Signaling by retinoic acid (Homo sapiens)

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9, 17, 22, 4427, 324, 6, 33, 5113, 55, 5739477, 153, 11, 50, 512010, 25, 44, 491916, 23, 4522, 39, 464, 6, 33, 515, 26, 36, 4827, 323, 11, 50, 518, 14, 19, 24, 34...21, 29, 37, 38, 565213, 55, 571, 13, 30, 40-42, 53endoplasmic reticulum lumenmitochondrial intermembrane spacecytosolmitochondrial matrixnucleoplasmRARG atRA RDH10,16,DHRS9,RDHE2RXRG DHRS9 NADP+DHRS3 TDP DLD PPARD ALDH1A1 SUMO-K102-CRABP2 DLD RDH11 CPT1A,BPDK isoformsDCA:PDK2atRA ADH1C DHRS4 CYP26C1PDHB NAD+ALDH1A2 SUMO-CRABP1:atRAPYRRARB atRA NADPHatRAH+RARG RARB NADHZn2+ p-lipo-PDHRDH5(24-318) ATPH2OO2PDHA1 NADPHlipo-K132,K259-DLAT ADH4 RXRA:PPARDALDH8A1FABP5 H+NADHADH1A PALM-CoARAR:RXR11cROLPhase II -Conjugation ofcompoundsRDHE2 RXRB RXRB PPARD AKR1C3H+PDK1 NAD+O2atRALCYP26C1 SUMO-K102-CRABP2PDHB TDP RARB FABP5RDH5(24-318), RDH11FABP5 H+FABP5:atRAPPARD p-S21-RXRA atROLSUMO-K-CRABP1SUMO-K102-CRABP2PDHA2 SUMO-K102-CRABP2 p-S21-RXRA SUMO-K102-CRABP2:atRAp-S21-RXRA SUMO2-K166,177,399-p-S219,269-RARA CYP26A1 CYP26A1,B1,C1ADPH2ONADP+11cRALCYP26B1 PDK2(?-407) FABP5ADH1A,1C,4 dimersRXRG atRA atRALPDHA2 RXRA atRA L-PCARNatRA SUMO-K102-CRABP2:atRAPDK3(?-406) atRA:RAR:RXRRDH13NADHSUMO-K102-CRABP2 PDHX RXRA Ac-CoAlipo-PDHRXRA FABP5:atRARXRA:PPARD:atRA:FABP5SUMO-K-CRABP1 atROLRXRB 4OH-atRACoA-SHALDH1A3 NAD+Mal-CoACARRARG RDH10 PDHX SUMO2-K166,177,399-p-S219,269-RARA RXRA:PPARD:atRARDH11,14,DHRS3,DHRS4atRA SUMO-CRABP2:atRA:RAR:RXRNADP+PDK4(?-411) ALDH1A1,2,3tetramers9cRALH+NADPHCPT1B RDH16 atRA H+NADHRDH14 RXRG PDHA1 atRA NAD+lipo-K132,K259-DLAT FAD H2ORDH11 FABP5 CPT1A 9cRASUMO2-K166,177,399-p-S219,269-RARA 4OH-9cRAFAD NADH111231, 541131, 542, 28, 31, 541118182, 28, 31, 5435


Description

Vitamin A (retinol) can be metabolised into active retinoid metabolites that function either as a chromophore in vision or in regulating gene expression transcriptionally and post-transcriptionally. Genes regulated by retinoids are essential for reproduction, embryonic development, growth, and multiple processes in the adult, including energy balance, neurogenesis, and the immune response. The retinoid used as a cofactor in the visual cycle is 11-cis-retinal (11cRAL). The non-visual cycle effects of retinol are mediated by retinoic acid (RA), generated by two-step conversion from retinol (Napoli 2012). All-trans-retinoic acid (atRA) is the major activated metabolite of retinol. An isomer, 9-cis-retinoic acid (9cRA) has biological activity, but has not been detected in vivo, except in the pancreas. An alternative route involves BCO1 cleavage of carotenoids into retinal, which is then reduced into retinol in the intestine (Harrison 2012). The two isomers of RA serve as ligands for retinoic acid receptors (RAR) that regulate gene expression. (Das et al. 2014). RA is catabolised to oxidised metabolites such as 4-hydroxy-, 18-hydroxy- or 4-oxo-RA by CYP family enzymes, these metabolites then becoming substrates for Phase II conjugation enzymes (Ross & Zolfaghari 2011). View original pathway at Reactome.

Comments

Reactome-Converter 
Pathway is converted from Reactome ID: 5362517
Reactome-version 
Reactome version: 75
Reactome Author 
Reactome Author: Jassal, Bijay

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Bibliography

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History

View all...
CompareRevisionActionTimeUserComment
129749view01:58, 22 May 2024EweitzModified title
114702view16:18, 25 January 2021ReactomeTeamReactome version 75
113147view11:21, 2 November 2020ReactomeTeamReactome version 74
112377view15:31, 9 October 2020ReactomeTeamReactome version 73
101716view14:53, 1 November 2018DeSlOntology Term : 'retinoic acid signaling pathway' added !
101280view11:16, 1 November 2018ReactomeTeamreactome version 66
100817view20:47, 31 October 2018ReactomeTeamreactome version 65
100358view19:22, 31 October 2018ReactomeTeamreactome version 64
100270view16:57, 31 October 2018ReactomeTeamNew pathway

External references

DataNodes

View all...
NameTypeDatabase referenceComment
11cRALMetaboliteCHEBI:16066 (ChEBI)
11cROLMetaboliteCHEBI:16302 (ChEBI)
4OH-9cRAMetaboliteCHEBI:63802 (ChEBI)
4OH-atRAMetaboliteCHEBI:63795 (ChEBI)
9cRAMetaboliteCHEBI:50648 (ChEBI)
9cRALMetaboliteCHEBI:78273 (ChEBI)
ADH1A ProteinP07327 (Uniprot-TrEMBL)
ADH1A,1C,4 dimersComplexR-HSA-5362706 (Reactome)
ADH1C ProteinP00326 (Uniprot-TrEMBL)
ADH4 ProteinP08319 (Uniprot-TrEMBL)
ADPMetaboliteCHEBI:456216 (ChEBI)
AKR1C3ProteinP42330 (Uniprot-TrEMBL)
ALDH1A1 ProteinP00352 (Uniprot-TrEMBL)
ALDH1A1,2,3 tetramersComplexR-HSA-5362725 (Reactome)
ALDH1A2 ProteinO94788 (Uniprot-TrEMBL)
ALDH1A3 ProteinP47895 (Uniprot-TrEMBL)
ALDH8A1ProteinQ9H2A2 (Uniprot-TrEMBL)
ATPMetaboliteCHEBI:30616 (ChEBI)
Ac-CoAMetaboliteCHEBI:15351 (ChEBI)
CARMetaboliteCHEBI:17126 (ChEBI)
CPT1A ProteinP50416 (Uniprot-TrEMBL)
CPT1A,BComplexR-HSA-549205 (Reactome)
CPT1B ProteinQ92523 (Uniprot-TrEMBL)
CYP26A1 ProteinO43174 (Uniprot-TrEMBL)
CYP26A1,B1,C1ComplexR-HSA-5362528 (Reactome)
CYP26B1 ProteinQ9NR63 (Uniprot-TrEMBL)
CYP26C1 ProteinQ6V0L0 (Uniprot-TrEMBL)
CYP26C1ProteinQ6V0L0 (Uniprot-TrEMBL)
CoA-SHMetaboliteCHEBI:15346 (ChEBI)
DCA
DCA:PDK2ComplexR-HSA-9011531 (Reactome)
DHRS3 ProteinO75911 (Uniprot-TrEMBL)
DHRS4 ProteinQ9BTZ2 (Uniprot-TrEMBL)
DHRS9 ProteinQ9BPW9 (Uniprot-TrEMBL)
DLD ProteinP09622 (Uniprot-TrEMBL)
FABP5 ProteinQ01469 (Uniprot-TrEMBL)
FABP5:atRAComplexR-HSA-5622128 (Reactome)
FABP5:atRAComplexR-HSA-5633258 (Reactome)
FABP5ProteinQ01469 (Uniprot-TrEMBL)
FAD MetaboliteCHEBI:16238 (ChEBI)
H+MetaboliteCHEBI:15378 (ChEBI)
H2OMetaboliteCHEBI:15377 (ChEBI)
L-PCARNMetaboliteCHEBI:17490 (ChEBI)
Mal-CoAMetaboliteCHEBI:15531 (ChEBI)
NAD+MetaboliteCHEBI:57540 (ChEBI)
NADHMetaboliteCHEBI:57945 (ChEBI)
NADP+MetaboliteCHEBI:18009 (ChEBI)
NADPHMetaboliteCHEBI:16474 (ChEBI)
O2MetaboliteCHEBI:15379 (ChEBI)
PALM-CoAMetaboliteCHEBI:15525 (ChEBI)
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)
PDK3(?-406) ProteinQ15120 (Uniprot-TrEMBL)
PDK4(?-411) ProteinQ16654 (Uniprot-TrEMBL)
PPARD ProteinQ03181 (Uniprot-TrEMBL)
PYRMetaboliteCHEBI:15361 (ChEBI)
Phase II -

Conjugation of

compounds
PathwayR-HSA-156580 (Reactome) Phase II of biotransformation is concerned with conjugation, that is using groups from cofactors to react with functional groups present or introduced from phase I on the compound. The enzymes involved are a set of transferases which perform the transfer of the cofactor group to the substrate. The resultant conjugation results in greatly increasing the excretory potential of compounds. Although most conjugations result in pharmacological inactivation or detoxification, some can result in bioactivation. Most of the phase II enzymes are located in the cytosol except UDP-glucuronosyltransferases (UGT), which are microsomal. Phase II reactions are typically much faster than phase I reactions therefore the rate-limiting step for biotransformation of a compound is usually the phase I reaction.
Phase II metabolism can deal with all the products of phase I metabolism, be they reactive (Type I substrate) or unreactive/poorly active (Type II substrate) compounds. With the exception of glutathione, the conjugating species needs to be made chemically reactive after synthesis. The availability of the cofactor in the synthesis may be a rate-limiting factor in some phase II pathways as it may prevent the formation of enough conjugating species to deal with the substrate or it's metabolite. As many substrates and/or their metabolites are chemically reactive, their continued presence may lead to toxicity.
RAR:RXRComplexR-HSA-5334826 (Reactome)
RARB ProteinP10826 (Uniprot-TrEMBL)
RARG ProteinP13631 (Uniprot-TrEMBL)
RDH10 ProteinQ8IZV5 (Uniprot-TrEMBL)
RDH10,16,DHRS9,RDHE2ComplexR-HSA-5615661 (Reactome)
RDH11 ProteinQ8TC12 (Uniprot-TrEMBL)
RDH11,14,DHRS3,DHRS4ComplexR-HSA-5419219 (Reactome)
RDH13ProteinQ8NBN7 (Uniprot-TrEMBL)
RDH14 ProteinQ9HBH5 (Uniprot-TrEMBL)
RDH16 ProteinO75452 (Uniprot-TrEMBL)
RDH5(24-318) ProteinQ92781 (Uniprot-TrEMBL)
RDH5(24-318), RDH11ComplexR-HSA-5621635 (Reactome)
RDHE2 ProteinQ8N3Y7 (Uniprot-TrEMBL)
RXRA ProteinP19793 (Uniprot-TrEMBL)
RXRA:PPARD:atRA:FABP5ComplexR-HSA-5422940 (Reactome)
RXRA:PPARD:atRAComplexR-HSA-5634107 (Reactome)
RXRA:PPARDComplexR-HSA-5422941 (Reactome)
RXRB ProteinP28702 (Uniprot-TrEMBL)
RXRG ProteinP48443 (Uniprot-TrEMBL)
SUMO-CRABP1:atRAComplexR-HSA-5622116 (Reactome)
SUMO-CRABP2:atRA:RAR:RXRComplexR-HSA-5634105 (Reactome)
SUMO-K-CRABP1 ProteinP29762 (Uniprot-TrEMBL)
SUMO-K-CRABP1ProteinP29762 (Uniprot-TrEMBL)
SUMO-K102-CRABP2 ProteinP29373 (Uniprot-TrEMBL)
SUMO-K102-CRABP2:atRAComplexR-HSA-5622130 (Reactome)
SUMO-K102-CRABP2:atRAComplexR-HSA-5634101 (Reactome)
SUMO-K102-CRABP2ProteinP29373 (Uniprot-TrEMBL)
SUMO2-K166,177,399-p-S219,269-RARA ProteinP10276 (Uniprot-TrEMBL)
TDP MetaboliteCHEBI:58937 (ChEBI)
Zn2+ MetaboliteCHEBI:29105 (ChEBI)
atRA MetaboliteCHEBI:15367 (ChEBI)
atRA:RAR:RXRComplexR-HSA-5622126 (Reactome)
atRAMetaboliteCHEBI:15367 (ChEBI)
atRALMetaboliteCHEBI:17898 (ChEBI)
atROLMetaboliteCHEBI:17336 (ChEBI)
lipo-K132,K259-DLAT ProteinP10515 (Uniprot-TrEMBL)
lipo-PDHComplexR-HSA-70070 (Reactome)
p-S21-RXRA ProteinP19793 (Uniprot-TrEMBL)
p-lipo-PDHComplexR-HSA-210342 (Reactome)

Annotated Interactions

View all...
SourceTargetTypeDatabase referenceComment
11cRALArrowR-HSA-5362721 (Reactome)
11cROLR-HSA-5362721 (Reactome)
4OH-9cRAArrowR-HSA-211923 (Reactome)
4OH-atRAArrowR-HSA-5362525 (Reactome)
9cRAArrowR-HSA-5696101 (Reactome)
9cRALR-HSA-5696101 (Reactome)
9cRAR-HSA-211923 (Reactome)
ADH1A,1C,4 dimersmim-catalysisR-HSA-5362564 (Reactome)
ADPArrowR-HSA-203946 (Reactome)
AKR1C3mim-catalysisR-HSA-5615668 (Reactome)
ALDH1A1,2,3 tetramersmim-catalysisR-HSA-5362522 (Reactome)
ALDH8A1mim-catalysisR-HSA-5696101 (Reactome)
ATPR-HSA-203946 (Reactome)
Ac-CoAArrowR-HSA-203946 (Reactome)
ArrowR-HSA-203946 (Reactome)
CARR-HSA-200406 (Reactome)
CPT1A,Bmim-catalysisR-HSA-200406 (Reactome)
CYP26A1,B1,C1mim-catalysisR-HSA-5362525 (Reactome)
CYP26C1mim-catalysisR-HSA-211923 (Reactome)
CoA-SHArrowR-HSA-200406 (Reactome)
DCA:PDK2TBarR-HSA-203946 (Reactome)
FABP5:atRAArrowR-HSA-5622129 (Reactome)
FABP5:atRAArrowR-HSA-5633256 (Reactome)
FABP5:atRAR-HSA-5422942 (Reactome)
FABP5:atRAR-HSA-5633256 (Reactome)
FABP5ArrowR-HSA-5634100 (Reactome)
FABP5R-HSA-5622129 (Reactome)
H+ArrowR-HSA-5362518 (Reactome)
H+ArrowR-HSA-5362522 (Reactome)
H+ArrowR-HSA-5362564 (Reactome)
H+ArrowR-HSA-5362721 (Reactome)
H+ArrowR-HSA-5696101 (Reactome)
H+R-HSA-211923 (Reactome)
H+R-HSA-5362525 (Reactome)
H+R-HSA-5419165 (Reactome)
H+R-HSA-5615668 (Reactome)
H+R-HSA-5623643 (Reactome)
H2OArrowR-HSA-211923 (Reactome)
H2OArrowR-HSA-5362525 (Reactome)
H2OR-HSA-5362522 (Reactome)
H2OR-HSA-5696101 (Reactome)
L-PCARNArrowR-HSA-200406 (Reactome)
Mal-CoATBarR-HSA-200406 (Reactome)
NAD+R-HSA-5362518 (Reactome)
NAD+R-HSA-5362522 (Reactome)
NAD+R-HSA-5362564 (Reactome)
NAD+R-HSA-5362721 (Reactome)
NAD+R-HSA-5696101 (Reactome)
NADHArrowR-HSA-203946 (Reactome)
NADHArrowR-HSA-5362518 (Reactome)
NADHArrowR-HSA-5362522 (Reactome)
NADHArrowR-HSA-5362564 (Reactome)
NADHArrowR-HSA-5362721 (Reactome)
NADHArrowR-HSA-5696101 (Reactome)
NADP+ArrowR-HSA-211923 (Reactome)
NADP+ArrowR-HSA-5362525 (Reactome)
NADP+ArrowR-HSA-5419165 (Reactome)
NADP+ArrowR-HSA-5615668 (Reactome)
NADP+ArrowR-HSA-5623643 (Reactome)
NADPHR-HSA-211923 (Reactome)
NADPHR-HSA-5362525 (Reactome)
NADPHR-HSA-5419165 (Reactome)
NADPHR-HSA-5615668 (Reactome)
NADPHR-HSA-5623643 (Reactome)
O2R-HSA-211923 (Reactome)
O2R-HSA-5362525 (Reactome)
PALM-CoAR-HSA-200406 (Reactome)
PDK isoformsmim-catalysisR-HSA-203946 (Reactome)
PYRTBarR-HSA-203946 (Reactome)
R-HSA-200406 (Reactome) Carnitine palmitoyl transferase 1 (CPT1) associated with the inner mitochondrial membrane, catalyzes the reaction of palmitoyl-CoA (PALM-CoA) from the cytosol with carnitine (CAR) in the mitochondrial intermembrane space to form palmitoylcarnitine (L-PCARN) and CoA-SH. Three CPT1 isoforms exist; CPT1A, B and C. In the body, CPT1A is most abundant in liver while CPT1B is abundant in muscle. CPT1C is mainly expressed in neurons and localises to the ER and not to the mitochondria. It has little or no enzymatic activity in fatty acid oxidation. Both CPT1A and CPT1B are inhibited by malonyl-CoA (Morillas et al. 2002, 2004; Zammit et al. 2001; Zhu et al. 1997). Mutations in CPT1A are associated with defects in fatty acid metabolism and fasting intolerance, consistent with the role assigned to CPT1 from studies in vitro and in animal models (IJlst et al. 1998; Gobin et al. 2003).
In the nucleus, cellular retinoic acid-binding protein 1 or 2 (CRABP1 or 2), bound to all-trans-retinoic acid (atRA), directly binds to the heterodimeric complex of retinoic acid receptor alpha RXRA) and peroxisome proliferator-activated receptor delta (PPARD). When bound to PPARD, atRA can significantly increase the expression of proteins involved in fatty acid oxidation such as CPT1A via its induction of PPARD (Amengual et al. 2012).
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-211923 (Reactome) Endogenous retinoic acids (RA) which play a role in gene regulation exist as either cis or trans isomers. While CYP26C1 can also hydroxylate the trans form, it is unique in 4-hydroxylating the 9-cis isomer of RA (9cRA) in vitro (Taimi et al. 2004). However, the importance of 9cRA as an endogenous retinoid outside of the pancreas has not been demonstrated.
R-HSA-5334827 (Reactome) Cellular retinoic acid-binding protein 2 (CRABP2) is a cytosolic, lipid-binding protein thought to bind its natural ligand, all-trans-retinoic acid (atRA) and mediate its delivery to retinoic acid receptors (RARs) within the nucleus (Kleywegt et al. 1994). CRABP2 forms a beta-barrel structure within which a hydrophobic ligand can be accommodated. Once atRA binds to CRABP2, the resulting complex translocates to the nucleus (Budhu & Noy 2002). A ligand activated nuclear-localisation signal appears to be critical for nuclear localisation (Sessler & Noy 2005). Sumoylation of CRABPs is also essential for atRA-induced dissociation of CRABPs from the ER membrane. For CRABP2, the site K102 is sumoylated (Majumdar et al. 2011).
R-HSA-5334854 (Reactome) In the nucleus, cellular retinoic acid binding protein 2 (CRABP2), bound to all trans retinoic acid (atRA), directly binds to heterodimeric nuclear retinoic acid receptors (RAR:RXR) to form a complex through which atRA is channeled from the binding protein to RAR (Majumdar et al. 2011). The RAR:RXR heterodimer can be formed between any of three receptor isoforms for each; RARA, RARB, or RARG with RXRA, RXRB, or RXRG (Neiderreither and Dolle 2008). RARA requires sumoylation and phosphorylation for ligand binding and nuclear localisation (Zhu et al. 2009, Santos & Kim 2010).

RAR:RXR bind to their RA response elements (RARE, composed of tandem direct repeats of 5'-AGGTCA-3' spaced by either 2 bp or 5 bp (DR2, DR5) in response to their physiological ligand atRA, and regulate gene expression in various biological processes.
R-HSA-5362518 (Reactome) Multiple retinol dehydrogenases (RDH), members of the short-chain dehydrogenase/reductase (SDR) gene family, are candidates for catalysing conversion of retinol into retinal under physiological conditions (Napoli 2012). These include RDH16 (aka RoDH-4, RDH-E, Rdh1), RDH10, DHRS9 (aka retSDR8) and RDHE2. Two of these, Rdh1 (human ortholog RDH16) and Rdh10 (human ortholog RDH10), have been knocked out in mice and display RA-associated phenotypes. Both are membrane bound oxidoreductases that reversibly catalyse the first and rate limiting step in retinoic acid biosynthesis, and use NAD+ as cofactor to the corresponding aldehyde all trans retinal (atRAL) (Gough et al. 1998, Jurukovski et al. 1999, Pecozzi et al. 2003). The other RDH are currently under study, but have not been ablated in mice.
R-HSA-5362522 (Reactome) Several aldehyde dehydrogenases catalyse the irreversible oxidation of retinal to retinoic acid. ALDH1A1, 2 and 3 utilise NAD+ as cofactor to oxidise all-trans-retinal (atRAL) to all-trans-retinoic acid (atRA). They are cytosolic enzymes which are functional in their homotetrameric states (Yoshida et al. 1993, Duester 2008, Bchini et al. 2013).
R-HSA-5362525 (Reactome) All-trans-retinoic acid (atRA) is a biologically activated metabolite of vitamin A (retinol) and is essential for reproduction, embryonic development, growth, and multiple processes in the adult, including energy balance, neurogenesis, and the immune response. Cytochrome P450 26A1 and B1 (CYP26A1 and B1) play a key role in retinoid metabolism (Ross & Zolfaghari 2011). They 4-hydroxylate all-trans-retinoic acid (atRA), delivered by CRABP1, to form all-trans-4-hydroxyretinoic acid (4OH-atRA) which can then be eliminated from the body. CYP26A1 and B1 are also able to 4-hydroxylate 9-cis-retinoic acid and 13-cis-retinoic acid (9cRA and 13cRA respectively) in vitro. These enzymes are also produce 18-hydroxy and 4-oxo forms of these retinoic acids (not shown here).

The inactivation of RA by CYP26B1 is essential for postnatal survival and maintenance of the undifferentiated state of male germ cells during embryonic development in Sertoli cells. Excessive RA also has teratogenic effects in the limb and craniofacial skeleton. Defects in CYP26B1 can cause radiohumeral fusions with other skeletal and craniofacial anomalies (RHFCA; MIM:614416) (Laue et al. 2011).
R-HSA-5362564 (Reactome) Some alcohol dehydrogenases (ADHs) utilise NAD+ as cofactor to reversibly oxidise all-trans-retinol (atROL) to all-trans-retinal (atRAL), a retinoid aldehyde, in vitro (von Bahr-Lindstrom et al. 1986, Ikuta et al. 1986, von Bahr-Lindstrom et al. 1991, Xie et al. 1997). ADH1A (ADH1) and ADH4 have high activity and ADH1C (ADH3) has low activity with non-physiological amounts of retinol in vitro. ADH1A and ADH1C metabolize toxic amounts of retinol in vivo, but ADH4 does not. Physiological contributions of ADHs to retinol metabolism have not been demonstrated, in contrast to RDHs.
R-HSA-5362721 (Reactome) 11-cis-retinol dehydrogenase (RDH5) and RDH11 catalyse the final step in the biosynthesis of 11-cis-retinal (11cRAL), the universal chromophore of visual pigments, whereas RDH8, RDH12, and DHRS3 (retSDR1) catalyze the conversion of all-trans-retinal (atRAL) into all-trans-retinol (atROL) to maintain the cycle (Parker & Crouch 2010). Defects in the RDH5 gene can cause fundus albipunctatus (RPA; MIM:136880), a rare form of stationary night blindness characterised by a delay in the regeneration of cone and rod photopigments (Yamamoto et al. 1999).
R-HSA-5419165 (Reactome) Multiple reductases may contribute to the reduction of all-trans-retinal (atRAL) to all-trans-retinol (atROL), including RDH11 (aka PSDR1, RalR1), RDH14, DHRS3 (aka retSDR1, RDH17) and DHRS4 (aka RRD, SCAD-SRL) (Haeseleer et al. 1998, Haeseleer et al. 2002, Kedishvili et al. 2002, Lin et al. 2001, Zhen et al. 2003, Belyaeva et al. 2008).
R-HSA-5422942 (Reactome) In the nucleus, all-trans-retinoic acid (atRA), bounds to epidermal fatty acid-binding protein (FABP5), is transferred to the heterodimeric complex of retinoic acid receptor alpha RXRA) and peroxisome proliferator-activated receptor delta (PPARD). When bound to PPARD, atRA can significantly increase the expression of proteins involved in fatty acid oxidation and energy metabolism via its induction of PPARD (Wolf 2010, Amengual et al. 2012, Noy 2013).
R-HSA-5615668 (Reactome) The cytosolic aldo-keto reductase 1C3 (AKR1C3) can reduce all-trans-retinal (atRAL) to all-trans-retinol (atROL) (Ruiz et al. 2011). AKR1C3 functions to reduce synthesis of atRA to prevent toxic or teratogenic effects of excess atRA.
R-HSA-5622129 (Reactome) Epidermal fatty acid-binding protein (FABP5) is a cytosolic, lipid-binding protein thought to bind all-trans-retinoic acid (atRA) and mediate its delivery to retinoic acid receptors (RARs) within the nucleus (Hohoff et al. 1999, Smathers & Petersen 2011).
R-HSA-5622134 (Reactome) All-trans-retinoic acid (atRA) metabolism can be mediated by CYP26 degradation. Cellular retinol-binding protein I (CRABP1) binds and delivers atRA to CY26 enzymes (Noy 2000).
R-HSA-5623643 (Reactome) Multiple reductases may contribute to the reduction of all-trans-retinal (atRAL) to all-trans-retinol (atROL). Human retinol dehydrogenase 13 (RDH13) is located on the outer surface of the mitochondrial inner membrane where it is thought to protect mitochondria against oxidative stress associated with the highly reactive retinaldehyde (Belyaeva et al. 2008).
R-HSA-5633256 (Reactome) Epidermal fatty acid-binding protein (FABP5) is a cytosolic, lipid-binding protein thought to bind all-trans-retinoic acid (atRA) and mediate its delivery to retinoic acid receptors (RARs) within the nucleus (Hohoff et al. 1999, Smathers & Petersen 2011).
R-HSA-5634100 (Reactome) In the nucleus, all-trans-retinoic acid (atRA), bounds to epidermal fatty acid-binding protein (FABP5), is transferred to the heterodimeric complex of retinoic acid receptor alpha RXRA) and peroxisome proliferator-activated receptor delta (PPARD). When bound to PPARD, atRA can significantly increase the expression of proteins involved in fatty acid oxidation and energy metabolism via its induction of PPARD (Wolf 2010, Amengual et al. 2012, Noy 2013).
R-HSA-5634103 (Reactome) In the nucleus, cellular retinoic acid binding protein 2 (CRABP2), bound to all trans retinoic acid (atRA), directly binds to heterodimeric nuclear retinoic acid receptors (RAR:RXR) to form a complex through which atRA is channeled from the binding protein to RAR (Majumdar et al. 2011). The RAR:RXR heterodimer can be formed between any of three receptor isoforms for each; RARA, RARB, or RARG with RXRA, RXRB, or RXRG (Neiderreither and Dolle 2008). RARA requires sumoylation and phosphorylation for ligand binding and nuclear localisation (Zhu et al. 2009, Santos & Kim 2010).

RAR:RXR bind to their RA response elements (RARE, composed of tandem direct repeats of 5'-AGGTCA-3' spaced by either 2 bp or 5 bp (DR2, DR5) in response to their physiological ligand atRA, and regulate gene expression in various biological processes.
R-HSA-5634104 (Reactome) Cellular retinoic acid-binding protein 2 (CRABP2) is a cytosolic, lipid-binding protein thought to bind its natural ligand, all-trans-retinoic acid (atRA) and mediate its delivery to retinoic acid receptors (RARs) within the nucleus (Kleywegt et al. 1994). CRABP2 forms a beta-barrel structure within which a hydrophobic ligand can be accommodated. Once atRA binds to CRABP2, the resulting complex translocates to the nucleus (Budhu & Noy 2002). A ligand activated nuclear-localisation signal appears to be critical for nuclear localisation (Sessler & Noy 2005). Sumoylation of CRABPs is also essential for atRA-induced dissociation of CRABPs from the ER membrane. For CRABP2, the site K102 is sumoylated (Majumdar et al. 2011).
R-HSA-5696101 (Reactome) Aldehyde dehydrogenase family 8 member A1 (ALDH8A1, ALDH12) can preferentially mediate the oxidation of 9-cis-retinal (9cRAL) into the retinoid X receptor ligand 9-cis-retinoic acid (9cRA) (Lin & Napoli 2000). ALDH8A1 might function in the pathway of 9-cis-retinal metabolism.
RAR:RXRR-HSA-5334854 (Reactome)
RDH10,16,DHRS9,RDHE2mim-catalysisR-HSA-5362518 (Reactome)
RDH11,14,DHRS3,DHRS4mim-catalysisR-HSA-5419165 (Reactome)
RDH13mim-catalysisR-HSA-5623643 (Reactome)
RDH5(24-318), RDH11mim-catalysisR-HSA-5362721 (Reactome)
RXRA:PPARD:atRA:FABP5ArrowR-HSA-5422942 (Reactome)
RXRA:PPARD:atRA:FABP5R-HSA-5634100 (Reactome)
RXRA:PPARD:atRAArrowR-HSA-200406 (Reactome)
RXRA:PPARD:atRAArrowR-HSA-5634100 (Reactome)
RXRA:PPARDR-HSA-5422942 (Reactome)
SUMO-CRABP1:atRAArrowR-HSA-5622134 (Reactome)
SUMO-CRABP1:atRAR-HSA-5362525 (Reactome)
SUMO-CRABP2:atRA:RAR:RXRArrowR-HSA-5334854 (Reactome)
SUMO-CRABP2:atRA:RAR:RXRR-HSA-5634103 (Reactome)
SUMO-K-CRABP1ArrowR-HSA-5362525 (Reactome)
SUMO-K-CRABP1R-HSA-5622134 (Reactome)
SUMO-K102-CRABP2:atRAArrowR-HSA-5334827 (Reactome)
SUMO-K102-CRABP2:atRAArrowR-HSA-5634104 (Reactome)
SUMO-K102-CRABP2:atRAR-HSA-5334854 (Reactome)
SUMO-K102-CRABP2:atRAR-HSA-5634104 (Reactome)
SUMO-K102-CRABP2ArrowR-HSA-5634103 (Reactome)
SUMO-K102-CRABP2R-HSA-5334827 (Reactome)
atRA:RAR:RXRArrowR-HSA-5634103 (Reactome)
atRAArrowR-HSA-5362522 (Reactome)
atRALArrowR-HSA-5362518 (Reactome)
atRALArrowR-HSA-5362564 (Reactome)
atRALR-HSA-5362522 (Reactome)
atRALR-HSA-5419165 (Reactome)
atRALR-HSA-5615668 (Reactome)
atRALR-HSA-5623643 (Reactome)
atRAR-HSA-5334827 (Reactome)
atRAR-HSA-5622129 (Reactome)
atRAR-HSA-5622134 (Reactome)
atROLArrowR-HSA-5419165 (Reactome)
atROLArrowR-HSA-5615668 (Reactome)
atROLArrowR-HSA-5623643 (Reactome)
atROLR-HSA-5362518 (Reactome)
atROLR-HSA-5362564 (Reactome)
lipo-PDHR-HSA-203946 (Reactome)
p-lipo-PDHArrowR-HSA-203946 (Reactome)
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