Acebutolol
hydrochloride is a selective, hydrophilic beta-adrenoreceptor blocking
agent with mild intrinsic sympathomimetic activity for use in treating
patients with hypertension and ventricular arrhythmias. It is marketed
in capsule form for oral administration. Acebutolol Hydrochloride
Capsules, USP are available in two strengths which contain 200 or 400
mg of acebutolol as the hydrochloride salt. The inactive ingredients
are gelatin, methylparaben, povidone, pregelatinized starch,
propylparaben, sodium lauryl sulfate, stearic acid, titanium dioxide,
FD&C Blue #1, FD&C Red #40, D&C Yellow #10, D&C Red
#28, FD&C Blue #2, and black iron oxide.
Acebutolol
HCl is a white or slightly off-white powder freely soluble in water,
and less soluble in alcohol. Chemically it is defined as the
hydrochloride salt of (±)
N-[3-Acetyl-4-[2-hydroxy-3-[(1-methylethyl)amino]propoxy]phenyl]
butanamide.
Acebutolol
HCl is a white or slightly off-white powder freely soluble in water,
and less soluble in alcohol. Chemically it is defined as the
hydrochloride salt of (±)
N-[3-Acetyl-4-[2-hydroxy-3-[(1-methylethyl)amino]propoxy]phenyl]
butanamide.CLINICAL PHARMACOLOGY
Acebutolol is a
cardioselective, beta-adrenoreceptor blocking agent, which possesses
mild intrinsic sympathomimetic activity (ISA) in its therapeutically
effective dose range.
Pharmacodynamics
β1-cardioselectivity
has been demonstrated in experimental animal studies. In anesthetized
dogs and cats, acebutolol is more potent in antagonizing
isoproterenol-induced tachycardia (β1) than in antagonizing isoproterenol-induced vasodilatation (β2).
In guinea pigs and cats, it is more potent in antagonizing this
tachycardia than in antagonizing isoproterenol-induced bronchodilatation
(β2). ISA of acebutolol has been demonstrated in
catecholamine-depleted rats by tachycardia induced by intravenous
administration of this agent. A membrane-stabilizing effect has been
detected in animals, but only with high concentrations of acebutolol.
Clinical studies have demonstrated β1-blocking activity at the recommended doses by: a) reduction in the resting heart rate and decrease in exercise-induced tachycardia; b) reduction in cardiac output at rest and after exercise; c) reduction of systolic and diastolic blood pressures at rest and postexercise; d) inhibition of isoproterenol-induced tachycardia.
The β1-selectivity of acebutolol has also been demonstrated on the basis of the following vascular and bronchial effects:
Clinical studies have demonstrated β1-blocking activity at the recommended doses by: a) reduction in the resting heart rate and decrease in exercise-induced tachycardia; b) reduction in cardiac output at rest and after exercise; c) reduction of systolic and diastolic blood pressures at rest and postexercise; d) inhibition of isoproterenol-induced tachycardia.
The β1-selectivity of acebutolol has also been demonstrated on the basis of the following vascular and bronchial effects:
Pharmacokinetics and Metabolism
Acebutolol
is well absorbed from the GI tract. It is subject to extensive
first-pass hepatic biotransformation, with an absolute bioavailability
of approximately 40% for the parent compound. The major metabolite, an
N-acetyl derivative (diacetolol), is pharmacologically active. This
metabolite is equipotent to acebutolol and in cats is more
cardioselective than acebutolol; therefore, this first-pass phenomenon
does not attenuate the therapeutic effect of acebutolol. Food intake
does not have a significant effect on the area under the plasma
concentration-time curve (AUC) of acebutolol although the rate of
absorption and peak concentration decreased slightly.
The plasma elimination half-life of acebutolol is approximately 3 to 4 hours, while that of its metabolite, diacetolol, is 8 to 13 hours. The time to reach peak concentration for acebutolol is 2.5 hours and for diacetolol, after oral administration of acebutolol hydrochloride, 3.5 hours.
Within the single oral dose range of 200 to 400 mg, the kinetics are dose proportional. However, this linearity is not seen at higher doses, probably due to saturation of hepatic biotransformation sites. In addition, after multiple dosing the lack of linearity is also seen by AUC increases of approximately 100% as compared to single oral dosing. Elimination via renal excretion is approximately 30% to 40% and by non-renal mechanisms 50% to 60%, which includes excretion into the bile and direct passage through the intestinal wall.
Acebutolol hydrochloride has a low binding affinity for plasma proteins (about 26%).
Acebutolol and its metabolite, diacetolol, are relatively hydrophilic and, therefore, only minimal quantities have been detected in the cerebrospinal fluid (CSF).
Drug interaction studies with tolbutamide and warfarin indicated no influence on the therapeutic effects of these compounds. Digoxin and hydrochlorothiazide plasma levels were not affected by concomitant acebutolol administration. The kinetics of acebutolol were not significantly altered by concomitant administration of hydrochlorothiazide, hydralazine, sulfinpyrazone, or oral contraceptives.
In patients with renal impairment, there is no effect on the elimination half-life of acebutolol, but there is decreased elimination of the metabolite, diacetolol, resulting in a two- to three-fold increase in its half-life. For this reason, the drug should be administered with caution in patients with renal insufficiency (see PRECAUTIONS). Acebutolol and its major metabolite are dialyzable.
Acebutolol crosses the placental barrier, and is secreted in breast milk.
In geriatric patients, the bioavailability of acebutolol and its metabolite is increased, approximately two-fold, probably due to decreases in the first-pass metabolism and renal function in the elderly.
The plasma elimination half-life of acebutolol is approximately 3 to 4 hours, while that of its metabolite, diacetolol, is 8 to 13 hours. The time to reach peak concentration for acebutolol is 2.5 hours and for diacetolol, after oral administration of acebutolol hydrochloride, 3.5 hours.
Within the single oral dose range of 200 to 400 mg, the kinetics are dose proportional. However, this linearity is not seen at higher doses, probably due to saturation of hepatic biotransformation sites. In addition, after multiple dosing the lack of linearity is also seen by AUC increases of approximately 100% as compared to single oral dosing. Elimination via renal excretion is approximately 30% to 40% and by non-renal mechanisms 50% to 60%, which includes excretion into the bile and direct passage through the intestinal wall.
Acebutolol hydrochloride has a low binding affinity for plasma proteins (about 26%).
Acebutolol and its metabolite, diacetolol, are relatively hydrophilic and, therefore, only minimal quantities have been detected in the cerebrospinal fluid (CSF).
Drug interaction studies with tolbutamide and warfarin indicated no influence on the therapeutic effects of these compounds. Digoxin and hydrochlorothiazide plasma levels were not affected by concomitant acebutolol administration. The kinetics of acebutolol were not significantly altered by concomitant administration of hydrochlorothiazide, hydralazine, sulfinpyrazone, or oral contraceptives.
In patients with renal impairment, there is no effect on the elimination half-life of acebutolol, but there is decreased elimination of the metabolite, diacetolol, resulting in a two- to three-fold increase in its half-life. For this reason, the drug should be administered with caution in patients with renal insufficiency (see PRECAUTIONS). Acebutolol and its major metabolite are dialyzable.
Acebutolol crosses the placental barrier, and is secreted in breast milk.
In geriatric patients, the bioavailability of acebutolol and its metabolite is increased, approximately two-fold, probably due to decreases in the first-pass metabolism and renal function in the elderly.
INDICATIONS AND USAGE
Hypertension
Acebutolol
hydrochloride capsules are indicated for the management of
hypertension in adults. They may be used alone or in combination with
other antihypertensive agents, especially thiazide-type diuretics.
Ventricular Arrhythmias
Acebutolol
hydrochloride capsules are indicated in the management of ventricular
premature beats; it reduces the total number of premature beats, as
well as the number of paired and multiform ventricular ectopic beats,
and R-on-T beats.
CONTRAINDICATIONS
Acebutolol
hydrochloride capsules are contraindicated in: 1) persistently severe
bradycardia; 2) second- and third-degree heart block; 3) overt cardiac
failure; and 4) cardiogenic shock (see WARNINGS).
WARNINGS
Cardiac Failure
Sympathetic
stimulation may be essential for support of the circulation in
individuals with diminished myocardial contractility, and its
inhibition by beta-adrenergic receptor blockade may precipitate more
severe failure. Although beta blockers should be avoided in overt
cardiac failure, acebutolol can be used with caution in patients with a
history of heart failure who are controlled with digitalis and/or
diuretics. Both digitalis and acebutolol impair AV conduction. If
cardiac failure persists, therapy with acebutolol should be withdrawn.
In Patients Without a History of Cardiac Failure
In
patients with aortic or mitral valve disease or compromised left
ventricular function, continued depression of the myocardium with
beta-blocking agents over a period of time may lead to cardiac failure.
At the first signs of failure, patients should be digitalized and/or
be given a diuretic and the response observed closely. If cardiac
failure continues despite adequate digitalization and/or diuretic,
acebutolol therapy should be withdrawn.
Exacerbation of Ischemic Heart Disease Following Abrupt Withdrawal
Following
abrupt cessation of therapy with certain beta-blocking agents in
patients with coronary artery disease, exacerbation of angina pectoris
and, in some cases, myocardial infarction and death have been reported.
Therefore, such patients should be cautioned against interruption of
therapy without a physician's advice. Even in the absence of overt
ischemic heart disease, when discontinuation of acebutolol is planned,
the patient should be carefully observed, and should be advised to
limit physical activity to a minimum while acebutolol is gradually
withdrawn over a period of about two weeks. (If therapy with an
alternative beta-blocker is desired, the patient may be transferred
directly to comparable doses of another agent without interruption of
beta-blocking therapy.) If an exacerbation of angina pectoris occurs,
antianginal therapy should be restarted immediately in full doses and
the patient hospitalized until his condition stabilizes.
Peripheral Vascular Disease
Treatment
with beta-antagonists reduces cardiac output and can precipitate or
aggravate the symptoms of arterial insufficiency in patients with
peripheral or mesenteric vascular disease. Caution should be exercised
with such patients, and they should be observed closely for evidence of
progression of arterial obstruction.
Bronchospastic Diseases
PATIENTS WITH BRONCHOSPASTIC DISEASE SHOULD, IN GENERAL, NOT RECEIVE A BETA BLOCKER. Because of its relative β1-selectivity,
however, low doses of acebutolol may be used with caution in patients
with bronchospastic disease who do not respond to, or who cannot
tolerate, alternative treatment. Since β1-selectivity is not
absolute and is dose-dependent, the lowest possible dose of acebutolol
should be used initially, preferably in divided doses to avoid the
higher plasma levels associated with the longer dose-interval. A
bronchodilator, such as a theophylline or a β2-stimulant, should be made available in advance with instructions concerning its use.
Anesthesia and Major Surgery
The
necessity, or desirability, of withdrawal of a beta-blocking therapy
prior to major surgery is controversial. Beta-adrenergic receptor
blockade impairs the ability of the heart to respond to
beta-adrenergically mediated reflex stimuli. While this might be of
benefit in preventing arrhythmic response, the risk of excessive
myocardial depression during general anesthesia may be enhanced and
difficulty in restarting and maintaining the heart beat has been
reported with beta blockers. If treatment is continued, particular care
should be taken when using anesthetic agents which depress the
myocardium, such as ether, cyclopropane and trichlorethylene, and it is
prudent to use the lowest possible dose of acebutolol. Acebutolol,
like other beta blockers, is a competitive inhibitor of beta-receptor
agonists, and its effect on the heart can be reversed by cautious
administration of such agents (e.g., dobutamine or isoproterenol-see OVERDOSAGE).
Manifestations of excessive vagal tone (e.g., profound bradycardia, hypotension) may be corrected with atropine 1 to 3 mg IV in divided doses.
Manifestations of excessive vagal tone (e.g., profound bradycardia, hypotension) may be corrected with atropine 1 to 3 mg IV in divided doses.
Diabetes and Hypoglycemia
Beta blockers may
potentiate insulin-induced hypoglycemia and mask some of its
manifestations such as tachycardia; however, dizziness and sweating are
usually not significantly affected. Diabetic patients should be warned
of the possibility of masked hypoglycemia.
Thyrotoxicosis
Beta-adrenergic
blockade may mask certain clinical signs (tachycardia) of
hyperthyroidism. Abrupt withdrawal of beta blockade may precipitate a
thyroid storm; therefore, patients suspected of developing
thyrotoxicosis from whom acebutolol therapy is to be withdrawn should
be monitored closely.
PRECAUTIONS
Risk of Anaphylactic Reaction
While
taking beta-blockers, patients with a history of severe anaphylactic
reaction to a variety of allergens may be more reactive to repeated
challenge, either accidental, diagnostic, or therapeutic. Such patients
may be unresponsive to the usual doses of epinephrine used to treat
allergic reaction.
Impaired Renal or Hepatic Function
Studies
on the effect of acebutolol in patients with renal insufficiency have
not been performed in the United States. Foreign published experience
shows that acebutolol has been used successfully in chronic renal
insufficiency. Acebutolol is excreted through the G.I. tract, but the
active metabolite, diacetolol, is eliminated predominantly by the
kidney. There is a linear relationship between renal clearance of
diacetolol and creatinine clearance. Therefore, the daily dose of
acebutolol should be reduced by 50% when the creatinine clearance is
less than 50 mL/min and by 75% when it is less than 25 mL/min.
Acebutolol should be used cautiously in patients with impaired hepatic
function.
Acebutolol has been used successfully and without problems in elderly patients in the U.S. clinical trials without specific adjustment of dosage. However, elderly patients may require lower maintenance doses because the bioavailability of both acebutolol and its metabolite are approximately doubled in this age group.
Acebutolol has been used successfully and without problems in elderly patients in the U.S. clinical trials without specific adjustment of dosage. However, elderly patients may require lower maintenance doses because the bioavailability of both acebutolol and its metabolite are approximately doubled in this age group.
Information for Patients
Patients,
especially those with evidence of coronary artery disease, should be
warned against interruption or discontinuation of acebutolol therapy
without a physician's supervision. Although cardiac failure rarely
occurs in properly selected patients, those being treated with
beta-adrenergic blocking agents should be advised to consult a
physician if they develop signs or symptoms suggestive of impending
CHF, or unexplained respiratory symptoms.
Patients should also be warned of possible severe hypertensive reactions from concomitant use of alpha-adrenergic stimulants, such as the nasal decongestants commonly used in OTC cold preparations and nasal drops.
Patients should also be warned of possible severe hypertensive reactions from concomitant use of alpha-adrenergic stimulants, such as the nasal decongestants commonly used in OTC cold preparations and nasal drops.
Clinical Laboratory Findings
Acebutolol,
like other beta-blockers, has been associated with the development of
antinuclear antibodies (ANA). In prospective clinical trials, patients
receiving acebutolol had a dose-dependent increase in the development
of positive ANA titers and the overall incidence was higher than that
observed with propranolol. Symptoms (generally persistent arthralgias
and myalgias) related to this laboratory abnormality were infrequent
(less than 1% with both drugs). Symptoms and ANA titers were reversible
upon discontinuation of treatment.
Drug Interactions
Catecholamine-depleting
drugs, such as reserpine, may have an additive effect when given with
beta-blocking agents. Patients treated with acebutolol plus
catecholamine depletors should, therefore, be observed closely for
evidence of marked bradycardia or hypotension which may present as
vertigo, syncope/presyncope, or orthostatic changes in blood pressure
without compensatory tachycardia. Exaggerated hypertensive responses
have been reported from the combined use of beta-adrenergic antagonists
and alpha-adrenergic stimulants, including those contained in
proprietary cold remedies and vasoconstrictive nasal drops. Patients
receiving beta-blockers should be warned of this potential hazard.
Blunting of the antihypertensive effect of beta-adrenoceptor blocking agents by non-steroidal anti-inflammatory drugs has been reported.
No significant interactions with digoxin, hydrochlorothiazide, hydralazine, sulfinpyrazone, oral contraceptives, tolbutamide, or warfarin have been observed.
Blunting of the antihypertensive effect of beta-adrenoceptor blocking agents by non-steroidal anti-inflammatory drugs has been reported.
No significant interactions with digoxin, hydrochlorothiazide, hydralazine, sulfinpyrazone, oral contraceptives, tolbutamide, or warfarin have been observed.
Carcinogenesis, Mutagenesis, Impairment of Fertility
Chronic
oral toxicity studies in rats and mice, employing dose levels as high
as 300 mg/kg/day, which is equivalent to 15 times the maximum
recommended (60 kg) human dose, did not indicate a carcinogenic
potential for acebutolol. Diacetolol, the major metabolite of
acebutolol in man, was without carcinogenic potential in rats when
tested at doses as high as 1800 mg/kg/day. Acebutolol and diacetolol
were also shown to be devoid of mutagenic potential in the Ames Test.
Acebutolol, administered orally to two generations of male and female
rats at doses of up to 240 mg/kg/day (equivalent to 12 times the
maximum recommended therapeutic dose in a 60-kg human) and diacetolol,
administered to two generations of male and female rats at doses of up
to 1000 mg/kg/day, had no significant impact on reproductive
performance or fertility.
Pregnancy
Teratogenic Effects
Labor And Delivery
The
effect of acebutolol on labor and delivery in pregnant women is
unknown. Studies in animals have not shown any effect of acebutolol on
the usual course of labor and delivery.
0 التعليقات:
إرسال تعليق