Antimineralocorticoid

Skeletal formulae of aldosterone antagonists

An antimineralocorticoid, or an aldosterone antagonist, is a diuretic drug which antagonizes the action of aldosterone at mineralocorticoid receptors. This group of drugs is often used as adjunctive therapy, in combination with other drugs, for the management of chronic heart failure. Spironolactone, the first member of the class, is also used in the management of hyperaldosteronism (including Conn's syndrome) and female hirsutism (due to additional antiandrogen actions). Most antimineralocorticoids, including spironolactone, are steroidal spirolactones. Finerenone is a non-steroidal antimineralocorticoid.

Mechanism of action

Aldosterone antagonists are, as the name suggests, receptor antagonists at the mineralocorticoid receptor. Antagonism of these receptors inhibits sodium resorption in the collecting duct of the nephron in the kidneys. This interferes with sodium/potassium exchange, reducing urinary potassium excretion and weakly increasing water excretion (diuresis).^[1]

In congestive heart failure, they are used in addition to other drugs for additive diuretic effect, which reduces edema and the cardiac workload.

Examples

Members of this class in clinical use include:

Widespread use
- Spironolactone — the first and most widely used member of this class
- Eplerenone — much more selective than spironolactone on target, but somewhat less potent and efficacious
Uncommon use (to date)
- Canrenone and potassium canrenoate — very limited use
- Finerenone — non-steroidal and more potent and selective than either eplerenone or spironolactone

Some drugs also have antimineralocorticoid effects secondary to their main mechanism of actions. Examples include progesterone, drospirenone, gestodene, and benidipine.^[2]

References

↑ Rossi S, editor. Australian Medicines Handbook 2006. Adelaide: Australian Medicines Handbook; 2006.
↑ Kosaka H, Hirayama K, Yoda N, Sasaki K, Kitayama T, Kusaka H, Matsubara M (2010). "The L-, N-, and T-type triple calcium channel blocker benidipine acts as an antagonist of mineralocorticoid receptor, a member of nuclear receptor family". Eur. J. Pharmacol. 635 (1-3): 49–55. doi:10.1016/j.ejphar.2010.03.018. PMID 20307534.

External links

Aldosterone Antagonists at the US National Library of Medicine Medical Subject Headings (MeSH)
MeSH list of agents 82000451

Mineralocorticoids and antimineralocorticoids (H02)

Mineralocorticoids	11-Deoxycorticosterone (desoxycortone) 11-Deoxycortisol (cortodoxone) Aldosterone Corticosterone Cortisol (hydrocortisone) Desoxycortone acetate Desoxycortone enanthate Fludrocortisone Fludrocortisone acetate

Antimineralocorticoids	Steroidal: Canrenoate potassium (potassium canrenoate) Canrenoic acid Canrenone Drospirenone Dydrogesterone Eplerenone Gestodene Progesterone Quingestrone Spironolactone Non-steroidal: Amlodipine Benidipine Felodipine Finerenone Nifedipine Nimodipine Nitrendipine

Synthesis modifiers	Acetoxolone Aminoglutethimide Carbenoxolone Enoxolone Ketoconazole Metyrapone Mitotane Trilostane

^#WHO-EM ^‡Withdrawn from market Clinical trials: ^†Phase III ^§Never to phase III See also: Androgens and antiandrogens • Estrogens and antiestrogens • Progestogens and antiprogestogens • Glucocorticoids and antiglucocorticoids

Antihypertensives: diuretics (C03)

Sulfonamides
(and etacrynic acid)

CA inhibitors (at PT)	Acetazolamide

Loop (Na-K-Cl at AL)	Furosemide^# Bumetanide Etacrynic acid Etozolin Muzolimine Ozolinone Piretanide Tienilic acid Torasemide

Thiazides (Na-Cl at DCT, Calcium-sparing)	Altizide Bendroflumethiazide Chlorothiazide Cyclopenthiazide Cyclothiazide Epitizide Hydrochlorothiazide^# Hydroflumethiazide Mebutizide Methyclothiazide Polythiazide Trichlormethiazide

Thiazide-likes (primarily DCT)	Quinethazone Clopamide Chlortalidone Mefruside Clofenamide Metolazone Meticrane Xipamide Indapamide Clorexolone Fenquizone

Potassium-sparing (at CD)

ESC blockers	Amiloride^# Triamterene Benzamil

Aldosterone antagonists	Spirolactones: Spironolactone^# Eplerenone Potassium canrenoate Canrenone Non-steroidal: Finerenone

Osmotic diuretics (PT, DL)

Vasopressin receptor inhibitors
(DCT and CD)

Other

Ethanol, Isopropanol, 2M2B
mercurial diuretics (Chlormerodrin, Mersalyl, Meralluride)
Theobromine
Cicletanine

^#WHO-EM
^‡Withdrawn from market
Clinical trials:
- ^†Phase III
- ^§Never to phase III

Mineralocorticoid receptor modulators

Agonists	11-Deoxycorticosterone (desoxycortone) 11-Deoxycortisol (cortodoxone) 16α,18-Dihydroxy-11-deoxycorticosterone 17α-Hydroxyaldosterone 18-Hydroxy-11-deoxycorticosterone 19-Norprogesterone Aldosterone Corticosterone Desoxycortone acetate Desoxycortone enanthate Desoxycortone glucoside Desoxycortone pivalate Hydrocortisone (cortisol) Fludrocortisone Fludrocortisone acetate Mometasone furoate Prednisolone Prednisone

Antagonists	Steroidal: 3α-Hydroxytibolone 3β-Hydroxytibolone 6β-Hydroxy-7α-thiomethylspironolactone 7α-Thiomethylspironolactone 17α-Hydroxyprogesterone 18-Deoxyaldosterone Canrenoate potassium (potassium canrenoate) Canrenoic acid Canrenone Dicirenone Dimethisterone Drospirenone Dydrogesterone Eplerenone Gestodene Guggulsterone Medrogestone Mespirenone Mexrenoate potassium Mexrenoic acid Mexrenone Oxprenoic acid Oxprenoate potassium (RU-28318) Pregnenolone Progesterone Prorenoate potassium Prorenoic acid (prorenoate) Prorenone RO-14-9012 RU-26752 SC-5233 SC-8109 SC-11927 SC-19886 SC-24813 SC-25152 SC-26519 SC-27169 Spirorenone Spironolactone Spiroxasone Tibolone Trimegestone ZK-91587 ZK-97894 Non-steroidal: Amlodipine Apararenone Benidipine BR-4628 Esaxerenone Felodipine Finerenone Nifedipine Nimodipine Nitrendipine PF-03882845 SM-368229

See also: Androgenics • Estrogenics • Glucocorticoidics • Progestogenics • Steroid hormone metabolism modulators

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