Everything about Mineralocorticoid totally explained
Mineralocorticoids are a class of
steroid hormones characterised by their similarity to
aldosterone and their influence on
salt and water balance.
Physiology
The name
mineralocorticoid derives from early observations that these hormones were involved in the retention of
sodium, a
mineral. The primary
endogenous mineralocorticoid is
aldosterone, although a number of other endogenous hormones (including
progesterone and
deoxycorticosterone) have mineralocorticoid function.
Aldosterone acts on the kidneys to provide active reabsorption of
sodium and an associated passive reabsorption of
water, as well as the active secretion of
potassium in the principal cells of the cortical
collecting tubule and active secretion of
protons via proton
ATPases in the lumenal membrane of the
intercalated cells of the
collecting tubule. This in turn results in an increase of
blood pressure and
blood volume.
Aldosterone is produced in the cortex of the
adrenal gland and its secretion is mediated principally by
angiotensin II, but also by
adrenocorticotrophic hormone (ACTH) and local
potassium levels.
Mode of Action
Mineralocorticoids bind to the cytosolic
mineralocorticoid receptor. This type of
receptor gets activated upon
ligand binding. After a hormone binds to the corresponding receptor, the newly formed
receptor-ligand complex tes itself into the
cell nucleus, where it binds to many hormone response elements (
HRE) in the
promoter region of the target
genes in the
DNA.
The opposite mechanism is called
transrepression. The
hormone receptor without ligand binding interacts with
heat shock proteins and prevents the
transcription of targeted genes.
Aldosterone and
cortisol have similar affinity for the mineralocorticoid receptor however, glucocorticoids circulate at roughly 100 times the level of mineralocorticoids. An enzyme exists in mineralocorticoid target tissues to prevent overstimulation by glucocorticoids. This enzyme,
11-beta hydroxysteroid dehydrogenase type II, catalyzes the deactivation of glucocorticoids to 11-dehydro metabolites.
Licorice is known to be an inhibitor of this enzyme and chronic consumption can result in a condition known as
pseudohyperaldosteronism.
18 hydroxy 11 deoxycorticosterone (also designated 18OH-DOC) is a steroid hormone probably used to conserve
sodium and stimulate
hydrogen ion (or acid) excretion. 18OH-DOC lowers urine pH but has no affect on
potassium excretion. This would seem to indicate that 18OH-DOC's primary purpose is to stimulate hydrogen ion or
ammonium excretion. Under low sodium intake 18 OH DOC is increased in serum. There is a marked increase in serum 18OH DOC after injection of insulin and this may be due to the
hypokalemic (low serum potassium) tendency after a rise in insulin which in turn would make the serum more acidic. Since 18OH-DOC lowers urine pH (increases acidity) but has no affect on potassium excretion, this would seem to indicate that 18OH-DOC's primary purpose is to stimulate hydrogen ion or ammonium excretion. Its use by the body to conserve potassium would be indirect by virtue of hydrogen ion's interference with potassium excretion. This interference is further indicated because injecting sodium bicarbonate or even hyperventilating (breathing rapidly beyond need) can triple potassium excretion. The daily rhythm for potassium and hydrogen ion excretion show a rather close inverse relationship, which gives additional circumstantial support to the supposition that they compete at a common site. 18OH-DOC is strongly dependent on the potassium cell or plasma content, because in potassium deficient rats markedly less 18OH-DOC is converted to 18OH-corticosterone and less yet if sodium is deficient.
ACTH (a peptide hormone) has a large affect on 18OH DOC, causing 18OH DOC to go down to zero when ACTH does. This could be for the primary purpose of keeping serum immune enzymes and cell fluids at a high
pH (alkaline) during internal infection, but not doing so during the intestinal infection of diarrhea, during which disease the resulting dehydration forces ACTH to decline. It probably is important normally to keep the vacuoles where pathogens are digested at a high pH because if the pH or alkalinity isn't high enough, the pathogens inside the immune cells are not digested and thus released intact. So when an intestinal disease isn't calling for ACTH to decline, the indirect potassium conserving attribute of 18OH-DOC by virtue of stimulating acid excretion would be valuable, as would also increased acid excretion during internal disease be valuable.
18OH DOC may act primarily by blocking aldosterone's effect on potassium, and must have
aldosterone to assist it with sodium. Nichols, et al, have been able to show that injection of 18OH-DOC, which raised blood levels of this hormone ten times, were more retentive of sodium than a similar amount of aldosterone. So there must be a synergism involved. At the same time, the ratio of sodium to potassium excretion declined very little for 18OH-DOC, while for aldosterone, the ratio fell to as little as 1/3 that of control men. This implies a considerable sparing of potassium by 18OH-DOC. Urine potassium excretion isn't altered by 18OH-DOC injection.
Angiotensin II has very little effect on 18OH-DOC and is ambiguous nor does serum potassium above 4.8 mEq/litter (187 mg). This last isn't surprising since 18OH-DOC shouldn't be used by the body at high serum potassium. Under low sodium intake, 18OH-DOC rises in the serum. ACTH causes a marked increase in 18OH-DOC, probably by a generalized affect on the
zona fasciculata of the
adrenal cortex where 18OH-DOC is synthesized. So when it's necessary for sodium to be unloaded during the dehydration induced decline of ACTH during diarrhea in order to preserve osmotic pressure, the resulting 18OH-DOC decline would assist in this.
18OH-DOC is deeply involved in one of the three forms (at least) of
hypertension (high blood pressure).
Pathophysiology
Hyperaldosteronism (the syndrome caused by elevated aldosterone) generally results from adrenal neoplasms. The two main resulting problems:
- Hypertension and edema due to excessive Na+ and water retention.
- Accelerated excretion of potassium ions. With extreme K+ loss there's muscle weakness and eventually paralysis.
Underproduction, or hypoaldosteronism, leads to the salt-wasting state associated with
Addison's disease, although classical
congenital adrenal hyperplasia and other disease states may also cause this situation.
Pharmacology
An example of synthetic mineralocorticoids is
fludrocortisone (Florinef). Important mineralocorticoid inhibitors are
spironolactone and
eplerenone.
Further Information
Get more info on 'Mineralocorticoid'.
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