Pharmacology Lecture 6: Adrenergic Agonists PDF

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Dr Salem Abukres

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pharmacology adrenergic agonists physiology medicine

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This document is a lecture on adrenergic agonists, covering various aspects of pharmacology, such as characteristics and mechanisms of action. It details different types of adrenergic agonists and their effects.

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1 Pharmacology Lecture 6 Dr Salem Abukres Adrenergic Agonists Characteristics of Adrenergic Agonist: Most of the adrenergic drugs are derivatives of β-phenylethylamine (Figure 1)....

1 Pharmacology Lecture 6 Dr Salem Abukres Adrenergic Agonists Characteristics of Adrenergic Agonist: Most of the adrenergic drugs are derivatives of β-phenylethylamine (Figure 1). Substitutions on the benzene ring or on the ethylamine side chains produce a variety of compounds with varying abilities to differentiate between α and β receptors and to penetrate the CNS. Two important structural features of these drugs are 1) the number and location of OH substitutions on the benzene ring and 2) the nature of the substituent on the amino nitrogen. A. Catecholamines Sympathomimetic amines that contain the 3,4-dihydroxybenzene group (such as epinephrine, norepinephrine, isoproterenol, and dopamine) are called catecholamines. These compounds share the following properties: 1. High potency: Catecholamines (with –OH groups in the 3 and 4 positions on the benzene ring) show the highest potency in directly activating α or β receptors. 2. Rapid inactivation: Catecholamines are metabolized by Catechol-O- methyltransferase (COMT) and by (Monoaminoxidase) MAO. Thus, catecholamines have only a brief period of action when given parenterally, and they are inactivated (ineffective) when administered orally. 3. Poor penetration into the CNS: Catecholamines are polar and, therefore, do not readily penetrate into the CNS. Nevertheless, most catecholamines have some clinical effects (anxiety, tremor, and headaches) that are attributable to action on the CNS. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 2 B. Non-catecholamines Compounds lacking the catechol hydroxyl groups have longer half-lives, because they are not inactivated by COMT. These include phenylephrine, ephedrine, and amphetamine (Figure 1). These agents are poor substrates for MAO (an important route of metabolism) and, thus, show a prolonged duration of action. Increased lipid solubility of many of the non-catecholamines (due to lack of polar hydroxyl groups) permits greater access to the CNS. Mechanism of action of adrenergic agonists: 1. Direct-acting agonists: These drugs act directly on α or β receptors, producing effects similar to those that occur following stimulation of sympathetic nerves or release of epinephrine from the adrenal medulla (Figure 2). Examples of direct-acting agonists include epinephrine, norepinephrine, isoproterenol, and phenylephrine. 2. Indirect-acting agonists: These agents may block the reuptake of norepinephrine or cause the release of norepinephrine (Figure 2). The norepinephrine then traverses the synapse and binds to α or β receptors. Examples of reuptake inhibitors and agents that cause norepinephrine release include cocaine and amphetamines, respectively. 3. Mixed-action agonists: Ephedrine and its stereoisomer, pseudoephedrine, both stimulate adrenoceptors directly and release norepinephrine from the adrenergic neuron (Figure 2). Figure 1: Structures of several important adrenergic agonists. Drugs containing the catechol ring are shown in yellow. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 3 Direct-acting agonists: Direct-acting agonists bind to adrenergic receptors on effector organs without interacting with the presynaptic neuron. As a group, these agents are widely used clinically. A. Epinephrine Epinephrine is one of the four catecholamines (epinephrine, norepinephrine, dopamine, and dobutamine) commonly used in therapy. The first three are naturally occurring neurotransmitters, and the latter is a synthetic compound. In the adrenal medulla, norepinephrine is methylated to yield epinephrine, which is stored in chromaffin cells along with norepinephrine. On stimulation, the adrenal medulla releases about 80% epinephrine and 20% norepinephrine directly into the circulation. Figure 2: Sites of action of direct-, indirect-, and mixed-acting adrenergic agonists. Epinephrine interacts with both α and β receptors. At low doses, β effects (vasodilation) on the vascular system predominate, whereas at high doses, α effects (vasoconstriction) are the strongest. 1. Actions: a. Cardiovascular: The major actions of epinephrine are on the cardiovascular system. Epinephrine strengthens the contractility of the myocardium (positive inotrope: β1 action) and increases its rate of contraction (positive chronotrope: β1 action). Therefore, cardiac output increases. These effects increase oxygen demands on the myocardium. Epinephrine activates β1 receptors on the kidney to cause renin release. Renin is an enzyme involved in the production of angiotensin II, a potent vasoconstrictor. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 4 Epinephrine constricts arterioles in the skin, mucous membranes, and viscera (α effects), and it dilates vessels going to the liver and skeletal muscle (β2 effects). Renal blood flow is decreased. Therefore, the cumulative effect is an increase in systolic blood pressure, coupled with a slight decrease in diastolic pressure due to β2 receptor– mediated vasodilation in the skeletal muscle vascular bed (Figure 3). b. Respiratory: Epinephrine causes powerful bronchodilation by acting directly on bronchial smooth muscle (β2 action). It also inhibits the release of allergy mediators such as histamines from mast cells. c. Hyperglycemia: Epinephrine has a significant hyperglycemic effect because of increased glycogenolysis in the liver (β2 effect), increased release of glucagon (β2 effect), and a decreased release of insulin (α2 effect). d. Lipolysis: Epinephrine initiates lipolysis through agonist activity on the β receptors of adipose tissue.. 2. Therapeutic uses: a. Bronchospasm: in treatment of acute asthma and anaphylactic shock, epinephrine is the drug of choice and can be life saving in this setting. Within a few minutes after subcutaneous administration, respiratory function greatly improves. However, selective β2 agonists, such as albuterol, are Figure 3: Cardiovascular effects of intravenous infusion of low doses of epinephrine. favored in the chronic treatment of asthma because of a longer duration of action and minimal cardiac stimulatory effects. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 5 b. Anaphylactic shock: Epinephrine is the drug of choice for the treatment of type I hypersensitivity reactions (including anaphylaxis) in response to allergens. c. Cardiac arrest: Epinephrine may be used to restore cardiac rhythm in patients with cardiac arrest. d. Anesthetics: Local anesthetic solutions may contain low concentrations (for example, 1:100,000 parts) of epinephrine. Epinephrine greatly increases the duration of local anesthesia by producing vasoconstriction at the site of injection. This allows the local anesthetic to persist at the injection site before being absorbed into the systemic circulation. Adverse effects: Epinephrine can produce adverse CNS effects that include anxiety, fear, tension, headache, and tremor. It can trigger cardiac arrhythmias, particularly if the patient is receiving digoxin. Epinephrine can also induce pulmonary edema. Epinephrine may have enhanced cardiovascular actions in patients with hyperthyroidism, and the dose must be reduced in these individuals. Epinephrine increases the release of endogenous stores of glucose. In diabetic patients, dosages of insulin may have to be increased. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 6 B. Norepinephrine Because norepinephrine is the neurotransmitter of adrenergic nerves, it should, theoretically, stimulate all types of adrenergic receptors. However, when administered in therapeutic doses, the α- adrenergic receptor is most affected. 1. Cardiovascular actions: a. Vasoconstriction: Norepinephrine causes a rise in peripheral resistance due to intense vasoconstriction of most vascular beds, including the kidney (α1 effect). Both systolic and diastolic blood pressures increase (Figure 4). [Note: Norepinephrine causes greater vasoconstriction than epinephrine, because it does not induce compensatory vasodilation via β2 receptors on blood vessels supplying skeletal muscles. The weak β2 activity of norepinephrine also explains why it is not useful in the treatment of asthma or anaphylaxis.] b. Baroreceptor reflex: Norepinephrine increases bradycardia, which is blood pressure, and this stimulates the baroreceptors, inducing a rise in vagal activity. The increased vagal activity produces a reflex Figure 4: Cardiovascular effects of intravenous infusion of norepinephrine. sufficient to counteract the local actions of norepinephrine on the heart. When atropine, which blocks the transmission of vagal effects, is given before norepinephrine, stimulation of the heart by norepinephrine is evident as tachycardia. 2. Therapeutic uses: Norepinephrine is used to treat shock, because it increases vascular resistance and, therefore, increases blood pressure. It has no other clinically significant uses. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 7 C. Isoproterenol Isoproterenol is a direct-acting synthetic catecholamine that stimulates both β1- and β2- adrenergic receptors. Its non-selectivity is one of its drawbacks and the reason why it is rarely used therapeutically. Its action on α receptors is insignificant. Isoproterenol produces intense stimulation of the heart, increasing heart rate, contractility, and cardiac output (Figure 4). It is as active as epinephrine in this action. Isoproterenol also dilates the arterioles of skeletal muscle (β2 effect), resulting in decreased peripheral resistance. Because of its cardiac stimulatory action, it may increase systolic blood pressure slightly, but it greatly reduces mean arterial and diastolic blood pressures (Figure 4). Isoproterenol is a potent bronchodilator (β2 effect). The use of isoproterenol has largely been replaced with other drugs, but it may be useful in atrioventricular (AV) block. The adverse effects of isoproterenol are similar to those of epinephrine. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 8 D. Dopamine Dopamine [DOE-pa-meen], the immediate metabolic precursor of norepinephrine, occurs naturally in the CNS in the basal ganglia, where it functions as a neurotransmitter. Dopamine can activate α- and β- adrenergic receptors. For example, at higher doses, it causes vasoconstriction by activating α1 receptors, whereas at lower doses, it stimulates β1 cardiac receptors. 1. Actions: a. Cardiovascular: Dopamine exerts a stimulatory effect on the β1 receptors of the heart, having both positive inotropic and chronotropic effects (Figure 6.13). At very high doses, dopamine activates α1 receptors on the vasculature, resulting in vasoconstriction. Figure 5: Clinically important actions of isoproterenol and dopamine. b. Renal and visceral: Dopamine dilates renal and splanchnic arterioles by activating dopaminergic receptors, thereby increasing blood flow to the kidneys and other viscera (Figure 6.13). These receptors are not affected by α- or β-blocking drugs. Therefore, dopamine is clinically useful in the treatment of shock, in which significant increases in sympathetic activity might compromise renal function. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 9 2. Therapeutic uses: Dopamine is the drug of choice for cardiogenic and septic shock and is given by continuous infusion. It raises blood pressure by stimulating the β1 receptors on the heart to increase cardiac output and α1 receptors on blood vessels to increase total peripheral resistance. In addition, it enhances perfusion to the kidney and splanchnic areas, as described above. E. Fenoldopam Fenoldopam is an agonist of peripheral dopamine D1 receptors. It is used as rapid- acting vasodilators to treat sever hypertension in hospitalized patients, acting on coronary arteries, kidney arterioles, and mesenteric arteries. F. Dobutamine Dobutamine is a synthetic, direct-acting catecholamine that is a β1 receptor agonist. It increases cardiac rate and output with few vascular effects. Dobutamine is used to increase cardiac output in acute heart failure, as well as for inotropic support after cardiac surgery. The drug increases cardiac output and does not significantly elevate oxygen demands of the myocardium, a major advantage over other sympathomimetic drugs. G. Oxymetazoline Oxymetazoline is a direct-acting synthetic adrenergic agonist that stimulates both α1- and α2-adrenergic receptors. Oxymetazoline is found in many over-the-counter short- term nasal spray decongestants, as well as in ophthalmic drops for the relief of redness of the eyes associated with swimming, colds, and contact lenses. Oxymetazoline directly stimulates α receptors on blood vessels supplying the nasal mucosa and conjunctiva, thereby producing vasoconstriction and decreasing congestion. It is absorbed in the systemic circulation regardless of the route of administration and may produce nervousness, headaches, and trouble sleeping. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 10 H. Phenylephrine Phenylephrine is a direct-acting, synthetic adrenergic drug that binds primarily to α1 receptors. Phenylephrine is a vasoconstrictor that raises both systolic and diastolic blood pressures. It has no effect on the heart itself but, rather, induces reflex bradycardia when given parenterally. The drug is used to treat hypotension in hospitalized or surgical patients (especially those with a rapid heart rate). Large doses can cause hypertensive headache and cardiac irregularities. Phenylephrine acts as a nasal decongestant when applied topically or taken orally. I. Clonidine Clonidine is an α2 agonist that is used for the treatment of hypertension. It can also be used to minimize the symptoms that accompany withdrawal from opiates, tobacco smoking, and benzodiazepines. Clonidine acts centrally on presynaptic α2 receptors to produce inhibition of sympathetic vasomotor centers, decreasing sympathetic outflow to the periphery. The most common side effects of clonidine are lethargy, sedation, constipation, and xerostomia. Abrupt discontinuance must be avoided to prevent rebound hypertension. J. Albuterol and terbutaline Albuterol and terbutaline are short-acting β2 agonists used primarily as bronchodilators and administered by a metered-dose inhaler. Albuterol is the short-acting β2 agonist of choice for the management of acute asthma symptoms. Terbutaline is also used off-label as a uterine relaxant to suppress premature labor. One of the most common side effects of these agents is tremor, but patients tend to develop tolerance to this effect. When these drugs are administered orally, they may cause tachycardia or arrhythmia (due to β1 receptor activation), especially in patients with underlying cardiac disease. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 11 Monoamine oxidase inhibitors (MAOIs) also increase the risk of adverse cardiovascular effects, and concomitant use should be avoided. K. Salmeterol and formoterol Salmeterol and formoterol are long acting β agonists (LABAs) that are β2 selective. A single dose by a metered-dose inhalation device, such as a dry powder inhaler, provides sustained bronchodilation over 12 hours, compared with less than 3 hours for albuterol. These agents are not recommended as monotherapy, but are highly efficacious when combined with a corticosteroid. L. Mirabegron Mirabegron is a β3 agonist that relaxes the detrusor smooth muscle and increases bladder capacity. It is used for patients with overactive bladder. Mirabegron may increase blood pressure and should not be used in patients with uncontrolled hypertension. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 12 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 13 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 14 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 15 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 16 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 17 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 18 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 19 Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 20 INDIRECT-ACTING ADRENERGIC AGONISTS Indirect-acting adrenergic agonists cause the release, inhibit the reuptake, or inhibit the degradation of epinephrine or norepinephrine. They potentiate the effects of epinephrine or norepinephrine produced endogenously, but do not directly affect postsynaptic receptors. A. Amphetamine The marked central stimulatory action of amphetamine is often mistaken by drug abusers as its only action. However, the drug can also increase blood pressure significantly by α1 agonist action on the vasculature, as well as β1-stimulatory effects on the heart. B. Tyramine Tyramine is not a clinically useful drug, but it is important because it is found in fermented foods, such as aged cheese. It is a normal by-product of tyrosine metabolism. Normally, it is oxidized by MAO in the gastrointestinal tract, but, if the patient is taking MAOIs, it can precipitate serious vasopressor episodes. C. Cocaine Cocaine is unique among local anesthetics in having the ability to block the sodium- chloride (Na+/Cl-)-dependent norepinephrine transporter required for cellular uptake of norepinephrine into the adrenergic neuron. Consequently, norepinephrine accumulates in the synaptic space, resulting in enhanced sympathetic activity and potentiation of the actions of epinephrine and norepinephrine. Therefore, small doses of the catecholamines produce greatly magnified effects in an individual taking cocaine. In addition, the duration of action of epinephrine and norepinephrine is increased. Like amphetamines, it can increase blood pressure by α1 agonist actions and β stimulatory effects. MIXED-ACTION ADRENERGIC AGONISTS Ephedrine and pseudoephedrine are mixed-action adrenergic agents. They not only release stored norepinephrine from nerve endings but also directly stimulate both α Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres 21 and β receptors. Thus, a wide variety of adrenergic actions ensue that are similar to those of epinephrine, although less potent. Ephedrine and pseudoephedrine are not catechols and are poor substrates for COMT and MAO. Therefore, these drugs have a long duration of action. Ephedrine and pseudoephedrine have excellent absorption orally and penetrate into the CNS. Ephedrine raises systolic and diastolic blood pressures by vasoconstriction and cardiac stimulation and can be used to treat hypotension. Ephedrine produces bronchodilation, but it is less potent and slower acting than epinephrine or isoproterenol. It was previously used to prevent asthma attacks but has been replaced by more effective medications. Ephedrine produces a mild stimulation of the CNS. This increases alertness, decreases fatigue, and prevents sleep. It also improves athletic performance. [Note: The clinical use of ephedrine is declining because of the availability of better, more potent agents that cause fewer adverse effects. Ephedrine-containing herbal supplements (mainly ephedra- containing products) have been banned by the U.S. Food and Drug Administration because of life-threatening cardiovascular reactions.] Pseudoephedrine is primarily used orally to treat nasal and sinus congestion. Pharmacology Lecture 6 Adrenergic agonist Dr Salem Abukres

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