| Beta blockers | |
|---|---|
| Drug class | |
Skeletal formula of propranolol, the first clinically successful beta blocker
| |
| Class identifiers | |
| Synonyms | beta-blockers, β-blockers, beta-adrenergic blocking agents, beta antagonists, beta-adrenergic antagonists, beta-adrenoreceptor antagonists, beta adrenergic receptor antagonists, BB |
| Use | Hypertension, arrhythmia, etc. |
| ATC code | C07 |
| Biological target | beta receptors |
| Clinical data | |
| Drugs.com | Drug Classes |
| Consumer Reports | Best Buy Drugs |
| WebMD | MedicineNet RxList |
| External links | |
| MeSH | D000319 |
Beta blockers (beta-blockers, β-blockers, etc.) are a class of medications that are predominantly used to manage abnormal heart rhythms, and to protect the heart from a second heart attack (myocardial infarction) after a first heart attack (secondary prevention). They are also widely used to treat high blood pressure (hypertension), although they are no longer the first choice for initial treatment of most patients.
Beta blockers are competitive antagonists that block the receptor sites for the endogenous catecholamines epinephrine (adrenaline) and norepinephrine (noradrenaline) on adrenergic beta receptors, of the sympathetic nervous system, which mediates the fight-or-flight response. Some block activation of all types of β-adrenergic receptors and others are selective for one of the three known types of beta receptors, designated β1, β2 and β3 receptors. β1-adrenergic receptors are located mainly in the heart and in the kidneys. β2-adrenergic receptors are located mainly in the lungs, gastrointestinal tract, liver, uterus, vascular smooth muscle, and skeletal muscle. β3-adrenergic receptors are located in fat cells.
Beta receptors are found on cells of the heart muscles, smooth muscles, airways, arteries, kidneys, and other tissues that are part of the sympathetic nervous system and lead to stress responses, especially when they are stimulated by epinephrine (adrenaline). Beta blockers interfere with the binding to the receptor of epinephrine and other stress hormones, and weaken the effects of stress hormones.
In 1964, James Black synthesized the first clinically significant beta blockers—propranolol and pronethalol; it revolutionized the medical management of angina pectoris and is considered by many to be one of the most important contributions to clinical medicine and pharmacology of the 20th century.
For the treatment of primary hypertension, meta-analyses of studies which mostly used atenolol have shown that although beta blockers are more effective than placebo in preventing stroke and total cardiovascular events, they are not as effective as diuretics, medications inhibiting the renin–angiotensin system (e.g., ACE inhibitors), or calcium channel blockers.
Medical uses
Large differences exist in the pharmacology of agents within the
class, thus not all beta blockers are used for all indications listed
below.
Indications for beta blockers include:
- Angina pectoris (contraindicated for Prinzmetal's angina)
- Atrial fibrillation
- Cardiac arrhythmia
- Congestive heart failure
- Essential tremor
- Glaucoma (As eye drops, they decrease intraocular pressure by lowering aqueous humor secretion.)
- Hypertension, although they are generally not preferred as an initial treatment.
- Hyperthyroidism
- Migraine prophylaxis
- Mitral valve prolapse
- Myocardial infarction
- Phaeochromocytoma, in conjunction with α-blocker
- Postural orthostatic tachycardia syndrome
- Symptomatic control (tachycardia, tremor) in anxiety and hyperthyroidism
- Theophylline overdose
Beta blockers have also been used for:
- Acute aortic dissection
- Hypertrophic obstructive cardiomyopathy
- Long QT syndrome
- Marfan syndrome (treatment with propranolol slows progression of aortic dilation and its complications)
- Prevention of variceal bleeding in portal hypertension
- Possible mitigation of hyperhidrosis
- Social and other anxiety disorders
- Controversially, for reduction of perioperative mortality in non-cardiac surgery, but the best evidence suggests that they increase mortality when used this way
Congestive heart failure
Although beta blockers were once contraindicated in congestive heart failure,
as they have the potential to worsen the condition due to their effect
of decreasing cardiac contractility, studies in the late 1990s showed
their efficacy at reducing morbidity and mortality.
Bisoprolol, carvedilol, and sustained-release metoprolol are specifically indicated as adjuncts to standard ACE inhibitor and diuretic
therapy in congestive heart failure, although at doses typically much
lower than those indicated for other conditions. Beta blockers are only
indicated in cases of compensated, stable congestive heart failure; in
cases of acute decompensated heart failure, beta blockers will cause a
further decrease in ejection fraction, worsening the patient's current
symptoms.
Beta blockers are known primarily for their reductive effect on
heart rate, although this is not the only mechanism of action of
importance in congestive heart failure. Beta blockers, in addition to their sympatholytic β1 activity in the heart, influence the renin–angiotensin system at the kidneys. Beta blockers cause a decrease in renin
secretion, which in turn reduces the heart oxygen demand by lowering
extracellular volume and increasing the oxygen-carrying capacity of
blood. Heart failure characteristically involves increased catecholamine
activity on the heart, which is responsible for a number of deleterious
effects, including increased oxygen demand, propagation of inflammatory
mediators, and abnormal cardiac tissue remodeling, all of which
decrease the efficiency of cardiac contraction and contribute to the low
ejection fraction.
Beta blockers counter this inappropriately high sympathetic activity,
eventually leading to an improved ejection fraction, despite an initial
reduction in ejection fraction.
Trials have shown beta blockers reduce the absolute risk of death
by 4.5% over a 13-month period. In addition to reducing the risk of
mortality, the numbers of hospital visits and hospitalizations were also
reduced in the trials.
Therapeutic administration of beta blockers for congestive heart
failure ought to begin at very low doses (1/8 of target) with gradual
escalation of the dose. The heart of the patient must adjust to
decreasing stimulation by catecholamines and find a new equilibrium at a
lower adrenergic drive.
Anxiety
Officially, beta blockers are not approved for anxiolytic use by the U.S. Food and Drug Administration. However, many controlled trials in the past 25 years indicate beta blockers are effective in anxiety disorders, though the mechanism of action is not known. The physiological symptoms of the fight-or-flight
response (pounding heart, cold/clammy hands, increased respiration,
sweating, etc.) are significantly reduced, thus enabling anxious
individuals to concentrate on the task at hand.
Musicians, public speakers, actors, and professional dancers have been known to use beta blockers to avoid performance anxiety, stage fright, and tremor during both auditions and public performances. The application to stage fright was first recognized in The Lancet in 1976, and by 1987, a survey conducted by the International Conference of Symphony Orchestra Musicians,
representing the 51 largest orchestras in the United States, revealed
27% of its musicians had used beta blockers and 70% obtained them from
friends, not physicians.
Beta blockers are inexpensive, said to be relatively safe, and on one
hand, seem to improve musicians' performances on a technical level,
while some, such as Barry Green, the author of "The Inner Game of Music"
and Don Greene, a former Olympic diving coach who teaches Juilliard
students to overcome their stage fright naturally, say the performances
may be perceived as "soulless and inauthentic".
Cardiac surgery
The use of beta blockers around the time of cardiac surgery decreases the risk of heart dysrhythmias. Starting them around the time of other types of surgery, however, may worsen outcomes.
Performance-enhancing use
Because
they promote lower heart rates and reduce tremors, beta blockers have
been used in professional sports where high accuracy is required,
including archery, shooting, golf and snooker. Beta blockers are banned by the International Olympic Committee. In the 2008 Summer Olympics, 50-metre pistol silver medalist and 10-metre air pistol bronze medalist Kim Jong-su tested positive for propranolol and was stripped of his medals.
For similar reasons, beta blockers have also been used by surgeons.
Adverse effects
Adverse drug reactions associated with the use of beta blockers include: nausea, diarrhea, bronchospasm, dyspnea, cold extremities, exacerbation of Raynaud's syndrome, bradycardia, hypotension, heart failure, heart block, fatigue, dizziness, alopecia (hair loss), abnormal vision, hallucinations, insomnia, nightmares, sexual dysfunction, erectile dysfunction and/or alteration of glucose and lipid metabolism. Mixed α1/β-antagonist therapy is also commonly associated with orthostatic hypotension. Carvedilol therapy is commonly associated with edema. Due to the high penetration across the blood–brain barrier, lipophilic beta blockers, such as propranolol and metoprolol,
are more likely than other less lipophilic beta blockers to cause sleep
disturbances, such as insomnia, vivid dreams and nightmares.
Adverse effects associated with β2-adrenergic receptor
antagonist activity (bronchospasm, peripheral vasoconstriction,
alteration of glucose and lipid metabolism) are less common with β1-selective
(often termed "cardioselective") agents, but receptor selectivity
diminishes at higher doses. Beta blockade, especially of the beta-1
receptor at the macula densa, inhibits renin release, thus decreasing the release of aldosterone. This causes hyponatremia and hyperkalemia.
Hypoglycemia can occur with beta blockade because β2-adrenoceptors normally stimulate glycogen breakdown (glycogenolysis) in the liver and pancreatic release of the hormone glucagon,
which work together to increase plasma glucose. Therefore, blocking
β2-adrenoceptors lowers plasma glucose. β1-blockers have fewer metabolic
side effects in diabetic patients; however, the fast heart rate that
serves as a warning sign for insulin-induced low blood sugar may be
masked, resulting in hypoglycemia unawareness. This is termed beta blocker induced hypoglycemia unawareness. Therefore, beta blockers are to be used cautiously in diabetics.
A 2007 study revealed diuretics and beta blockers used for hypertension increase a patient's risk of developing diabetes mellitus, while ACE inhibitors and angiotensin II receptor antagonists (angiotensin receptor blockers) actually decrease the risk of diabetes.
Clinical guidelines in Great Britain, but not in the United States,
call for avoiding diuretics and beta blockers as first-line treatment of
hypertension due to the risk of diabetes.
Beta blockers must not be used in the treatment of selective
alpha-adrenergic agonist overdose. The blockade of only beta receptors
increases blood pressure, reduces coronary blood flow, left ventricular function, and cardiac output and tissue perfusion by means of leaving the alpha-adrenergic system stimulation unopposed. Beta blockers with lipophilic properties and CNS penetration such as metoprolol and labetalol may be useful for treating CNS and cardiovascular toxicity from a methamphetamine overdose. The mixed alpha-
and beta blocker labetalol is especially useful for treatment of
concomitant tachycardia and hypertension induced by methamphetamine.
The phenomenon of "unopposed alpha stimulation" has not been reported
with the use of beta blockers for treatment of methamphetamine toxicity. Other appropriate antihypertensive drugs to administer during hypertensive crisis resulting from stimulant overdose are vasodilators such as nitroglycerin, diuretics such as furosemide, and alpha blockers such as phentolamine.
Weight gain
Weight
gain can occur as a side effect of some beta blockers, especially the
older ones, such as cardioselective beta blockers including atenolol
(Tenormin) and metoprolol (Lopressor, Toprol-XL). The average weight
gain is about 2.6 pounds (about 1.2 kilograms).
Newer beta blockers, such as carvedilol (Coreg), don't usually cause
weight gain as a side effect. Weight may rise in the first weeks of
taking the beta blocker and then generally stabilizes.
Contraindications
Contraindications for beta-blockers include:
- Abrupt discontinuations
- Acute bronchospasm
- Acute heart failure
- Asthma
- AV block
- Bradycardia
- Bronchitis
- Cardiogenic shock
- Cerebrovascular disease
- Chronic obstructive pulmonary disease (COPD)
- Diabetes mellitus
- Emphysema
- Hepatic disease
- Hypersensitivity
- Hyperthyroidism
- Hypotension
- Myopathy
- Pheochromocytoma
- Psoriasis
- Kidney failure
- Stroke
- Thyroid disease
- Vasospastic angina
- Wolff-Parkinson-White Syndrome
Asthma
The 2007
National Heart, Lung, and Blood Institute (NHLBI) asthma guidelines
recommend against the use of non-selective beta blockers in asthmatics,
while allowing for the use of cardioselective beta blockers.
Cardioselective beta-blocker (β1 blockers), if really required,
can be prescribed at the least possible dose to those with mild to
moderate respiratory symptoms. β2-agonists can somewhat mitigate β-Blocker-induced bronchospasm where it exerts greater efficacy on reversing selective β-blocker-induced bronchospasm than the nonselective β-blocker-induced worsening asthma and/or COPD.
Cocaine
Beta
blockers should not be used as a first-line treatment in the acute
setting for cocaine-induced acute coronary syndrome (CIACS). No recent
studies have been identified that show the benefit of beta blockers in
reducing coronary vasospasm, or coronary vascular resistance, in
patients with CIACS. In the multiple case studies identified, the use of
beta blockers in CIACS resulted in detrimental outcomes, and the
discontinuation of beta blockers used in the acute setting led to
improvement in clinical course.
The guidelines by the American College of Cardiology/American Heart
Association also support this idea, and recommend against the use of
beta blockers in cocaine-induced ST-segment elevation myocardial
infarction (MI) because of the risk of coronary vasospasm.
Though, in general, beta blockers improve mortality in patients who
have suffered MI, it is unclear whether patients with CIACS will benefit
from this mortality reduction because no studies assess the use of beta
blockers in the long term, and because cocaine users may be prone to
continue to abuse the substance, thus complicating the effect of drug
therapy.
Diabetes mellitus
Epinephrine signals early warning of the upcoming hypoglycemia.
Beta-blockers' inhibition on epinephrine's effect can somewhat exacerbate hypoglycemia by interfering with glycogenesis and mask signs of hypoglycemia such as tachycardia, palpitations, diaphoresis, and tremors. Diligent blood glucose level monitoring is necessary for a patient with diabetes mellitus on beta-blocker.
Hyperthyroidism
Though
beta-blockers can be useful to manage acute symptoms in thyrotoxic
patients to reduce tachycardia, tremor, and anxiety, beta-blockers
should be used with caution as tachycardia is a useful monitoring
parameter in thyroid disease. Abrupt withdrawal can result in thyroid
storm.
Bradycardia or AV block
Unless
a pacemaker is present, beta-blockers can severely depress conduction
in the AV node, resulting in reduction of heart rate and cardiac output.
Usage of beta-blockers in tachycardic patients with
Wolff-Parkinson-White Syndrome can result in severe bradycardia,
necessitating treatment with a pacemaker.
Toxicity
Glucagon, used in the treatment of overdose, increases the strength of heart contractions, increases intracellular cAMP, and decreases renal vascular resistance. It is, therefore, useful in patients with beta blocker cardiotoxicity. Cardiac pacing is usually reserved for patients unresponsive to pharmacological therapy.
People experiencing bronchospasm due to the β2 receptor-blocking effects of nonselective beta blockers may be treated with anticholinergic drugs, such as ipratropium, which are safer than beta agonists in patients with cardiovascular disease. Other antidotes for beta blocker poisoning are salbutamol and isoprenaline.
β-receptor antagonism
Stimulation of β1 receptors by epinephrine and norepinephrine induces a positive chronotropic and inotropic effect on the heart and increases cardiac conduction velocity and automaticity. Stimulation of β1 receptors on the kidney causes renin release. Stimulation of β2 receptors induces smooth muscle relaxation, induces tremor in skeletal muscle, and increases glycogenolysis in the liver and skeletal muscle. Stimulation of β3 receptors induces lipolysis.
Beta blockers inhibit these normal epinephrine- and norepinephrine-mediated sympathetic actions, but have minimal effect on resting subjects.
That is, they reduce the effect of excitement or physical exertion on heart rate and force of contraction, and also tremor,
and breakdown of glycogen. Beta blockers can have a constricting effect
on the bronchi of the lungs, possibly worsening or causing asthma
symptoms.
Since β2 adrenergic receptors can cause vascular
smooth muscle dilation, beta blockers may cause some vasoconstriction.
However, this effect tends to be small because the activity of β2 receptors is overshadowed by the more dominant vasoconstricting α1
receptors. By far the greatest effect of beta blockers remains in the
heart. Newer, third-generation beta blockers can cause vasodilation
through blockade of alpha-adrenergic receptors.
Accordingly, nonselective beta blockers are expected to have antihypertensive effects.
The primary antihypertensive mechanism of beta blockers is unclear, but
may involve reduction in cardiac output (due to negative chronotropic
and inotropic effects). It may also be due to reduction in renin release from the kidneys, and a central nervous system effect to reduce sympathetic activity (for those beta blockers that do cross the blood–brain barrier, e.g. propranolol).
Antianginal effects result from negative chronotropic and
inotropic effects, which decrease cardiac workload and oxygen demand.
Negative chronotropic
properties of beta blockers allow the lifesaving property of heart rate
control. Beta blockers are readily titrated to optimal rate control in
many pathologic states.
The antiarrhythmic effects of beta blockers arise from sympathetic nervous system blockade—resulting in depression of sinus node function and atrioventricular node conduction, and prolonged atrial refractory periods. Sotalol, in particular, has additional antiarrhythmic properties and prolongs action potential duration through potassium channel blockade.
Blockade of the sympathetic nervous system on renin release leads to reduced aldosterone via the renin–angiotensin–aldosterone system, with a resultant decrease in blood pressure due to decreased sodium and water retention.
Intrinsic sympathomimetic activity
Also
referred to as intrinsic sympathomimetic effect, this term is used
particularly with beta blockers that can show both agonism and
antagonism at a given beta receptor, depending on the concentration of
the agent (beta blocker) and the concentration of the antagonized agent
(usually an endogenous compound, such as norepinephrine). See partial agonist for a more general description.
Some beta blockers (e.g. oxprenolol, pindolol, penbutolol, labetalol and acebutolol) exhibit intrinsic sympathomimetic activity (ISA). These agents are capable of exerting low-level agonist activity at the β-adrenergic receptor while simultaneously acting as a receptor site antagonist. These agents, therefore, may be useful in individuals exhibiting excessive bradycardia with sustained beta blocker therapy.
Agents with ISA are not used after myocardial infarctions, as
they have not been demonstrated to be beneficial. They may also be less
effective than other beta blockers in the management of angina and tachyarrhythmia.
α1-receptor antagonism
Some beta blockers (e.g., labetalol and carvedilol) exhibit mixed antagonism of both β- and α1-adrenergic receptors, which provides additional arteriolar vasodilating action.
Examples
Dichloroisoprenaline, the first beta blocker
Nonselective agents
Nonselective beta blockers display both β1 and β2 antagonism.
- Propranolol
- Bucindolol (has additional α1-blocking activity)
- Carteolol
- Carvedilol (has additional α1-blocking activity)
- Labetalol (has additional α1-blocking activity)
- Nadolol
- Oxprenolol (has intrinsic sympathomimetic activity)
- Penbutolol (has intrinsic sympathomimetic activity)
- Pindolol (has intrinsic sympathomimetic activity)
- Sotalol (not considered a "typical beta blocker")
- Timolol
β1-selective agents
β1-selective beta blockers are also known as cardioselective beta blockers.
- Acebutolol (has intrinsic sympathomimetic activity, ISA)
- Atenolol
- Betaxolol
- Bisoprolol
- Celiprolol (has intrinsic sympathomimetic activity)
- Metoprolol
- Nebivolol
- Esmolol
β2-selective agents
β3-selective agents
β1 selective antagonist and β3 agonist agents
Comparative information
Pharmacological differences
- Agents with intrinsic sympathomimetic action (ISA)
- Acebutolol, pindolol, labetalol, mepindolol, oxprenolol, celiprolol, penbutolol
- Agents organized by lipid solubility (lipophilicity)
- High lipophilicity: propranolol, labetalol
- Intermediate lipophilicity: metoprolol, bisoprolol, carvedilol, acebutolol, timolol, pindolol
- Low lipophilicity (also known as hydrophilic beta blockers): atenolol, nadolol, and sotalol
- Agents with membrane stabilizing effect
- Carvedilol, propranolol > oxprenolol > labetalol, metoprolol, timolol
Indication differences
- Agents specifically labeled for cardiac arrhythmia
- Agents specifically labeled for congestive heart failure
- Agents specifically labeled for glaucoma
- Agents specifically labeled for myocardial infarction
- Atenolol, metoprolol (immediate release), propranolol (immediate release), timolol, carvedilol (after left ventricular dysfunction), bisoprolol (preventive treatment before and primary treatment after heart attacks)
- Agents specifically labeled for migraine prophylaxis
Propranolol
is the only agent indicated for control of tremor, portal hypertension,
and esophageal variceal bleeding, and used in conjunction with
α-blocker therapy in phaeochromocytoma.
Other effects
Beta
blockers, due to their antagonism at beta-1 adrenergic receptors,
inhibit both the synthesis of new melatonin and its secretion by the pineal gland. The neuropsychiatric side effects of some beta blockers (e.g. sleep disruption, insomnia) may be due to this effect.
Some pre-clinical and clinical research suggests that some beta blockers may be beneficial for cancer treatment. However, other studies do not show a correlation between cancer survival and beta blocker usage. Also, a 2017 meta-analysis failed to show any benefit for the use of beta blockers in breast cancer.
Beta blockers have also been used for the treatment of schizoid personality disorder.
However, there is limited evidence supporting the efficacy of
supplemental beta-blocker use in addition to antipsychotic drugs for
treating schizophrenia.
Contrast media are not contraindicated in patients receiving beta blockers.
