11β-Hydroxysteroid dehydrogenase

11β-Hydroxysteroid dehydrogenase (HSD-11β or 11β-HSD) enzymes catalyze the conversion of inert 11 keto-products (cortisone) to active cortisol, or vice versa,^[1] thus regulating the access of glucocorticoids to the steroid receptors.

The human genome encodes two distinct HSD-11β isozymes (

11-oxosteroid by reducing NADP⁺ or NAD⁺. HSD-11βs are part of the larger class of oxidoreductases and HSD-11β Type 1 has oxidoreductase activity (the reverse of dehydrogenase activity). HSD-11βs participate in c21-steroid hormone metabolism and androgen and estrogen

metabolism.

Structural studies

Several structures for HSD-11β Type 1 have been solved to date with various mutations and inhibitors. There are no known structures for HSD-11β Type 2.

Function

Cortisol. Note the OH at the 11 position on ring C. (The other differences between the diagrams are not of consequence.)

Licorice, which contains glycyrrhizinic acid and enoxolone, can inhibit HSD-11β and lead to the apparent mineralocorticoid excess syndrome

. Cortisol levels consequently rise, and cortisol binding to the mineralocorticoid receptor produces clinical signs and symptoms of hypokalemia, alkalosis and hypertension (i.e., mineralocorticoid excess).

Isozymes

In humans, there are two 11β-HSD isozymes:[3]^[4]^[5]

Enzyme	Gene	Cofactor Dependence	Expression	Reactions catalyzed
HSD-11β Type 1	HSD11B1	NADPH -dependent	Highly expressed in key metabolic tissues including liver, adipose tissue, and the central nervous system.	Reduces cortisone to cortisol.
HSD-11β Type 2	HSD11B2	NAD⁺-dependent	Expressed in HSD2 neurons and placenta.	Oxidizes cortisol to cortisone.

Clinical Application

HSD-11βs are enzymes involved in steroid hormone physiology. HSD-11β Type 1 is found in metabolic tissues targeted by glucocorticoids and converts cortisone to active cortisol.^[6] HSD-11β Type 1 acts as a reductase producing active cortisol and the amplification of glucocorticoids. This enzyme is most abundant in the liver but can be found in most tissues in the body. HSD11B- Type 1 amplifies glucocorticoid concentrations in the liver and adipose tissue, glucocorticoid excess induces obesity with other features such as hypertension and diabetes mellitus.^[7]

HSD-11β Type 2 is expressed by aldosterone-selective tissues and protects the mineralocorticoid receptor from the activation by cortisol by converting it to cortisone using the enzyme 11-Oxoreductase. HSD-11β Type 2 protects tissues from continuous activation by decreasing local cortisol levels and preventing 11-Oxoreductase from activating.^[6] In tissues that do not express the mineralocorticoid receptor, such as the placenta and testis, it protects cells from the growth-inhibiting and/or pro-apoptotic effects of cortisol, particularly during embryonic development. Mutations in this gene cause the syndrome of apparent mineralocorticoid excess and hypertension.^[8]

Since the main functions of HSD-11βs are for the regulation of glucocorticoids, the two isozymes are linked to various overstimulation or depletion of glucocorticosteroids that result in chemical imbalances in the human body. The effects of the enzyme as it relates to specific body functions and its associated disorders are listed below.

Effect of Hyperlipidemia on 11β-hydroxysteroid-dehydrogenase

Hyperlipidemia has a great effect on 11β-hydroxysteroid-dehydrogenase.^[9] Glucocorticoid is dependent on Glucocorticoid plasma concentration, cellular glucocorticoid receptor expression and the pre-receptor hormone metabolism that is catalyzed by 11β-HSD.^[9] There are two types of 11β-Hydroxysteroid dehydrogenases that control cortisol concentration: HSD-11β Type 1 and HSD-11β Type 2.^[9] HSD-11β Type 1 is responsible for converting cortisone to cortisol by acting as an oxo-reductase because it is NADP(H) dependent, while HSD-11β Type 2 inactivates cortisol to cortisone via NAD.^[9] 10-d hyperlipidemia increases the HSD-11β Type 1 expression in visceral and subcutaneous adipose tissues.^[9] Hyperlipidemia decreases HSD-11β Type 2 expression in the liver and adipose tissue.^[9] Hyperlipidemia has a great influence on HSD-11β Type 1 and HSD-11β Type 2.^[9] This demonstrates that there is likely a relationship between hyperlipidemia and cortisol metabolism.^[9] Cushing's Disease, synonymous with hypercortisolism, involves overwhelming the cortisol-neutralizing ability of 11β-HSD2 with high concentrations of cortisol.^[10] This allows cortisol to outcompete aldosterone and bind to mineralocorticoid receptors, resulting in the activation of several pathways that increase blood pressure.^[11]

Activity of HSD-11βs in organs

HSD-11βs are active in organs and in the adrenal gland.^[12] The two isoenzymes take on various duties.^[12] During an active state, HSD-11β promotes the increase in glucocorticoids in the hepatocytes and also enhances gluconeogenesis.^[12] The type 2 isozyme converts active glucocorticoid hormones to inactive metabolites in target tissues such as kidney, salivary glands, intestines, etc.^[12] The activation of the two isozymes of HSD-11β in the kidneys and liver triggers the extra-adrenal formation in alloxan diabetes, which affiliates with the reduction in the synthesis of glucocorticoid hormones in the adrenal glands.^[12] The extra-adrenal formation leads to the increased local formation of corticosterone in the liver and has a high activity of reactions with gluconeogenesis.^[12] These gluconeogenesis reactions add to the continued metabolic disorders similar to that of diabetes.^[12] Thus HSD-11β Type 1 can serve as a potential treatment agents for diabetes, obesity, and metabolic syndrome due to increasing local corticosterone.^[12]

Involvement in the brain

HSD-11βs are expressed in the central nervous system of aged individuals.^[13] It is essential in Hypothalamo-Pituitary-Adrenal Axis function.^[13] HSD-11βs also partakes involvement in the decline of conscious intellectual activity due to aging.^[13] The enzyme also contributes to central effects are also during the development stages.^[13] For instance, the HSD-11βs Type 2shows frequently in fetal tissues such as a newborn's brain and placenta.^[13] If there is an absence or decline in HSD-11βs Type 2 in the fetus tissues, there are negative developmental consequences such as anxiety.^[13]

HSD-11βs are partly responsible for intracellular metabolism that determine the operation of glucocorticoids within cells.^[13] Glucocorticoids impact the brain development and ultimately the function of the central nervous system.^[13] So much so, that if there is a surplus or scant amounts of it, the consequences are deformities throughout one's entire life.^[13] HSD-11β Type 1 is responsible for activating glucocorticoids while HSD-11β Type 2 is responsible for deactivating them.^[13] The consequences for HSD-11β Type 1 activating glucocorticoids is that there is a decline in cognition especially as one ages.^[13] Contrarily, the effects of HSD-11β Type 2 occur during development.^[13] Some consequences of a high expression HSD-11β Type 2 are anxiety and cardiometabolic disorders, both of which are part of the early age glucocorticoid programming.^[13]

Involvement in Preterm Births

Infants born underweight are susceptible to having metabolic disease throughout their lives.^[14] The presence of glucocorticoids has contributed to the relatively low infant birth weight.^[14] A decrease in HSD-11β Type 2 in the placenta can lead to infant restriction in growth, specifically during the first 12 months of an infant's life.^[14] The reason for this is because the HSD-11β Type 2 is meant to be expressed in high quantities in the placenta, This is so because the enzymes secure the fetus from exposure to increased levels of glucocorticoids, which are linked to underweight newborns.^[14]

References

PMID 11250914
.

OCLC 1129099861
.

PMID 10232052
.

S2CID 46477930
.

PMID 19470627
.

^ ^a ^b Lindsay, Kaitlin. "Kaitlin Lindsay: Medical & Scientific Illustration". kaitlinlindsay.com. Archived from the original on 2019-04-22.

S2CID 72573025
.

^ "HSD11B2 Gene". www.greencards.org.

^
PMID 20688460. Archived from the original
(PDF) on 2018-07-19. Retrieved 2019-12-11.

PMID 20829617
.

S2CID 14749847
.

^
S2CID 24224772
.

^
PMID 21144857
.

^
PMID 24517145
.

Agarwal AK, Monder C, Eckstein B, White PC (1989). "Cloning and expression of rat cDNA encoding corticosteroid 11 beta-dehydrogenase". J. Biol. Chem. 264 (32): 18939–43.
PMID 2808402
.

Bush IE, Hunter SA, Meigs RA (1968). "Metabolism of 11-oxygenated steroids. Metabolism in vitro by preparations of liver". Biochem. J. 107 (2): 239–58.
PMID 4384445
.

Lakshmi V, Monder C (1988). "Purification and characterization of the corticosteroid 11 beta-dehydrogenase component of the rat liver 11 beta-hydroxysteroid dehydrogenase complex". Endocrinology. 123 (5): 2390–8.
PMID 3139396
.

Phillips DM, Lakshmi V, Monder C (1989). "Corticosteroid 11 beta-dehydrogenase in rat testis". Endocrinology. 125 (1): 209–16.
PMID 2661206
.

External links

11-beta-Hydroxysteroid+Dehydrogenases at the U.S. National Library of Medicine Medical Subject Headings (MeSH)

v
t
e
Oxidoreductases: alcohol oxidoreductases (EC 1.1)
1.1.1: NAD/NADP acceptor

3-hydroxyacyl-CoA dehydrogenase

3-hydroxybutyryl-CoA dehydrogenase

Alcohol dehydrogenase

Aldo-keto reductase
1A1

1B1

1B10

1C1

1C3

1C4

7A2

Aldose reductase

Beta-Ketoacyl ACP reductase

Carbohydrate dehydrogenases

Carnitine dehydrogenase

D-malate dehydrogenase (decarboxylating)

DXP reductoisomerase

Glucose-6-phosphate dehydrogenase

Glycerol-3-phosphate dehydrogenase

HMG-CoA reductase

IMP dehydrogenase

Isocitrate dehydrogenase

Lactate dehydrogenase

L-threonine dehydrogenase

L-xylulose reductase

Malate dehydrogenase

Malate dehydrogenase (decarboxylating)

Malate dehydrogenase (NADP+)

Malate dehydrogenase (oxaloacetate-decarboxylating)

Malate dehydrogenase (oxaloacetate-decarboxylating) (NADP+)

Phosphogluconate dehydrogenase

Sorbitol dehydrogenase

3β

3β-HSD

NSDHL

11β

11β-HSD1

11β-HSD2

17β

1.1.2: cytochrome acceptor

D-lactate dehydrogenase (cytochrome)

D-lactate dehydrogenase (cytochrome c-553)

Mannitol dehydrogenase (cytochrome)

1.1.3: oxygen acceptor

Glucose oxidase

L-gulonolactone oxidase

Xanthine oxidase

Alcohol oxidase

1.1.4: disulfide as acceptor

Vitamin K epoxide reductase

Vitamin-K-epoxide reductase (warfarin-insensitive)

1.1.5: quinone/similar acceptor

Malate dehydrogenase (quinone)

Quinoprotein glucose dehydrogenase

1.1.99: other acceptors

Choline dehydrogenase

L2HGDH

steroid metabolism
Mevalonate pathway
To HMG-CoA

Acetyl-Coenzyme A acetyltransferase

HMG-CoA synthase
(regulated step)

Ketogenesis

HMG-CoA lyase

3-hydroxybutyrate dehydrogenase

Thiophorase

To Mevalonic acid

HMG-CoA reductase

To DMAPP

Mevalonate kinase

Phosphomevalonate kinase

Pyrophosphomevalonate decarboxylase

Isopentenyl-diphosphate delta isomerase

Geranyl-

Dimethylallyltranstransferase

Geranyl pyrophosphate

To cholesterol
To lanosterol

Farnesyl-diphosphate farnesyltransferase

Squalene monooxygenase

Lanosterol synthase

7-Dehydrocholesterol path

Lanosterol 14α-demethylase

Sterol-C5-desaturase-like

7-Dehydrocholesterol reductase

Desmosterol path

24-Dehydrocholesterol reductase

To Bile acids

Cholesterol 7α-hydroxylase

Sterol 27-hydroxylase

Steroidogenesis
To pregnenolone

Cholesterol side-chain cleavage

To corticosteroids

aldosterone: 18-Hydroxylase

cortisol/cortisone: 17α-Hydroxylase

11β-HSD
1

2

both: 3β-HSD
1

2

21-Hydroxylase

11β-Hydroxylase

To sex hormones
To androgens

17α-Hydroxylase

17,20-Lyase

3β-HSD

17β-HSD

5α-Reductase

1

2

To estrogens

Aromatase

17β-HSD

Other/ungrouped

Steroid metabolism: sulfatase

Steroid sulfatase

sulfotransferase
SULT1A1

SULT2A1

Steroidogenic acute regulatory protein

Cholesterol total synthesis

Reverse cholesterol transport

v
t
e
Enzymes
Activity

Active site

Binding site

Catalytic triad

Oxyanion hole

Enzyme promiscuity

Diffusion-limited enzyme

Cofactor

Enzyme catalysis

Regulation

Allosteric regulation

Cooperativity

Enzyme inhibitor

Enzyme activator

Classification

EC number

Enzyme superfamily

Enzyme family

List of enzymes

Kinetics

Enzyme kinetics

Eadie–Hofstee diagram

Hanes–Woolf plot

Lineweaver–Burk plot

Michaelis–Menten kinetics

Types

EC1 Oxidoreductases (list)

EC2 Transferases (list)

EC3 Hydrolases (list)

EC4 Lyases (list)

EC5 Isomerases (list)

EC6 Ligases (list)

EC7 Translocases (list)

Portal:
Biology

Retrieved from "https://en.wikipedia.org/w/index.php?title=11β-Hydroxysteroid_dehydrogenase&oldid=1214424098"

[pmid11250914-1] PMID 11250914
.

[2] OCLC 1129099861
.

[pmid10232052-3] PMID 10232052
.

[pmid9000459-4] S2CID 46477930
.

[JCEM-5] PMID 19470627
.

[:3-6] Lindsay, Kaitlin. "Kaitlin Lindsay: Medical & Scientific Illustration". kaitlinlindsay.com. Archived from the original on 2019-04-22.

[7] S2CID 72573025
.

[8] "HSD11B2 Gene". www.greencards.org.

[:0-9] 
PMID 20688460. Archived from the original
(PDF) on 2018-07-19. Retrieved 2019-12-11.

[10] PMID 20829617
.

[11] S2CID 14749847
.

[:1-12] 
S2CID 24224772
.

[:2-13] 
PMID 21144857
.

[:4-14] 
PMID 24517145
.

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