Aldactone®
Spironolactone
Aldosterone Antagonist
Pfizer
http://www.pfizer.com/pfizer/main.jsp
Aldactone Monograph PDF download here.
CPS:PIS_m012200
Pharmacology
Spironolactone is a specific pharmacologic
antagonist of aldosterone, acting primarily through competitive binding of
receptors at the aldosterone-dependent sodium-potassium exchange site in the
distal convoluted renal tubule. Spironolactone causes increased amounts of
sodium and water to be excreted, while potassium loss is minimized. Spironolactone
acts both as a diuretic and as an antihypertensive drug by this mechanism. It
may be given alone or with other diuretic agents which act more proximally in
the renal tubule.
Increased levels of the
mineralocorticoid, aldosterone, are present in primary and secondary hyperaldosteronism.
Edematous states in which secondary aldosteronism is usually involved include
congestive heart failure, hepatic cirrhosis, and nephrotic syndrome. By
competing with aldosterone for receptor sites, spironolactone provides
effective therapy for the edema and ascites in those conditions. Spironolactone
counteracts secondary aldosteronism induced by the volume depletion and
associated sodium loss caused by diuretic therapy.
Spironolactone is
effective in lowering the systolic and diastolic blood pressure in patients
with primary hyperaldosteronism. It is also effective in most cases of
essential hypertension, despite the fact that aldosterone secretion may be
within normal limits in benign essential hypertension.
Through its action in
antagonizing the effect of aldosterone, spironolactone inhibits the exchange of
sodium for potassium in the distal renal tubule and helps to prevent potassium
loss.
Spironolactone has not
been demonstrated to elevate serum uric acid, to precipitate gout, or to alter
carbohydrate metabolism.
Spironolactone is
rapidly and extensively metabolized. Sulfur-containing products are the
predominant metabolites and are thought to be primarily responsible for the
therapeutic effects of the drug. Approximately 25 to 30% of the dose
administered is converted to canrenone, which attains peak serum levels
2 to 4 hours after single oral administration of spironolactone. In
the dose range of 25 to 200 mg, an approximately linear relationship
exists between a single dose of spironolactone and plasma levels of canrenone.
Plasma concentrations
of canrenone decline in 2 distinct phases, the first phase lasting from 3 to 12 hours,
being more rapid than the second phase lasting from 12 to 96 hours. Canrenone clearance
data, following multiple doses of spironolactone, indicate that accumulation of
canrenone in the body with 100 mg once a day would be lower than with
25 mg 4 times a day. Both spironolactone and canrenone are more than
90% bound to plasma proteins. The metabolites of spironolactone are excreted
both in the urine (32 to 53%), and through biliary excretion in the feces
(14 to 36%).
Indications
Primary Hyperaldosteronism: Spironolactone is a
useful agent in the diagnosis of primary hyperaldosteronism. In the presence of
hypokalemic alkalosis and hypertension, a diagnosis of primary hyperaldosteronism
should be considered if both blood pressure and serum electrolytes return to
normal following treatment with spironolactone.
Spironolactone is
useful in the pre-operative treatment of patients with primary hyperaldosteronism
and for the maintenance therapy of such patients who decline surgery, or who
are unsuitable for surgery.
Edematous Conditions: Congestive Heart Failure
(CHF): Spironolactone is useful in the management of edema and sodium retention
in CHF when the patient is only partially responsive to, or intolerant of,
other therapeutic measures. Spironolactone may be used alone or with thiazides.
It is indicated in patients with CHF taking digitalis when other therapies are
considered inappropriate.
Cirrhosis of the Liver Accompanied by Edema
and/or Ascites: Aldosterone levels may be exceptionally high in this condition.
Spironolactone is indicated for maintenance therapy, in combination with bed
rest and the restriction of fluid and sodium.
Nephrotic Syndrome: Spironolactone is useful for
inducing a diuresis in patients not responsive to glucocorticoid therapy (for
the nephrotic syndrome), and not responding to other diuretics. However, spironolactone
has not been shown to affect the basic pathological process.
Essential Hypertension: Spironolactone is
indicated, usually in combination with other drugs, for patients who cannot be
treated adequately with other agents or for whom other agents are considered
inappropriate. Spironolactone alone has mild to moderate antihypertensive activity.
Hypokalemia: Spironolactone is indicated for
treatment of hypokalemia when other measures are considered inappropriate or
inadequate. It is also indicated for the prophylaxis of hypokalemia in
digitalis therapy when other measures are inadequate or inappropriate.
Contraindications
Anuria, acute renal insufficiency, significant
impairment of renal function, hyperkalemia, and sensitivity to spironolactone.
Warnings
Potassium (K+) Supplementation: Do
not give potassium supplementation (including dietary potassium) in conjunction
with spironolactone therapy. Excessive potassium intake may cause hyperkalemia
in patients receiving spironolactone. Do not administer spironolactone
concurrently with other potassium sparing diuretics.
Turmorigenicity: Spironolactone, in chronic
toxicity studies, has been shown to be a tumorigen in rats.
Use spironolactone only
for conditions described under Indications.
Precautions
Electrolyte Balance: Because of the diuretic
action of spironolactone, patients should be carefully evaluated for possible
disturbance of fluid and electrolyte balance.
Hyperkalemia: Hyperkalemia may occur in patients
treated with spironolactone if the potassium intake is excessive. This can
cause cardiac irregularities, some of which may be fatal. Hyperkalemia may also
occur even in the absence of potassium supplementation, particularly in
patients with impaired renal function, elderly patients, or patients with
diabetes. Consequently, no potassium supplementation should ordinarily be given
with spironolactone. Hyperkalemia can be treated promptly by rapid i.v.
administration of glucose (20 to 50%) and regular insulin, using
0.25 to 0.5 units of insulin/g of glucose. This is a temporary
measure to be repeated if required. Spironolactone should be discontinued and
potassium intake (including dietary potassium) restricted.
Hyponatremia: During the administration of spironolactone
patients suffering from sodium depletion must be attentively monitored and
signs of electrolyte imbalance must be carefully checked.
Spironolactone may, if
administered concomitantly with other diuretics, cause or aggravate hyponatremia,
as manifested by dryness of the mouth, thirst, lethargy, and drowsiness.
Metabolic Effects: Hyperchloremic metabolic
acidosis: Spironolactone may induce or worsen hyperchloremic metabolic
acidosis.
Acidosis and Renal Function: Rare reports of
acidosis have been reported with spironolactone.
Drug Interactions
Diuretics and Antihypertensives: Although spironolactone
may be administered concomitantly with diuretics and antihypertensives, the
effect of spironolactone is additive. Thus, it is advisable to reduce the dose
of these drugs. In particular, the dose of ganglionic blocking agents should be
reduced by at least 50% when spironolactone is added to the regimen.
Hyperkalemia has been
associated with the use of angiotensin converting enzyme (ACE) inhibitors in
combination with potassium-sparing diuretics.
Norepinephrine: Spironolactone reduces the
vascular responsiveness to norepinephrine. Caution should be exercised in the
management of patients subjected to regional or general anesthesia.
Digoxin: Spironolactone has been shown to
increase the half-life of digoxin. This may result in increased serum digoxin
levels and subsequent digitalis toxicity. It may be necessary to reduce the
maintenance dose of digoxin when spironolactone is administered, and the
patient should be carefully monitored to avoid over- or underdigitalization.
Carbenoxolone: Carbenoxolone may cause sodium
retention and thus decrease the effectiveness of spironolactone. Concurrent use
of the two agents should be avoided.
Nonsteroidal Anti-inflammatory Drugs: Although
it has been reported that ASA, mefenamic acid, and indomethacin may interfere
with the diuretic action of spironolactone due to inhibition of intrarenal
synthesis of prostaglandins, it has been shown that ASA does not alter the
effect of spironolactone on blood pressure, serum electrolytes, urea nitrogen,
or plasma renin activity in hypertensive patients.
Hyperkalemia has been
associated with the use of indomethacin in combination with potassium-sparing
diuretics.
Gynecomastia: Gynecomastia may develop with the
use of spironolactone and physicians should be advised of its possible
occurrence. The development of gynecomastia appears to be related to both
dosage and duration of therapy and is normally reversible when the drug is
discontinued. If gynecomastia develops, discontinue the drug. In rare instances
some breast enlargement may persist.
Management of Cirrhosis: Although high doses of spironolactone
are required to treat edema and ascites in patients with cirrhosis, the drug
dosage may be decreased before diuresis is complete to avoid the possibility of
dehydration.
Pregnancy
Spironolactone and its metabolites may cross the
placental barrier. Therefore, the use of spironolactone requires that the
potential benefits be weighed against the possible hazard to the mother and
fetus. In rats, feminization of the fetus has been reported at high doses.
Lactation
Canrenone, a metabolite of spironolactone,
appears in breast milk. If use of the drug is deemed essential, an alternative
method of infant feeding should be instituted.
Laboratory Tests: General: Spironolactone
therapy may cause transient elevation of BUN, especially in patients with
pre-existing renal impairment.
Several reports of
possible interference with digoxin radioimmunoassays by spironolactone or its
metabolites have appeared in the literature. Neither the extent nor the
potential clinical significance of this interference (which may be
assay-specific) has been fully established.
Discontinue spironolactone
for at least 4, and preferably 7, days prior to plasma cortisol
determinations, if they are to be done by the method of Mattingly, that
is, by fluorometric assay. No interference has been demonstrated with the
competitive protein binding technique or radioimmunoassay technique.
Adrenal Vein Catheterization and Plasma Renin
Activity: Discontinue spironolactone several days prior to adrenal vein
catheterization for measurement of aldosterone concentrations and measurements
of plasma renin activity.
Adverse Effects
Gynecomastia is observed not infrequently. In
rare instances, gynecomastia may persist. Other adverse reactions that have been
reported in association with spironolactone are: gastrointestinal symptoms
(including nausea, vomiting, cramping, diarrhea, gastric bleeding, gastritis
and ulceration), drowsiness, lethargy, headache, maculopapular or erythematous cutaneous
eruptions, urticaria, mental confusion, drug fever, ataxia, inability to
achieve or maintain erection, impotence, abnormal semen (decreased motility and
sperm count), irregular menses or amenorrhea and postmenopausal bleeding.
Carcinoma of the breast has been reported in patients taking spironolactone,
but a cause and effect relationship has not been established. A few cases of agranulocytosis
have been reported in patients taking spironolactone.
Adverse reactions are
usually reversible upon discontinuation of the drug.
Overdose
For management of a
suspected drug overdose, CPhA recommends that you contact your regional
Poison Control Centre. See the CPS Directory section for a list of
Poison Control Centres.
Symptoms
There have been no reports of fatal overdose in
man (except indirectly through hyperkalemia). Nausea and vomiting occurs and
(much more rarely) drowsiness, mental confusion, diarrhea, or a maculopapular
or erythematous rash. These manifestations disappear promptly on
discontinuation of medication. Hyperkalemia may be exacerbated.
Treatment
No specific antidote. No persistent toxicity has
occurred or is expected. Appearance of effects described above requires only
discontinuation of drug. Induce vomiting and evacuate the stomach by lavage.
For hyperkalemia, discontinue spironolactone, reduce potassium intake, consider
administration of potassium-excreting diuretics, i.v. glucose with regular
insulin (see Precautions), ion-exchange resins, or dialysis. Treat fluid
depletion and electrolyte imbalances appropriately if present.
Dosage
Diagnosis and Treatment of Primary Hyperaldosteronism:
As an initial diagnostic measure to provide presumptive evidence of primary hyperaldosteronism
while patients are on normal diets.
Long Test: Administer 400 mg/day for
3 to 4 weeks. Correction of hypokalemia and hypertension provides
presumptive evidence for the diagnosis of primary hyperaldosteronism.
Short Test: Administer 400 mg/day for
4 days. If serum potassium increases or urinary potassium decreases during
spironolactone administration, but reverts when spironolactone is discontinued,
a presumptive diagnosis of primary hyperaldosteronism should be considered.
After the diagnosis of
primary hyperaldosteronism has been established by more definitive testing procedures,
spironolactone may be administered in doses of 75 to 400 mg/day
in preparation for surgery. For those unsuitable for surgery, spironolactone
may be employed for long-term maintenance therapy at the lowest effective
dosage determined for the individual.
Edematous Disorders Associated with Congestive
Heart Failure, Cirrhosis and the Nephrotic Syndrome: When given as the sole
agent for diuresis, continue administration for at least 5 days. If an
adequate response has been achieved within 5 days, continue dosage at the
same level (or in selected patients, at a reduced dosage) in either single or
divided daily doses. Some may respond adequately to a dosage of only 75 mg
daily. If adequate diuresis is not obtained within 5 days, a second
diuretic also should be given for additive effect. Occasionally for severe,
resistant edema, one may add a potent glucocorticoid to this combined therapy.
Normally, an initial daily dosage of 100 mg (but may range from
25 to 200 mg/day) of spironolactone administered in either single or
divided doses is recommended.
Children: The initial daily dosage should
provide approximately 3 mg/kg of body weight administered in either single
or divided doses. This dose should be reduced to 1 to 2 mg/kg for
maintenance therapy or combination use with other diuretics.
Essential Hypertension: Usually in combination
with other drugs, spironolactone is indicated for patients who cannot be
treated adequately with other agents or for whom other agents are considered
inappropriate. Spironolactone has mild to moderate antihypertensive activity.
Adults: Initial daily dosage: 50 to
100 mg/day (in either single or divided doses) of spironolactone is
recommended. Spironolactone may also be given with diuretics that act more
proximally in the renal tubule or with other antihypertensive agents. Since a
stabilized response may not occur before 2 weeks, continue treatment in
either single or divided daily doses for that duration of time. Subsequently,
adjust dosage in response to patient's needs. Most patients will respond to
doses not exceeding 200 mg/day.
Hypokalemia: Spironolactone in dosages ranging
from 25 to 100 mg/day is useful in treating a diuretic-induced hypokalemia,
when oral potassium supplements or other potassium-sparing regimens are inappropriate.
See also Table 1 for
summary of dosage recommendations.
CPS:Aldactone_t1Click here for Table 1
Table 1: Aldactone
Dosage Recommendationsa
|
Condition
|
Type of Test
|
In Single or Divided
Daily Doses
|
|
|
Initial Dosage
|
Maximum Dosage
|
|
|
Primary Hyperaldosteronism:
|
|
|
Long Test
|
400 mg/day x
3–4 weeks
|
—
|
|
|
Short Test
|
400 mg/day x
4 days
|
—
|
|
|
In Preparation for Surgery:
|
100–400 mg/day
|
400 mg/day
|
|
|
Edematous Disorders:
|
|
Congestive Heart Failure
|
—
|
100 mg/day
|
200 mg/day
|
|
|
|
Urinary:
|
|
|
Cirrhosis
|
Na+/K+ ratio >1
|
100 mg/day
|
100 mg/day
|
|
|
|
Na+/K+ ratio <1
|
200–400 mg/day
|
400 mg/day
|
|
|
Nephrotic Syndrome
|
—
|
100 mg/day
|
200 mg/day
|
|
|
Essential hypertension
|
—
|
50–100 mg/day
|
200 mg/day
|
|
|
Hypokalemia
|
—
|
25–100 mg/day
|
100 mg/day
|
|
a Maintenance dosage should be
individually determined and may be lower than the recommended initial dose.
Supplied
25 mg
Each white to off-white, round, standard,
biconvex tablet, 8.7 mm diameter, impressed 
on one side, the other
side plain and with peppermint aroma, contains: spironolactone 25 mg. Nonmedicinal
ingredients: calcium sulfate, cornstarch, magnesium stearate, peppermint
flavoring and povidone. Bottles of 100. Store below 25°C.
100 mg
Each white to off-white, round, standard,
biconvex tablet, 11.1 mm diameter, impressed 
on one side, the other
side plain and with peppermint aroma, contains: spironolactone 100 mg. Nonmedicinal
ingredients: calcium sulfate, cornstarch, magnesium stearate, peppermint
flavoring and povidone. Bottles of 100. Store below 25°C.
