Metabolism of steroid hormones (Homo sapiens)

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Description

Steroid hormones are synthesized primarily in the adrenal gland and gonads. They regulate energy metabolism and stress responses (glucocorticoids), salt balance (mineralocorticoids), and sexual development and function (androgens and estrogens). All steroids are synthesized from cholesterol. Steroid hormone synthesis is largely regulated at the initial steps of cholesterol mobilization and transport into the mitochondrial matrix for conversion to pregnenolone. In the body, the fate of pregnenolone is tissue-specific: in the zona fasciculata of the adrenal cortex it is converted to cortisol, in the zona glomerulosa to aldosterone, and in the gonads to testosterone and then to estrone and estradiol. These pathways are outlined in the figure below, which also details the sites on the cholesterol molecule that undergo modification in the course of these reactions.

Vitamin D3 (cholecalciferol) is a steroid hormone that plays a role in regulating calcium and bone metabolism. The processes by which it is synthesized, modified, and transported in the body are annotated here. Source:Reactome.</div>

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Bibliography

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History

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Revision	Action	Time	User	Comment
115089	view	17:04, 25 January 2021	ReactomeTeam	Reactome version 75
113531	view	12:01, 2 November 2020	ReactomeTeam	Reactome version 74
112729	view	16:13, 9 October 2020	ReactomeTeam	Reactome version 73
101645	view	11:51, 1 November 2018	ReactomeTeam	reactome version 66
101181	view	21:38, 31 October 2018	ReactomeTeam	reactome version 65
100707	view	20:10, 31 October 2018	ReactomeTeam	reactome version 64
100257	view	16:56, 31 October 2018	ReactomeTeam	reactome version 63
99810	view	15:20, 31 October 2018	ReactomeTeam	reactome version 62 (2nd attempt)
99354	view	12:48, 31 October 2018	ReactomeTeam	reactome version 62
94495	view	09:01, 14 September 2017	Mkutmon	reactome version 61
87913	view	12:59, 25 July 2016	Ryanmiller	Ontology Term : 'classic metabolic pathway' added !
83163	view	10:14, 18 November 2015	ReactomeTeam	Version54
81521	view	13:03, 21 August 2015	ReactomeTeam	Version53
76990	view	08:28, 17 July 2014	ReactomeTeam	Fixed remaining interactions
76695	view	12:06, 16 July 2014	ReactomeTeam	Fixed remaining interactions
76021	view	10:08, 11 June 2014	ReactomeTeam	Re-fixing comment source
75730	view	11:20, 10 June 2014	ReactomeTeam	Reactome 48 Update
75080	view	14:02, 8 May 2014	Anwesha	Fixing comment source for displaying WikiPathways description
74727	view	08:48, 30 April 2014	ReactomeTeam	New pathway

External references

DataNodes

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Name	Type	Database reference	Comment
11-deoxycortisol	Metabolite	CHEBI:28324 (ChEBI)
11DCORST	Metabolite	CHEBI:16973 (ChEBI)
11DCORT	Metabolite	CHEBI:28324 (ChEBI)
17aHPREG	Metabolite	CHEBI:28750 (ChEBI)
17aHPROG	Metabolite	CHEBI:17252 (ChEBI)
18HCORST	Metabolite	CHEBI:16485 (ChEBI)
20a,22b-DHCHOL	Metabolite	CHEBI:1294 (ChEBI)
22beta-hydroxycholesterol	Metabolite	CHEBI:1301 (ChEBI)
7-dehydrocholesterol	Metabolite	CHEBI:17759 (ChEBI)
AKR1B1	Protein	P15121 (Uniprot-TrEMBL)
ALDO	Metabolite	CHEBI:27584 (ChEBI)
ANDST	Metabolite	CHEBI:16422 (ChEBI)
CDL	Metabolite	CHEBI:17933 (ChEBI)
CDL	Metabolite	CHEBI:17933 (ChEBI)
CGA	Protein	P01215 (Uniprot-TrEMBL)
CH3CHO	Metabolite	CHEBI:15343 (ChEBI)
CHOL	Metabolite	CHEBI:16113 (ChEBI)
COR	Metabolite	CHEBI:16962 (ChEBI)
CORST	Metabolite	CHEBI:16827 (ChEBI)
CORT	Metabolite	CHEBI:17650 (ChEBI)
CTA	Metabolite	CHEBI:47828 (ChEBI)
CTL	Metabolite	CHEBI:17823 (ChEBI)
CUBN	Protein	O60494 (Uniprot-TrEMBL)
CUBN:GC:CDL	Complex	R-HSA-350115 (Reactome)
CUBN	Protein	O60494 (Uniprot-TrEMBL)
CYP11A1	Protein	P05108 (Uniprot-TrEMBL)
CYP11B2	Protein	P19099 (Uniprot-TrEMBL)
CYP17A1	Protein	P05093 (Uniprot-TrEMBL)
CYP19A1	Protein	P11511 (Uniprot-TrEMBL)
CYP21A2	Protein	P08686 (Uniprot-TrEMBL)
CYP24A1	Protein	Q07973 (Uniprot-TrEMBL)
CYP27B1(?-508)	Protein	O15528 (Uniprot-TrEMBL)	The start coordinate is not yet known
CYP2R1	Protein	Q6VVX0 (Uniprot-TrEMBL)
Cubilin:DBP:Calcidiol	Complex	R-HSA-350085 (Reactome)
Cubilin:DBP:Calcidiol	Complex	R-HSA-350092 (Reactome)
Cytochrome P450 (CYP11B1 based)	Protein	R-HSA-3219421 (Reactome)	This CandidateSet contains sequences identified by William Pearson's analysis of Reactome catalyst entities. Catalyst entity sequences were used to identify analagous sequences that shared overall homology and active site homology. Sequences in this Candidate set were identified in an April 24, 2012 analysis.
DBP:vitamin D3	Complex	R-HSA-352339 (Reactome)
DHEA	Metabolite	CHEBI:28689 (ChEBI)
DHTEST	Metabolite	CHEBI:16330 (ChEBI)
E1	Metabolite	CHEBI:17263 (ChEBI)
EST17b	Metabolite	CHEBI:16469 (ChEBI)
GC	Protein	P02774 (Uniprot-TrEMBL)
GC:CDL	Complex	R-HSA-209892 (Reactome)
GC	Protein	P02774 (Uniprot-TrEMBL)
H+	Metabolite	CHEBI:15378 (ChEBI)
H2O	Metabolite	CHEBI:15377 (ChEBI)
HCOOH	Metabolite	CHEBI:30751 (ChEBI)
HSD11B1	Protein	P28845 (Uniprot-TrEMBL)
HSD11B1 dimer	Complex	R-HSA-193980 (Reactome)
HSD17B1	Protein	P14061 (Uniprot-TrEMBL)
HSD17B1 dimer	Complex	R-HSA-804966 (Reactome)
HSD17B3-like Proteins	Protein	R-HSA-3902489 (Reactome)	This CandidateSet contains sequences identified by William Pearson's analysis of Reactome catalyst entities. Catalyst entity sequences were used to identify analagous sequences that shared overall homology and active site homology. Sequences in this Candidate set were identified in an April 24, 2012 analysis.
HSD2B1 or HSD3B2 dimer	Complex	R-HSA-196357 (Reactome)
HSD3B1	Protein	P14060 (Uniprot-TrEMBL)
HSD3B2	Protein	P26439 (Uniprot-TrEMBL)
ISCAL	Metabolite	CHEBI:17998 (ChEBI)
LGMN	Protein	Q99538 (Uniprot-TrEMBL)
LHB	Protein	P01229 (Uniprot-TrEMBL)
LRP2	Protein	P98164 (Uniprot-TrEMBL)
Lutropin	Complex	R-HSA-378969 (Reactome)
MePeOH	Metabolite	CHEBI:63910 (ChEBI)
NAD+	Metabolite	CHEBI:15846 (ChEBI)
NADH	Metabolite	CHEBI:16908 (ChEBI)
NADP+	Metabolite	CHEBI:18009 (ChEBI)
NADPH	Metabolite	CHEBI:16474 (ChEBI)
O2	Metabolite	CHEBI:15379 (ChEBI)
P4	Metabolite	CHEBI:17026 (ChEBI)
POMC(138-176)	Protein	P01189 (Uniprot-TrEMBL)
PREG	Metabolite	CHEBI:16581 (ChEBI)
SRD5A1-3	Protein	R-HSA-469656 (Reactome)
STAR	Protein	P49675 (Uniprot-TrEMBL)
STAR	Protein	P49675 (Uniprot-TrEMBL)
StAR-related cholesterol-binding proteins	Protein	R-HSA-196094 (Reactome)
TEST	Metabolite	CHEBI:17347 (ChEBI)
VD3	Metabolite	CHEBI:28940 (ChEBI)
VD3	Metabolite	CHEBI:28940 (ChEBI)
cholesterol	Metabolite	CHEBI:16113 (ChEBI)
cholesterol:STAR	Complex	R-HSA-196090 (Reactome)
cholesterol:StAR-related protein	Complex	R-HSA-196124 (Reactome)
cholesterol	Metabolite	CHEBI:16113 (ChEBI)
pregn-5-ene-3,20-dione-17-ol	Metabolite	CHEBI:63843 (ChEBI)
pregn-5-ene-3,20-dione	Metabolite	CHEBI:63837 (ChEBI)

Annotated Interactions

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Source	Target	Type	Database reference	Comment
	11-deoxycortisol	Arrow	R-HSA-193981 (Reactome)
11-deoxycortisol			R-HSA-194025 (Reactome)
	11DCORST	Arrow	R-HSA-193964 (Reactome)
	11DCORST	Arrow	R-HSA-193996 (Reactome)
11DCORST			R-HSA-193996 (Reactome)
11DCORST			R-HSA-194017 (Reactome)
	11DCORT	Arrow	R-HSA-194025 (Reactome)
11DCORT			R-HSA-193997 (Reactome)
	17aHPREG	Arrow	R-HSA-193068 (Reactome)
17aHPREG			R-HSA-193070 (Reactome)
17aHPREG			R-HSA-196372 (Reactome)
	17aHPROG	Arrow	R-HSA-193072 (Reactome)
	17aHPROG	Arrow	R-HSA-193961 (Reactome)
17aHPROG			R-HSA-193099 (Reactome)
17aHPROG			R-HSA-193981 (Reactome)
	18HCORST	Arrow	R-HSA-193995 (Reactome)
18HCORST			R-HSA-193965 (Reactome)
	20a,22b-DHCHOL	Arrow	R-HSA-193065 (Reactome)
20a,22b-DHCHOL			R-HSA-193101 (Reactome)
	22beta-hydroxycholesterol	Arrow	R-HSA-193054 (Reactome)
22beta-hydroxycholesterol			R-HSA-193065 (Reactome)
7-dehydrocholesterol			R-HSA-209754 (Reactome)
AKR1B1		mim-catalysis	R-HSA-196060 (Reactome)
	ALDO	Arrow	R-HSA-193965 (Reactome)
	ANDST	Arrow	R-HSA-193073 (Reactome)
	ANDST	Arrow	R-HSA-193099 (Reactome)
ANDST			R-HSA-193060 (Reactome)
ANDST			R-HSA-193064 (Reactome)
	CDL	Arrow	R-HSA-209766 (Reactome)
	CDL	Arrow	R-HSA-209845 (Reactome)
	CDL	Arrow	R-HSA-350158 (Reactome)
CDL			R-HSA-209766 (Reactome)
CDL			R-HSA-209868 (Reactome)
CDL			R-HSA-209944 (Reactome)
	CH3CHO	Arrow	R-HSA-193070 (Reactome)
	CH3CHO	Arrow	R-HSA-193099 (Reactome)
	COR	Arrow	R-HSA-194023 (Reactome)
	CORST	Arrow	R-HSA-194017 (Reactome)
CORST			R-HSA-193995 (Reactome)
	CORT	Arrow	R-HSA-193997 (Reactome)
	CORT	Arrow	R-HSA-194036 (Reactome)
CORT			R-HSA-194023 (Reactome)
CORT			R-HSA-194036 (Reactome)
	CTA	Arrow	R-HSA-209765 (Reactome)
	CTL	Arrow	R-HSA-209868 (Reactome)
CTL			R-HSA-209765 (Reactome)
	CUBN:GC:CDL	Arrow	R-HSA-350186 (Reactome)
CUBN:GC:CDL			R-HSA-350168 (Reactome)
	CUBN	Arrow	R-HSA-350158 (Reactome)
CUBN			R-HSA-350186 (Reactome)
CYP11A1		mim-catalysis	R-HSA-193054 (Reactome)
CYP11A1		mim-catalysis	R-HSA-193065 (Reactome)
CYP11A1		mim-catalysis	R-HSA-193101 (Reactome)
CYP11B2		mim-catalysis	R-HSA-193965 (Reactome)
CYP11B2		mim-catalysis	R-HSA-193995 (Reactome)
CYP17A1		mim-catalysis	R-HSA-193068 (Reactome)
CYP17A1		mim-catalysis	R-HSA-193070 (Reactome)
CYP17A1		mim-catalysis	R-HSA-193072 (Reactome)
CYP17A1		mim-catalysis	R-HSA-193099 (Reactome)
CYP19A1		mim-catalysis	R-HSA-193060 (Reactome)
CYP19A1		mim-catalysis	R-HSA-193143 (Reactome)
CYP21A2		mim-catalysis	R-HSA-193964 (Reactome)
CYP21A2		mim-catalysis	R-HSA-193981 (Reactome)
CYP24A1		mim-catalysis	R-HSA-209765 (Reactome)
CYP27B1(?-508)		mim-catalysis	R-HSA-209868 (Reactome)
CYP2R1		mim-catalysis	R-HSA-209845 (Reactome)
	Cubilin:DBP:Calcidiol	Arrow	R-HSA-209760 (Reactome)
	Cubilin:DBP:Calcidiol	Arrow	R-HSA-350168 (Reactome)
Cubilin:DBP:Calcidiol			R-HSA-209760 (Reactome)
Cubilin:DBP:Calcidiol			R-HSA-350158 (Reactome)
Cytochrome P450 (CYP11B1 based)		mim-catalysis	R-HSA-193997 (Reactome)
Cytochrome P450 (CYP11B1 based)		mim-catalysis	R-HSA-194017 (Reactome)
	DBP:vitamin D3	Arrow	R-HSA-209738 (Reactome)
DBP:vitamin D3			R-HSA-350147 (Reactome)
	DHEA	Arrow	R-HSA-193070 (Reactome)
DHEA			R-HSA-193073 (Reactome)
	DHTEST	Arrow	R-HSA-469659 (Reactome)
	E1	Arrow	R-HSA-193060 (Reactome)
E1			R-HSA-804969 (Reactome)
	EST17b	Arrow	R-HSA-193143 (Reactome)
	EST17b	Arrow	R-HSA-804969 (Reactome)
	GC:CDL	Arrow	R-HSA-209944 (Reactome)
GC:CDL			R-HSA-350186 (Reactome)
	GC	Arrow	R-HSA-350147 (Reactome)
GC			R-HSA-209738 (Reactome)
GC			R-HSA-209944 (Reactome)
	H+	Arrow	R-HSA-193073 (Reactome)
	H+	Arrow	R-HSA-194023 (Reactome)
	H+	Arrow	R-HSA-196350 (Reactome)
	H+	Arrow	R-HSA-196372 (Reactome)
H+			R-HSA-193054 (Reactome)
H+			R-HSA-193060 (Reactome)
H+			R-HSA-193064 (Reactome)
H+			R-HSA-193065 (Reactome)
H+			R-HSA-193068 (Reactome)
H+			R-HSA-193070 (Reactome)
H+			R-HSA-193072 (Reactome)
H+			R-HSA-193099 (Reactome)
H+			R-HSA-193101 (Reactome)
H+			R-HSA-193143 (Reactome)
H+			R-HSA-193964 (Reactome)
H+			R-HSA-193965 (Reactome)
H+			R-HSA-193981 (Reactome)
H+			R-HSA-193995 (Reactome)
H+			R-HSA-193997 (Reactome)
H+			R-HSA-194017 (Reactome)
H+			R-HSA-196060 (Reactome)
H+			R-HSA-209765 (Reactome)
H+			R-HSA-209845 (Reactome)
H+			R-HSA-209868 (Reactome)
H+			R-HSA-469659 (Reactome)
H+			R-HSA-804969 (Reactome)
	H2O	Arrow	R-HSA-193054 (Reactome)
	H2O	Arrow	R-HSA-193060 (Reactome)
	H2O	Arrow	R-HSA-193065 (Reactome)
	H2O	Arrow	R-HSA-193068 (Reactome)
	H2O	Arrow	R-HSA-193070 (Reactome)
	H2O	Arrow	R-HSA-193072 (Reactome)
	H2O	Arrow	R-HSA-193099 (Reactome)
	H2O	Arrow	R-HSA-193101 (Reactome)
	H2O	Arrow	R-HSA-193143 (Reactome)
	H2O	Arrow	R-HSA-193964 (Reactome)
	H2O	Arrow	R-HSA-193965 (Reactome)
	H2O	Arrow	R-HSA-193981 (Reactome)
	H2O	Arrow	R-HSA-193995 (Reactome)
	H2O	Arrow	R-HSA-193997 (Reactome)
	H2O	Arrow	R-HSA-194017 (Reactome)
	H2O	Arrow	R-HSA-209765 (Reactome)
	H2O	Arrow	R-HSA-209845 (Reactome)
	H2O	Arrow	R-HSA-209868 (Reactome)
	HCOOH	Arrow	R-HSA-193060 (Reactome)
	HCOOH	Arrow	R-HSA-193143 (Reactome)
HSD11B1 dimer		mim-catalysis	R-HSA-194023 (Reactome)
HSD17B1 dimer		mim-catalysis	R-HSA-804969 (Reactome)
HSD17B3-like Proteins		mim-catalysis	R-HSA-193064 (Reactome)
HSD2B1 or HSD3B2 dimer		mim-catalysis	R-HSA-193052 (Reactome)
HSD2B1 or HSD3B2 dimer		mim-catalysis	R-HSA-193073 (Reactome)
HSD2B1 or HSD3B2 dimer		mim-catalysis	R-HSA-193961 (Reactome)
HSD2B1 or HSD3B2 dimer		mim-catalysis	R-HSA-196350 (Reactome)
HSD2B1 or HSD3B2 dimer		mim-catalysis	R-HSA-196372 (Reactome)
	ISCAL	Arrow	R-HSA-193101 (Reactome)
	ISCAL	Arrow	R-HSA-196125 (Reactome)
ISCAL			R-HSA-196060 (Reactome)
ISCAL			R-HSA-196125 (Reactome)
LGMN		mim-catalysis	R-HSA-350158 (Reactome)
LRP2		mim-catalysis	R-HSA-350168 (Reactome)
Lutropin		Arrow	R-HSA-193052 (Reactome)
Lutropin		Arrow	R-HSA-193064 (Reactome)
	MePeOH	Arrow	R-HSA-196060 (Reactome)
NAD+			R-HSA-193073 (Reactome)
NAD+			R-HSA-196350 (Reactome)
NAD+			R-HSA-196372 (Reactome)
	NADH	Arrow	R-HSA-193073 (Reactome)
	NADH	Arrow	R-HSA-196350 (Reactome)
	NADH	Arrow	R-HSA-196372 (Reactome)
	NADP+	Arrow	R-HSA-193054 (Reactome)
	NADP+	Arrow	R-HSA-193060 (Reactome)
	NADP+	Arrow	R-HSA-193064 (Reactome)
	NADP+	Arrow	R-HSA-193065 (Reactome)
	NADP+	Arrow	R-HSA-193068 (Reactome)
	NADP+	Arrow	R-HSA-193070 (Reactome)
	NADP+	Arrow	R-HSA-193072 (Reactome)
	NADP+	Arrow	R-HSA-193099 (Reactome)
	NADP+	Arrow	R-HSA-193101 (Reactome)
	NADP+	Arrow	R-HSA-193143 (Reactome)
	NADP+	Arrow	R-HSA-193964 (Reactome)
	NADP+	Arrow	R-HSA-193965 (Reactome)
	NADP+	Arrow	R-HSA-193981 (Reactome)
	NADP+	Arrow	R-HSA-193995 (Reactome)
	NADP+	Arrow	R-HSA-193997 (Reactome)
	NADP+	Arrow	R-HSA-194017 (Reactome)
	NADP+	Arrow	R-HSA-196060 (Reactome)
	NADP+	Arrow	R-HSA-209765 (Reactome)
	NADP+	Arrow	R-HSA-209845 (Reactome)
	NADP+	Arrow	R-HSA-209868 (Reactome)
	NADP+	Arrow	R-HSA-469659 (Reactome)
	NADP+	Arrow	R-HSA-804969 (Reactome)
NADP+			R-HSA-194023 (Reactome)
	NADPH	Arrow	R-HSA-194023 (Reactome)
NADPH			R-HSA-193054 (Reactome)
NADPH			R-HSA-193060 (Reactome)
NADPH			R-HSA-193064 (Reactome)
NADPH			R-HSA-193065 (Reactome)
NADPH			R-HSA-193068 (Reactome)
NADPH			R-HSA-193070 (Reactome)
NADPH			R-HSA-193072 (Reactome)
NADPH			R-HSA-193099 (Reactome)
NADPH			R-HSA-193101 (Reactome)
NADPH			R-HSA-193143 (Reactome)
NADPH			R-HSA-193964 (Reactome)
NADPH			R-HSA-193965 (Reactome)
NADPH			R-HSA-193981 (Reactome)
NADPH			R-HSA-193995 (Reactome)
NADPH			R-HSA-193997 (Reactome)
NADPH			R-HSA-194017 (Reactome)
NADPH			R-HSA-196060 (Reactome)
NADPH			R-HSA-209765 (Reactome)
NADPH			R-HSA-209845 (Reactome)
NADPH			R-HSA-209868 (Reactome)
NADPH			R-HSA-469659 (Reactome)
NADPH			R-HSA-804969 (Reactome)
O2			R-HSA-193054 (Reactome)
O2			R-HSA-193060 (Reactome)
O2			R-HSA-193065 (Reactome)
O2			R-HSA-193068 (Reactome)
O2			R-HSA-193070 (Reactome)
O2			R-HSA-193072 (Reactome)
O2			R-HSA-193099 (Reactome)
O2			R-HSA-193101 (Reactome)
O2			R-HSA-193143 (Reactome)
O2			R-HSA-193964 (Reactome)
O2			R-HSA-193965 (Reactome)
O2			R-HSA-193981 (Reactome)
O2			R-HSA-193995 (Reactome)
O2			R-HSA-193997 (Reactome)
O2			R-HSA-194017 (Reactome)
O2			R-HSA-209765 (Reactome)
O2			R-HSA-209845 (Reactome)
O2			R-HSA-209868 (Reactome)
	P4	Arrow	R-HSA-193052 (Reactome)
P4			R-HSA-193072 (Reactome)
P4			R-HSA-193964 (Reactome)
POMC(138-176)		Arrow	R-HSA-193064 (Reactome)
POMC(138-176)		Arrow	R-HSA-193070 (Reactome)
POMC(138-176)		Arrow	R-HSA-193073 (Reactome)
POMC(138-176)		Arrow	R-HSA-193997 (Reactome)
POMC(138-176)		Arrow	R-HSA-469659 (Reactome)
	PREG	Arrow	R-HSA-193097 (Reactome)
	PREG	Arrow	R-HSA-193101 (Reactome)
PREG			R-HSA-193068 (Reactome)
PREG			R-HSA-193097 (Reactome)
PREG			R-HSA-196350 (Reactome)
			R-HSA-193052 (Reactome)	Pregn-5-ene-3,20-dione isomerizes to progesterone. This reaction is catalyzed by the isomerase activity of 3 beta-HSD, associated with the endoplasmic reticulum membrane. The active form of the enzyme is a homodimer. The enzyme occurs in two isoforms that are similar in their biochemical properties but differ in their tissue expression: type I (HSD3B1) is found in placenta and skin, while type II (HSD3B2) is found in the adrenal glands and gonads. The hormone lutropin (LH) triggers ovulation and development of the corpus luteum, that in turn increases production of progesterone.
			R-HSA-193054 (Reactome)	Cholesterol and NADPH + H+ react to form 22beta-hydroxycholesterol, NADP+, and H2O, catalyzed by CYP11A (P450scc) associated with the inner mitochondrial membrane.
			R-HSA-193060 (Reactome)	The conversion of androstenedione (ANDST) to estrone (E1) is catalysed by aromatase (CYP19A1) associated with the endoplasmic reticulum membrane (Toda et al. 1990, Simpson et al. 1994).
			R-HSA-193064 (Reactome)	The 17HSD family of enzymes catalyze the final step in the synthesis of estradiol and testosterone. They convert inactive 17-ketosteroids to their active 17beta-hydroxy forms. Androstenedione, a ketosteroid, is reduced to testosterone, a highly potent androgen, by the enzyme 17beta-hydroxysteroid dehydrogenase isoform III (17HSD3). The other human isoforms of 17HSDs to take part in the final steps of active steroid biosynthesis are types 1 and VII, which reduce estrone to estradiol. Corticotropin (Adrenocorticotropic hormone, ACTH) acts through the ACTH receptor called melanocortin receptor type 2 (MC2R) to stimulate steroidogenesis, increasing the production of androgens (McKenna et al, 1997). In males, Lutropin (LH) stimulates testosterone production.
			R-HSA-193065 (Reactome)	22beta-hydroxycholesterol, NADPH + H+, and O2 react to form 20alpha,22beta-hydroxycholesterol, NADP+ and H2O, catalyzed by CYP11A (P450scc) associated with the inner mitochondrial membrane.
			R-HSA-193068 (Reactome)	Pregnenolone (PREG) and NADPH + H+ react to form 17alpha-hydroxypregnenolone (17aHPREG), NADP+, and H2O. Steroid 17 alpha hydroxylase/17,20 lyase (CYP17A1), associated with the endoplasmic reticulum membrane, catalyzes this reaction.
			R-HSA-193070 (Reactome)	17-alpha-hydroxypregnenolone, NADPH + H+, and O2 react to form DHA (dehydroepiandrostenedione), NADP+, H2O, and acetaldehyde. CYP17 (which also catalyzes 17-alpha-hydroxylation) catalyzes this lyase reaction. There are marked species differences in which substrate is used for this lyase activity. The human enzyme prefers 17alpha-pregnenolone (delta5 steroid) as substrate (Brock, BJ, Waterman, MR, 1999). Corticotropin (Adrenocorticotropic hormone, ACTH) acts through the ACTH receptor called melanocortin receptor type 2 (MC2R) to stimulate steroidogenesis, increasing the production of androgens (McKenna et al, 1997).
			R-HSA-193072 (Reactome)	Progesterone (P4), NADPH + H+, and O2 react to form 17alpha-hydroxyprogesterone (17aHPROG), NADP+, and H2O. This reaction is catalyzed by steroid 17 alpha hydroxylase/17,20 lyase (CYP17A1), associated with the endoplasmic reticulum membrane.
			R-HSA-193073 (Reactome)	In this two-step reaction catalyzed by 3beta-HSD associated with the endoplasmic reticulum membrane, the 3-hydroxyl group of DHA is oxidized to a keto group and the double bond in the steroid nucleus is then isomerized from the five to the 4 position. Corticotropin (Adrenocorticotropic hormone, ACTH) acts through the ACTH receptor called melanocortin receptor type 2 (MC2R) to stimulate steroidogenesis, increasing the production of androgens (McKenna et al, 1997).
			R-HSA-193097 (Reactome)	Pregenolone is translocated from the mitochondrial matrix to the cytosol. Neither transport proteins to mediate its movement across the inner mitochondrial membrane nor carrier proteins to facilitate its movement in the cytosol have been identified, and the mechanism of this translocation is unknown.
			R-HSA-193099 (Reactome)	17Alpha-hydroxyprogesterone (17aHPROG), NADPH + H+, and O2 react to form 4-Androstene-3, 17-dione (ANDST), NADP+, H2O, and acetaldehyde. Steroid 17 alpha hydroxylase/17,20 lyase (CYP17A1), which also catalyzes 17-alpha-hydroxylation, catalyzes this lyase reaction.
			R-HSA-193101 (Reactome)	20alpha,22beta-hydroxycholesterol (20a,22b-DHCHOL), NADPH + H+, and O2 react to form pregnenolone (PREG), isocaproaldehyde (ISCAL), NADP+ and H2O. This cleavage reaction is catalysed by CYP11A (P450scc) associated with the inner mitochondrial membrane (Strushkevich et al. 2011). PREG is substantially more hydrophilic than cholesterol (CHOL) and hydroxycholesterol (HCHOL) and is released into the mitochondrial matrix.
			R-HSA-193143 (Reactome)	The conversion of testosterone to estradiol is catalyzed by aromatase (CYP19A1) associated with the endoplasmic reticulum membrane.
			R-HSA-193961 (Reactome)	Pregn-5-ene-3,20-dione-17-ol isomerizes to 17-hydroxyprogesterone. This reaction is catalyzed by the isomerase activity of 3 beta-HSD, associated with the endoplasmic reticulum membrane. The active form of the enzyme is a homodimer. The enzyme occurs in two isoforms that are similar in their biochemical properties but differ in their tissue expression: type I (HSD3B1) is found in placenta and skin, while type II (HSD3B2) is found in the adrenal glands and gonads.
			R-HSA-193964 (Reactome)	Progesterone, NAPDH + H+, and O2 react to form 11-deoxycorticosterone, NADP+ and H2O. This reaction is catalyzed by CYP21A2 associated with the endoplasmic reticulum membrane.
			R-HSA-193965 (Reactome)	18-Hydroxycorticosterone and NADPH + H+ react to form aldosterone, NADP+, and H2O. This reaction is catalyzed by CYP11B2 associated with the inner mitochondrial membrane.
			R-HSA-193981 (Reactome)	17-Hydroxyprogesterone, NADPH + H+, and O2 react to form 11-deoxycortisol, NADP+, and H2O. This reaction is catalyzed by CYP21A2 (steroid 21-hydroxylase) associated with the endoplasmic reticulum membrane.
			R-HSA-193995 (Reactome)	Corticosterone, NADPH + H+, and O2 react to form 18-hydroxycorticosterone, NADP+, and H2O. This reaction is catalyzed by CYP11B2 associated with the inner mitochondrial membrane.
			R-HSA-193996 (Reactome)	11-deoxycorticosterone is synthesized in a reaction at the endoplasmic reticulum membrane and is further metabolized, ultimately to yield aldosterone, in reactions catalyzed by mitochondrial enzymes. The means by which 11-deoxycorticosterone translocates into the mitochondrial matrix, however, is unknown.
			R-HSA-193997 (Reactome)	Cytochrome P450 11B1, mitochondrial (CYP11B1) usually hydroxylates 11-deoxycortisol (11DCORT) to form cortisol (CORT). CYP11B1 is associated with the inner mitochondrial membrane. Corticotropin (Adrenocorticotropic hormone, ACTH) acts through the ACTH receptor, melanocortin receptor type 2 (MC2R) to stimulate steroidogenesis, increasing the production of androgens (McKenna et al, 1997).
			R-HSA-194017 (Reactome)	Cytochrome P450 11B2, mitochondrial (CYP11B2 aka aldosterone hydroxylase) is an enzyme necessary for aldosterone biosynthesis via corticosterone (CORST) and 18-hydroxycorticosterone (18HCORST). The 11-beta oxidation of 11-deoxycorticosterone (11DCORST) leads to corticosterone (CORST) and 18-hydroxylation of this leads to 18-hydroxycorticosterone (18HCORST). 18-oxidation of 18HCORST yields aldosterone.
			R-HSA-194023 (Reactome)	Cortisol and NADP+ react to form cortisone, NADPH, and H+. This reaction is catalyzed by 11beta-hydroxysteroid dehydrogenases 11B1 and B2 (HSD11B1, B2), associated with the endoplasmic reticulum membrane. The conversion of cortisol (CORT), an active hormone, into inactive cortisone (COR) occurs in many tissues in the body, notably in the liver, and appears to play a role in regulating cortison activity (Tannin et al. 1991, Stewart et al. 1987).
			R-HSA-194025 (Reactome)	11-deoxycortisol is synthesized in a reaction at the endoplasmic reticulum membrane and is further metabolized to cortisol in a reaction catalyzed by mitochondrial enzymes. The means by which 11-deoxycortisol translocates into the mitochondrial matrix, however, is unknown.
			R-HSA-194036 (Reactome)	Cortisol is translocated from the mitochondrial matrix into the cytosol by an unknown mechanism.
			R-HSA-196060 (Reactome)	Isocaproaldehyde is reduced by NADPH + H+ to yield 4-methylpentan-1-ol and NADP+. This cytosolic reaction is catalyzed by AKR1B1 (aldose reductase). The purified human enzyme has been shown to catalyze this reaction efficiently in vitro; its abundance in adrenal tissue in humans and other mammals and its concordant expression with other enzymes of steroid hormone synthesis are consistent with it performing this role in vivo as well (Matsuura et al. 1996; Lefrancois-Martinez et al. 2004). The metabolic fate of 4-methylpentan-1-ol is unknown.
			R-HSA-196086 (Reactome)	Cholesterol is released from its complex with STAR in the mitochondrial intermembrane space. The mechanism of this process in vivo remains incompletely understood.
			R-HSA-196125 (Reactome)	Isocaproaldehyde (4-methylpentanal) is translocated from the mitochondrial matrix to the cytosol. The transporter that mediates this reaction is unknown. The reaction is inferred to exist because isocaproaldehyde is generated within the mitochondrion while the enzyme that reduces it to the corresponding alcohol is located in the cytosol (Matsuura et al. 1996).
			R-HSA-196126 (Reactome)	Cholesterol traverses the cytosol and the mitochondrial intermembrane space complexed with carrier proteins. This process is essential for the synthesis of steroid hormones in humans. Nevertheless, molecular details of the transport process remain incompletely understood. A plausible model, supported by studies in vitro and in cells overexpressing cloned human proteins, is that cytosolic STAR-related proteins STARD4, 5, and 6 bind cholesterol liberated from lysosomes or cytosolic lipid droplets and carry it to the outer mitochondrial membrane (Rodriguez-Aguado et al. 2005; Soccio et al. 2002), where it is transferred to STAR protein and carried across the mitochondrial intermembrane space (Miller 2007). Mutations in the gene encoding STAR block synthesis of all steroid hormones in humans, indicating the critical importance of this transport step in the biosynthetic process (Bose et al. 1996). The transport step is also a key site for normal regulation of steroid hormone synthesis, as STAR protein is unstable and its synthesis is up-regulated in response to signals such as the binding of ACTH to its receptors on adrenal cells (Stocco 2001).
			R-HSA-196350 (Reactome)	Pregnenolone and NAD+ react to form pregn-5-ene-3,20-dione and NADH + H+. This reaction is catalyzed by the 3 beta-hydroxysteroid activity of 3-beta-hydroxysteroid dehydrogenase/isomerase (HSD3B) enzyme associated with the endoplasmic reticulum membrane. The active form of the enzyme is a homodimer. The enzyme occurs in two isoforms that are similar in their biochemical properties but differ in their tissue expression: type I (HSD3B1) is found in placenta and skin, while type II (HSD3B2) is found in the adrenal glands and gonads.
			R-HSA-196372 (Reactome)	17-Hydroxypregnenolone and NAD+ react to form pregn-5-ene-3,20-dione-17-ol and NADH + H+. This reaction is catalyzed by the 3 beta-hydroxysteroid activity of 3-beta-hydroxysteroid dehydrogenase/isomerase (HSD3B) enzyme associated with the endoplasmic reticulum membrane. The active form of the enzyme is a homodimer. The enzyme occurs in two isoforms that are similar in their biochemical properties but differ in their tissue expression: type I (HSD3B1) is found in placenta and skin, while type II (HSD3B2) is found in the adrenal glands and gonads.
			R-HSA-209738 (Reactome)	Vitamin D metabolites are lipophilic and must be transported in the circulation bound to plasma proteins. Vitamin D3 is transported to the liver bound to a plasma protein called vitamin D binding protein (DBP).
			R-HSA-209754 (Reactome)	The skin's exposure to UV rays from sunlight induces the photolytic cleavage of 7-dehydrocholesterol to previtamin D3. This is followed by thermal isomerization to form vitamin D3 (Cholecalciferol).
			R-HSA-209760 (Reactome)	The internalized complex enters the lysosome where it can be acted upon the protease legumain.
			R-HSA-209765 (Reactome)	Calcitriol (1,25(OH)2-D3) is biologically inactivated through a series of reactions beginning with 24-hydroxylation and is most likely a mechanism of elimination. 24-Hydroxylation of the vitamin D metabolites is largely regulated inversely to 1-hydroxylation, the initial step towards activation.
			R-HSA-209766 (Reactome)	Once out of the lysosome, calcidiol binds to intracellular vitamin D binding protein (IDBP) which facilitates the localization of vitamin D metabolites in the cell. IDBPs are related to the hsc-70 family of heat shock proteins and demonstrate a high nucleotide homology to that family. No IDBP protein has been documented yet so IDBP has not been annotated.
			R-HSA-209845 (Reactome)	To be functionally active, vitamin D is required to be dihydroxylated. The first hydroxylation at position 25 is carried out by vitamin D 25-hydroxylase (CYP2R1) in the liver, forming calcidiol (CDL) (Shinkyo et al. 2004).
			R-HSA-209868 (Reactome)	The second step in vitamin D3 activation requires hydroxylation of 25-hydroxyvitamin D3 (calcidiol, CDL) to 1alpha-25-dihydroxyvitamin D3 (calcitriol, CTL). This conversion is mediated by 25-hydroxyvitamin D-1alpha hydroxylase (CYP27B1) (Zehnder et al. 2002, Fritsche et al. 2003).
			R-HSA-209944 (Reactome)	Vitamin D binding protein (DBP), a plasma protein, carries the vitamin D metabolites in the circulation. Calcidiol translocates to the extracellular region where it binds with DBP and is transported to the kidney.
			R-HSA-350147 (Reactome)	Once vitamin D3 is released from DBP, it becomes available for hydroxylation.
			R-HSA-350158 (Reactome)	Mammalian legumain (asparagine-specific endoprotease) is a subfamily of cysteine proteases with no homology to other known proteases and is found in a wide range of organisms from parasites to plants and animals. Legumain requires acidic conditions for its degradative activity and has strict specificity for cleavage with an asparagine residue in the P1 site. Cubilin, once released from the complex, cycles back to the cell surface. Calcidiol also becomes available for further processing.
			R-HSA-350168 (Reactome)	Megalin (glycoprotein 330) is a member of the low density lipoprotein receptor family and is abundant in kidney proximal tubules. Megalin mediates the endocytic uptake of DBP:Calcidiol complexes to prevent loss of calcidiol in urine.
			R-HSA-350186 (Reactome)	Cubilin (CUBN) is a membrane-associated protein colocalizing with megalin. Its function is to sequester steroid carrier complexes such as vitamin D binding protein:calcidiol (GC:CDL) on the cell surface before megalin mediates their internalization (Nykjaer et al. 2001).
			R-HSA-469659 (Reactome)	The conversion of testosterone to the most potent androgen, 5-alpha-dihydrotestosterone (DHT), is catalyzed by the microsomal 5alpha-steroid reductase enzymes, of which there are three reported types in humans to date (SRD5A1-3) (Andersson S and Russell DW, 1990; Andersson S et al, 1991; Uemura M et al, 2008 respectively). These enzymes are expressed in the prostate and other androgen target sites. Defects in SRD5A2 are the cause of pseudovaginal perineoscrotal hypospadias, also known as male pseudohermaphroditism (Anwar R et al, 1997). Corticotropin (Adrenocorticotropic hormone, ACTH) acts through the ACTH receptor called melanocortin receptor type 2 (MC2R) to stimulate steroidogenesis, increasing the production of androgens (McKenna et al, 1997).
			R-HSA-804969 (Reactome)	Expression of HSD17B1 which is the main enzyme that catalyzes the hydrogenation of estrone is strongly restricted to placenta, ovaries, endometrium and breast tissue (Moeller and Adamski, 2009).
SRD5A1-3		mim-catalysis	R-HSA-469659 (Reactome)
	STAR	Arrow	R-HSA-196086 (Reactome)
STAR			R-HSA-196126 (Reactome)
	StAR-related cholesterol-binding proteins	Arrow	R-HSA-196126 (Reactome)
	TEST	Arrow	R-HSA-193064 (Reactome)
TEST			R-HSA-193143 (Reactome)
TEST			R-HSA-469659 (Reactome)
	VD3	Arrow	R-HSA-209754 (Reactome)
	VD3	Arrow	R-HSA-350147 (Reactome)
VD3			R-HSA-209738 (Reactome)
VD3			R-HSA-209845 (Reactome)
	cholesterol:STAR	Arrow	R-HSA-196126 (Reactome)
cholesterol:STAR			R-HSA-196086 (Reactome)
cholesterol:StAR-related protein			R-HSA-196126 (Reactome)
	cholesterol	Arrow	R-HSA-196086 (Reactome)
cholesterol			R-HSA-193054 (Reactome)
	pregn-5-ene-3,20-dione-17-ol	Arrow	R-HSA-196372 (Reactome)
pregn-5-ene-3,20-dione-17-ol			R-HSA-193961 (Reactome)
	pregn-5-ene-3,20-dione	Arrow	R-HSA-196350 (Reactome)
pregn-5-ene-3,20-dione			R-HSA-193052 (Reactome)

Metabolism of steroid hormones (Homo sapiens)

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