoamide cofactor associated with E1 is reduced at the same time. Next, the acetyl group derived from pyruvate is transferred to coenzyme A in two steps catalyzed by E2 (dihydrolipolyl transacetylase). Finally, the oxidized form of lipoamide is regenerated and electrons are transferred to NAD+ in two steps catalyzed by E3 (dihydrolipoyl dehydrogenase). The biochemical details of this reaction have been worked out with pyruvate dehydrogenase complex and subunits purified from bovine tissue and other non-human sources. Direct evidence for the roles of the corresponding human proteins comes from studies of patients expressing mutant forms of E1 alpha (Lissens et al. 2000), E1 beta (Brown et al. 2004), E2 (Head et al. 2005), and E3 (Brautigam et al. 2005).
R-HSA-71401 (Reactome) The mitochondrial alpha-ketoglutarate dehydrogenase complex catalyzes the reaction of alpha-ketoglutarate, CoASH, and NAD+ to form succinyl-CoA, CO2, and NADH. The enzyme complex contains multiple copies of three different proteins, E1 (OGDH), E2 (DLST), and E3 (DLD), each with distinct catalytic activities (Reed and Hackert 1990; Zhou et al 2001). The reaction starts with the oxidative decarboxylation of alpha ketoglutarate catalyzed by E1alpha and beta (alpha ketoglutarate dehydrogenase). Lipoamide cofactor associated with E1 is reduced at the same time. Next, the succinyl group derived from alpha ketoglutarate is transferred to coenzyme A in two steps catalyzed E2 (dihydrolipolyl transacetylase). Finally, the oxidized form of lipoamide is regenerated and electrons are transferred to NAD+ in two steps catalyzed by E3 (dihydrolipoyl dehydrogenase). The biochemical details of this reaction have been worked out with alpha ketoglutarate dehydrogenase complex and subunits purified from bovine tissue (McCartney et al. 1998). While all of the human proteins are known as predicted protein products of cloned genes, direct experimental evidence for their functions is available only for E3 (DLD) (Brautigam et al. 2005).
R-HSA-71775 (Reactome) Mitochondrial succinate CoA ligase (ADP-forming) catalyzes the reversible conversion of succinyl CoA to succinate plus Coenzyme A, coupled to the conversion of ADP and orthophosphate to ATP. The enzyme is a heterodimer containing SUCLG1 and SUCLA2 monomers.

The enzyme catalyzing the reaction in vertebrates is a heterodimer that occurs in two isoforms. The enzymes have been purified from pigeon and rat tissue and characterized in detail. Both isoforms, an alpha:betaA heterodimer and an alpha:betaG heterodimer, catalyze the reversible conversion of succinyl CoA to succinate plus Coenzyme A. The alpha:betaA heterodimer couples this conversion to the synthesis of ATP from ADP and orthophosphate, while the alpha:betaG heterodimer couples it to the synthesis of GTP from GDP and orthophosphate (Johnson et al. 1998a,b; Lambeth et al. 2004). Consistent with these results in model systems, patients homozygous for a mutant allele of the gene encoding the ADP enzyme beta subunit, SUCLA2, are deficient in succinyl CoA ligase activity (Elpeleg et al. 2005).

Both isoforms are found in vivo, and appear to be expressed at different levels in various tissues. Their relative contributions to the flux of carbon atoms through the TCA cycle are unknown. Genetic and biochemical data suggest that the alpha:betaA isoform may be required to catalyze the reverse reaction, conversion of succinate, Coenzyme A, and ATP to succinyl CoA, ADP, and orthophosphate for heme biosynthesis (Furuyama and Sassa 2000).

R-HSA-71783 (Reactome) Mitochondrial malate dehydrogenase catalyzes the reversible reaction of oxaloacetate and NADH + H+ to form malate and NAD+ (Luo et al. 2006). Unpublished crystallographic data indicate that the protein is a dimer (PDB 3E04).
R-HSA-71849 (Reactome) Cytosolic lactate dehydrogenase (LDH) catalyzes the freely reversible reaction of pyruvate (PYR) and NADH + H+ to form lactate (LACT) and NAD+. In liver parenchymal cells, this reaction allows lactate from red blood cells and exercising muscle to be converted to pyruvate which in turn is typically used for gluconeogenesis which also consumes the NADH from the reaction.

Lactate dehydrogenase is active as a tetramer. Two isoforms of lactate dehydrogenase, A and B, are widely expressed in human tissues, and all five tetramers - A4, A3B, A2B2, AB3, and B4 - are found (Read et al. 2001; Sakai et al. 1987; Yu et al. 2001). A third isoform, C, and its tetramer, C4, are found in testis (Millan et al. 1987; LeVan & Goldberg 1991). A fourth isoform, LDHAL6A, is less fully characterized than these others but limited data suggest that it may be testis-specific (Chen et al. 2009).

R-HSA-880002 (Reactome) ADHFE1 catalyzes the reversible reaction of (R)-2-hydroxyglutarate and succinate semialdehyde to form 2-oxoglutarate and 4-hydroxybutyrate (Struys et al. 2005). The localization of human ADHFE1 to the mitochondrial matrix is inferred from the location determined experimentally for its rat homolog (Kaufman et al. 1988).
R-HSA-880007 (Reactome) D2HDGH associated with the mitochondrial inner membrane catalyzes the FAD-dependent reaction of (R)-2-hydroxyglutarate to form 2-oxoglutarate (Achouri et al. 2004). D2HDGH mutations are associated with high levels of (R)-2-hydroxyglutarate in vivo and variable neurological symptoms (Struys et al. 2005; Wanders and Mooyer 1995)).
R-HSA-880033 (Reactome) ADHFE1 catalyzes the reversible reaction of 2-oxoglutarate and 4-hydroxybutyrate to form (R)-2-hydroxyglutarate and succinate semialdehyde (Struys et al. 2005). The localization of human ADHFE1 to the mitochondrial matrix is inferred from the location determined experimentally for its rat homolog (Kaufman et al. 1988).
R-HSA-880050 (Reactome) L2HDGH associated with the mitochondrial inner membrane catalyzes the FAD-dependent reaction of (S)-2-hydroxyglutarate to form 2-oxoglutarate (Rzem et al. 2006). L2HDGH mutations are associated with high levels of (S)-2-hydroxyglutarate in vivo and variable neurological symptoms (Rzem et al. 2004; Topcu et al. 2004).
R-HSA-9011543 (Reactome) Of the four human pyruvate dehydrogenase kinases (PDKs), PDK2 is the most ubiquitously expressed kinase and is most susceptible to inhibition by the drug dichloroacetate (DCA), an acid salt analogue of acetic acid. DCA binds to a hydrophobic pocket in the N-terminal domain of PDK2 and, in the presence of ADP, disrupts the binding of the kinase to the lipoyl (E2) domain of the pyruvate dehydrogenase complex (Klyuyeva et al. 2007, Li et al. 2009, Roche et al. 2001).
R-HSA-9011595 (Reactome) In the liver, dimeric glutathione S-transferase zeta 1 (GSTZ1 dimer, aka maleylacetoacetate isomerase, MAAI) mediates the dechlorination of the drug dichloroacetate (DCA) to glyoxylate (Ammini & Stacpoole 2003, Stacpoole et al. 1998, 2008). GSTZ1 is primarily found both in the cytosol and mitochondria (Li et al. 2011). Glyoxylate, the primary metabolite of DCA metabolism, is ultimately converted to oxalate and glycine. The reaction requires (but does not consume) glutathione (GSH). GSTZ1 also catalyses the penultimate step in tyrosine catabolism, thus avoiding the accumulation of toxic tyrosine intermediates. DCA inhibits its own metabolism apparently by a post-translationally mediated inhibition of hepatic GSTZ1 (Stacpoole et al. 1998). GSTZ1 inhibition can cause the build-up of tyrosine intermediates which are able to form protein adducts. Chronic administration of DCA in adult rodents, dogs and some humans causes reversible peripheral neuropathy and hepatotoxicity, possibly because of these reactive tyrosine intermediates (Stacpoole et al. 1998, James et al. 2017). The rate of GSTZ1 inactivation by DCA is influenced by age, GSTZ1 haplotype and cellular chloride concentration (Shroads et al. 2008, 2012, 2015, Jahn et al. 2016, James et al. 2017).
R-HSA-9012016 (Reactome) Fumarylacetoacetate hydrolase domain containing protein 1 (FAHD1) (Pircher et al. 2011, 2015, Jansen-Duerr et al. 2016) was identified to display a bi-functional catalytic mechanism (Weiss et al. 2018), being able to hydrolyse acylpyruvates (Pircher et al. 2011) similar to fumarylpyruvate hydrolase NagK of Ralstonia sp. (acetylpyruvate: vmax = 0,135 µmol/min/mg, KM = 4,6 µM), and to cleave oxaloacetate (OAA) via decarboxylation (Pircher et al. 2015) (OAA: vmax = 0,21 µmol/min/mg, KM = 32 µM). The enzyme is of dimeric form (Manjasetty et al. 2004) and uses Mg2+ or Mn2+ as cofactor. It is localized in the mitochondrial matrix (Pircher et al. 2011, Trukhina et al. 2002, Di Berardino et al. 1996). Its identification as ODx (Pircher et al. 2015) renders FAHD1 a possible antagonist to pyruvate carboxylase (PC) at a central position in the TCA cycle(Jansen-Duerr et al. 2016). It is believed that the ability of FAHD1 to decarboxylate OAA provides the basis of its requirement for maintaining healthy mitochondria in certain cells and tissues (Taferner et al. 2015, Petit et al. 2017). However, further studies of this topic are warranted.
R-HSA-9012036 (Reactome) One hallmark of cancer is altered cellular metabolism. Malic enzymes (MEs) are a family of homotetrameric enzymes that catalyse the reversible oxidative decarboxylation of L-malate to pyruvate, with a simultaneous reduction of NAD(P)+ to NAD(P)H. As MEs generate NADPH and NADH, they may play roles in energy production and reductive biosynthesis. Humans possess three ME isoforms; ME1 is cytosolic and utilises NADP+, ME3 is mitochondrial and can utilise NADP+ and ME2 is mitochondrial and can utililse either NAD+ or NADP+ (Chang & Tong 2003, Murugan & Hung 2012).

NADP-dependent malic enzyme (ME1, aka c-NADP-ME) is a cytosolic enzyme that oxidatively decarboxylates (s)-malate (MAL) to pyruvate (PYR) and CO2 using NADP+ as cofactor (Zelewski & Swierczynski 1991). ME1 exists as a dimer of dimers (Murugan & Hung 2012, Hsieh et al. 2014) and a divalent metal such as Mg2+ is essential for catalysis (Chang & Tong 2003).
R-HSA-9012268 (Reactome) One hallmark of cancer is altered cellular metabolism. Malic enzymes (MEs) are a family of homotetrameric enzymes that catalyse the reversible oxidative decarboxylation of L-malate to pyruvate, with a simultaneous reduction of NAD(P)+ to NAD(P)H. As MEs generate NADPH and NADH, they may play dual roles in energy production and reductive biosynthesis. Humans possess three ME isoforms; ME1 is cytosolic and utilises NADP+, ME3 is mitochondrial and can utilise NADP+ and ME2 is mitochondrial and can utililse either NAD+ or NADP+ (Chang & Tong 2003).

Mitochondrial NAD-dependent malic enzyme (ME2, aka m-NAD(P)-ME) oxidatively decarboxylates (s)-malate (MAL) to pyruvate (PYR) and CO2 using NAD+ (or NADP+) as cofactor (Loeber et al. 1991, Tao et al. 2003). ME2 exists as a dimer of dimers and requires a divalent metal such as Mg2+ for catalysis (Chang & Tong 2003, Murugan & Hung 2012). Unlike the other MEs, ME2's enzymatic activity can be allosterically activated by fumarate (FUMA) and inhibited by ATP (Yang et al. 2002). ME2 could play a critical role in cutaneous melanoma progression, the most life-threatening neoplasm of the skin. Targeting ME2 could be a novel approach to inhibiting melanoma cell proliferation and growth (Chang et al. 2015). ME2 has also been demonstrated to be involved in glioblastoma multiforme (GBM) growth, invasion and migration. Inhibition of ME2 could potentially be therapeutic in the treatment of GBM (Cheng et al. 2016).
R-HSA-9012349 (Reactome) One hallmark of cancer is altered cellular metabolism. Malic enzymes (MEs) are a family of homotetrameric enzymes that catalyse the reversible oxidative decarboxylation of L-malate to pyruvate, with a simultaneous reduction of NAD(P)+ to NAD(P)H. As MEs generate NADPH and NADH, they may play roles in energy production and reductive biosynthesis. Humans possess three ME isoforms; ME1 is cytosolic and utilises NADP+, ME3 is mitochondrial and can utilise NADP+ and ME2 is mitochondrial and can utililse either NAD+ or NADP+ (Chang & Tong 2003, Murugan & Hung 2012).

NADP-dependent malic enzyme (ME3, aka m-NADP-ME) is a mitochondrial enzyme that oxidatively decarboxylates (s)-malate (MAL) to pyruvate (PYR) and CO2 using NADP+ as cofactor (Loeber et al. 1994). ME1 exists as a dimer of dimers (Murugan & Hung 2012) and a divalent metal such as Mg2+ is essential for catalysis (Chang & Tong 2003). ME3 may play a role in insulin secretion (Hasan et al. 2015) but how it does this in panceratic beta cells has not been established yet.
R-HSA-9012374 (Reactome) Similar to other ions and metabolites, pyruvate (PYR) probably crosses the outer mitochondrial membrane through the relatively non-specific, voltage-dependent anion-selective channel protein 1 (VDAC1) (McCommis & Finck 2015). Humans with defective VDAC1 show impaired PYR oxidation and ATP production (Huizing et al. 1996).
RXRA:PPARD:atRAArrowR-HSA-203946 (Reactome)
SDH complex (ox.)mim-catalysisR-HSA-70994 (Reactome)
SUCC-CoAArrowR-HSA-71401 (Reactome)
SUCC-CoAR-HSA-70997 (Reactome)
SUCC-CoAR-HSA-71775 (Reactome)
SUCCAArrowR-HSA-70997 (Reactome)
SUCCAArrowR-HSA-71775 (Reactome)
SUCCAR-HSA-70994 (Reactome)
SUCCSAArrowR-HSA-880033 (Reactome)
SUCCSAR-HSA-880002 (Reactome)
SUCLA2:SUCLG1mim-catalysisR-HSA-70997 (Reactome)
SUCLG1:SUCLG2mim-catalysisR-HSA-71775 (Reactome)
VDAC1mim-catalysisR-HSA-9012374 (Reactome)
Zn2+ArrowR-HSA-880007 (Reactome)
glyoxylateArrowR-HSA-9011595 (Reactome)
lipo-PDHArrowR-HSA-204169 (Reactome)
lipo-PDHR-HSA-203946 (Reactome)
lipo-PDHmim-catalysisR-HSA-71397 (Reactome)
lipo-aKGDHmim-catalysisR-HSA-71401 (Reactome)
p-lipo-PDHArrowR-HSA-203946 (Reactome)
p-lipo-PDHR-HSA-204169 (Reactome)
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