L13, 14, 15 Adrenergic Receptor Agonists and Antagonists

Question 1

The sympathetic system is the ___ division of the ANS; the parasympathetic system is the ___ division of the ANS.

Answer 1

Thoracolumbar; craniosacral

Question 2

The sympathetic system has ___ arms, ___ fingers the parasymapthetic system has ___ arms, ___ fingers.

Answer 2

Short; long

Long; short

Question 3

Describe the exception of the adrenal gland.

Answer 3

Pre-ganglionic fibers project to the adrenal gland; ACh is released, which activates chromathin cells to produce NE/E. The hormones are released directly into circulation. There is no post-ganglionic nerve fiber

Question 4

Pre-ganglionic fibers release ___.

Answer 4

ACh

Question 5

Post-ganglionic parasympathetic fibers release ___.

Answer 5

ACh

Question 6

Post-ganglionic sympathetic fibers release ___. What is the exception to this?

Answer 6

NE; sympathetic fibers innervating sweat glands and some skeletal muscle blood vessels release ACh

Question 7

The adrenal gland releases ___ and ___.

Answer 7

NE and EPI

Question 8

True or false - some organs receive dual ANS innervation and some do not.

Answer 8

True

Question 9

Describe the effects of the parasympathetic system on the following organs: eye, heart, bronchioles, GI tract, bladder

Answer 9

Eye: pupillary constriction (miosis), accommodation
Heart: negative chronotropy (bradycardia)
Bronchioles: constriction of smooth muscle
GI tract: increased motility, secretions
Bladder: stimulates emptying

Question 10

Describe the effects of the sympathetic system on the following organs/functions: eye, heart, bronchioles, blood vessels, GI tract, bladder, metabolic functions

Answer 10

Eye: pupillary dilation (mydriasis)
Heart: increased chronotropy and inotropy
Bronchioles: smooth muscle relaxation
Blood vessels: constriction or relaxation
GI: decreased motility
Bladder: inhibits emptying
Metabolic functions: increased blood sugar

Question 11

Parasympathetic innervation of the eye leads to constriction of the ___, causing miosis, and constriction of the ___, leading to accommodation.

Answer 11

Sphincter muscles of the pupil; ciliary muscles

Question 12

Parasympathetic innervation of the heart reduces heart rate via the ___ and reduces conduction via the ___.

Answer 12

SA node; AV node

Question 13

Parasympathetic innervation of the bladder leads to contraction of the ___, causing bladder emptying.

Answer 13

Detrusor muscle

Question 14

Sympathetic innervation of the eye leads to constriction of the ___, causing mydriasis, and activation of the ___, leading to production of aqueous humor.

Answer 14

Dilator muscle; ciliary epithelium

Question 15

Sympathetic innervation of the heart increases heart rate via what process?

Answer 15

Accelerated SA node pacemaker depolarization

Question 16

What are the three main currents that contribute to SA node membrane potential?

Answer 16

1. Inward calcium current
2. Funny current
3. Outward potassium current

Question 17

How does sympathetic innervation accelerate SA node pacemaker depolarization?

Answer 17

Increases inward calcium current and funny current to promote faster phase 4 depolarization and lower the threshold for activation; it also stimulates increased calcium influx into myocytes, leading to greater contractile force

Question 18

Upon what two variables does the outcome of sympathetic innervation of blood vessels depend?

Answer 18

1. Relative density of receptor population (alpha1 vs. beta2) in the targeted vascular bed
2. Ligand available to mediate the vascular response (NE vs. E)

Question 19

Sympathetic innervation of the bladder leads to contraction of the ___ and relaxation of the ___, leading to inhibition of emptying.

Answer 19

Urethral sphincters; detrusor muscle

Question 20

What are the 5 broad steps of adrenergic neurotransmission?

Answer 20

1. Synthesis
2. Storage in vesicles
3. Release of catecholamines
4. Binding of NT to post- or pre-synaptic sites
5. Termination of action

Question 21

What happens during synthesis of adrenergic NT?

Answer 21

Tyrosine hydroxylase (rate-limiting enzyme) converts tyrosine to DOPA. DOPA is metabolized to DA. Half of DA is transported into vesicles via VMAT (the other half is metabolized)

Question 22

What happens during vesicle storage of adrenergic NT?

Answer 22

Dopamine can be converted to NE via dopamine beta-hydroxylase. EPI can be produced from NE via phenylethanolamine-N-methyltransferase. EPI and NE are also produced in the adrenal medulla.

Question 23

What happens during release of catecholamines?

Answer 23

Voltage dependent opening of calcium channels elevates intracellular calcium and stimulates the interaction of SNARE proteins to enable vesicle fusion and exocytosis of the vesicle contents

Question 24

The action of a NT depends upon what three things?

Answer 24

1. Receptor type
2. Second messenger system
3. Machinery of the cell type

Question 25

What are the three mechanisms of termination of action?

Answer 25

1. Re-uptake into nerve terminals or post-synaptic cell
2. Diffusion out of synaptic cleft
3. Metabolic transformation

Question 26

Where are alpha1 receptors located?

Answer 26

1. Most vascular smooth muscle*
2. Pupillary dilator muscle*
3. Pilomotor smooth muscle

Question 27

Where are alpha2 receptors located?

Answer 27

1. Adrenergic and cholinergic nerve terminals*
2. Platelets
3. Some vascular smooth muscle

Question 28

Where are beta1 receptors located?

Answer 28

1. Heart*

2. Juxtaglomerular cells*

Question 29

Where are beta2 receptors located?

Answer 29

1. Respiratory, uterine, and vascular smooth muscle*
2. Liver*
3. Pancreatic beta cells
4. Somatic motor nerve terminals (voluntary muscle)*

Question 30

Where are beta3 receptors located?

Answer 30

1. Fat cells

Question 31

Where are dopamine1 receptors located?

Answer 31

1. Renal and other splanchnic blood vessels*

Question 32

Where are dopamine2 receptors located?

Answer 32

1.Nerve terminals

Question 33

What are the effects of binding alpha1 receptors?

Answer 33

1. Contraction of vascular smooth muscle*
2. Contraction of pupillary dilator muscle (mydriasis)*
3. Contraction of pilomotor smooth muscle (erects hair)

Question 34

What are the effects of binding alpha2 receptors?

Answer 34

1. Inhibition of NT release at adrenergic and cholinergic nerve terminals*
2. Stimulates aggregation of platelets
3. Contracts some vascular smooth muscle

Question 35

What are the effects of binding beta1 receptors?

Answer 35

1. Stimulates increased rate and force of heart*

2. Stimulates renin release from juxtaglomerular cells*

Question 36

What are the effects of binding beta2 receptors?

Answer 36

1. Relaxation of respiratory, uterine, and vascular smooth muscle*
2. Stimulates glycogenolysis in the liver*
3. Stimulates insulin release from pancreatic beta cells
4. Causes a tremor via somatic motor nerve terminals*

Question 37

What are the effects of binding beta3 receptors?

Answer 37

1. Stimulates lipolysis in fat cells

Question 38

What are the effects of binding dopamine1 receptors?

Answer 38

1. Relaxes (reduces resistance) renal and other splanchnic blood vessels*

Question 39

What are the effects of binding dopamine2 receptors?

Answer 39

1. Inhibits adenylyl cyclase at nerve terminals

Question 40

Alpha1 adrenergic receptors are positively coupled to ___ via which G-protein?

Answer 40

PLC; G-alpha-q

Question 41

Describe what happens in vascular smooth muscle when an agonist binds to an alpha1 adrenergic receptor.

Answer 41

1. Agonist binds receptor
2. G-alpha-q subunit activates PLC
3. PLC liberates IP3 and DAG
4. IP3 activates an IP3 receptor that acts as a calcium release channel in the SR
5. Calcium is released into the intracellular space, increasing [Ca2] and stimulating smooth muscle contraction

Question 42

Alpha2 adrenergic receptors are negatively coupled to ___ via which G-protein?

Answer 42

Adenylyl cyclase; G-alpha-i subunit

Question 43

Describe what happens at an adrenergic nerve terminal when an agonist binds to an alpha2 adrenergic receptor.

Answer 43

1. Agonist binds to alpha-2 receptor
2. G-alpha-i inhibits adenylyl cyclase
3. This reduces cAMP, which reduces activation of PKA
4. Phosphorylation of N-type calcium channels on nerve terminals is reduced, reducing calcium influx during membrane depolarization and reducing vesicular release of NT

Question 44

Beta1 adrenergic receptors are positively coupled to ___ via which G-protein?

Answer 44

Adenylyl cyclase; G-alpha-s

Question 45

Describe what happens in a cardiac pacemaker cell when an agonist binds to an beta1 adrenergic receptor.

Answer 45

1. Agonist binds beta1 receptor
2. G-alpha-s activates adenylyl cyclase
3. Adenylyl cyclase produces cAMP
4. cAMP activates PKA
5. PKA phosphorylates Ca2+ channels in the membrane of SA node cells, leading to increased slow inward calcium current and faster nodal cell depolarization
6. cAMP also directly activates funny currents to increase the slope of depolarization

Question 46

Describe what happens in a cardiac myocyte cell when an agonist binds to an beta1 adrenergic receptor.

Answer 46

1. Agonist binds beta1 receptor
2. G-alpha-s activates adenylyl cyclase
3. Adenylyl cyclase produces cAMP
4. cAMP activates PKA
5. PKA phosphorylates L-type calcium channels in myocyte membranes, leading to enhanced calcium influx and larger trigger signals for release of Ca2+ from the SR. Trigger calcium also enters the SR, increasing storage so that the next trigger initiates larger efflux of calcium.

Question 47

Beta2 adrenergic receptors are positively coupled to ___ via which G-protein?

Answer 47

Adenylyl cyclase; G-alpha-s

Question 48

Describe what happens in vascular smooth muscle when an agonist binds to an beta2 adrenergic receptor.

Answer 48

1. Agonist binds beta1 receptor
2. G-alpha-s activates adenylyl cyclase
3. Adenylyl cyclase produces cAMP
4. cAMP activates PKA
5. PKA phosphorylates and INHIBITS MLCK. This prevents actin and myosin from interacting/muscle from contracting. This phosphorylation also reduces the affinity of MLCK for Ca-calmodulin, resulting in further reduction.

Question 49

Describe what happens in vascular smooth muscle when an agonist binds to an alpha2 adrenergic receptor.

Answer 49

Peripheral vasoconstriction through the opposite mechanism of beta-adrenergic receptors.

Question 50

What are the two categories of adrenomimetic agnoists?

Answer 50

1. Direct-acting

2. Indirect-acting

Question 51

What are the 2 categories of indirect-acting adrenomimetic agonists?

Answer 51

1. Releasers

2. Reuptake inhibitors

Question 52

What are the 2 categories of direct-acting adrenomimetic agonists?

Answer 52

1. Alpha agonists

2. Beta agonists

Question 53

What are the 3 categories of alpha agonists?

Answer 53

1. Nonselective
2. Alpha-1 selective
3. Alpha-2 selective

Question 54

What are the 3 categories of beta agonists?

Answer 54

1. Nonselective
2. Beta-1 selective
3. Beta-2 selective

Question 55

What are the 3 endogenous ligands for adrenergic receptors?

Answer 55

NE, EPI, DA

Question 56

MAP = ?
CO = ?

Answer 56

CO*TPR

HR * SV

Question 57

Total peripheral resistance (TPR) has a predominant effect on ___.

Answer 57

Diastolic pressure (determines rate at which blood leaves the arteries through the resistance vessels)

Question 58

Cardiac output (CO) has a predominant effect on ___.

Answer 58

Systolic pressure (contractility of the heart forces SV into the arterial tree during systole)

Question 59

TPR and diastolic pressure are affected more by ___ receptors expressed in the ___.

Answer 59

Alpha1, alpha2, and beta-2 adrenergic; vasculature

Question 60

CO and systolic pressure are affected more by ___ receptors expressed in ___.

Answer 60

Beta1 adrenergic; cardiac tissue

Question 61

What are the physiologic effects of epinephrine?

Answer 61

1. Low dose: lower diastolic blood pressure (beta2), increase CO/systolic BP (beta1)
2. Higher dose: increase TPR and CO (alpha1, alpha2, beta1)
3. Bronchodilation (beta2)
4. Decreased bronchial secretions (alpha1)

Question 62

What are the potential toxicities of epinephrine?

Answer 62

1. Arrhythmias*
2. Cerebral hemorrhage
3. Anxiety
4. Cold extremities
5. Pulmonary edema

Question 63

What adrenergic receptors does epinephrine stimulate?

Answer 63

Alpha1, Alpha2, Beta1, Beta2 (beta predominates at lower concentrations)

Question 64

What are the indications of epinephrine?

Answer 64

1. Anaphylaxis*
2. Cardiac arrest*
3. Bronchospasm*

Question 65

What are the contraindications of epinpherine?

Answer 65

Later term pregnancy

Question 66

Why is epinephrine short-acting?

Answer 66

It is very susceptible to degradation

Question 67

What receptors doe NE stimulate?

Answer 67

Alpha1, alpha2, beta1

Question 68

What are the physiological effects of NE?

Answer 68

1. Increase CO/HR/systolic BP (beta1)
2. Increase TPR/diastolic BP (alpha1, alpha2)
3. Decrease HR (baroreflex)
4. Overall increase in MAP

Question 69

What are the toxicities of NE?

Answer 69

1. Arrhythmias
2. Ischemia*
3. Hypertension

Question 70

What are the indications of NE?

Answer 70

1. Vasodilatory shock*

Question 71

What are the contraindications of NE?

Answer 71

1. Pre-existing vasoconstriction or ischemia*

2. Late term pregnancy

Question 72

NE is susceptible to degradation by metabolic enzymes; thus, it has a short ___ and must be given by controlled ___.

Answer 72

Half-life; infusion

Question 73

What receptors does DA stimulate?

Answer 73

Dopamine1, dopamine2, beta1, alpha1, alpha2

Question 74

What are the physiological effects of DA?

Answer 74

1. At low rate: decrease TPR (dopamine1) and increase CO (beta1)
2. At high rate: increase MAP and TPR (alpha1, alpha2, beta1)

Question 75

What are the toxicities of DA?

Answer 75

1. Low BP (low infusion rates)*

2. Ischemia (high infusion rate)*

Question 76

What are the indications of DA?

Answer 76

1. Cardiogenic shock*

Question 77

What are the contraindications of DA?

Answer 77

1. Tachyarrhythmias*

2. V. fib.

Question 78

What is isoproterenol?

Answer 78

Non-selective beta-adrenergic agonist (no affinity for alpha receptors)

Question 79

What receptors does isoproterenol stimulate?

Answer 79

Beta1, beta2

Question 80

What are the physiological effects of isoproterenol?

Answer 80

1. Decrease TPR, decrease diastolic BP (beta2)
2. Increase CO, increase systolic BP transiently, but this is overcome by #1 (beta1)
3. Small decrease in MAP
4. Bronchodilation (beta2)

Question 81

What are the toxicities of isoproterenol?

Answer 81

1. Tachyarrhythmias*

Question 82

What are the indications of isoproterenol?

Answer 82

1. Bradycardia w/heart block when TPR is high

Question 83

What are the contraindications of isoproterenol?

Answer 83

1. Angina w/arrhythmias

Question 84

What is dobutamine?

Answer 84

Selective beta-1 adrenergic receptor agonist

Question 85

What does dobutamine bind to?

Answer 85

Beta1>beta2>alpha (considered selective for beta1)

Question 86

What are the physiological effects of dobutamine?

Answer 86

1. Increase CO (beta1)
   * Note that the inotropic effect is > than the chronotropic effect due to lack of beta-2 mediated vasodilation and reflex tachycardia

Question 87

What are the toxicities of dobutamine?

Answer 87

1. Arrhythmias (beta1)
2. Hypotension (beta2)*
3. Hypertension (beta1)

Question 88

What are the indications of dobutamine?

Answer 88

1. Short-term fix for CHF or cardiogenic shock*

2. Excess beta-blockade*

Question 89

What are terbutaline and albuterol?

Answer 89

Selective beta-2 adrenergic agonists

Question 90

What are the physiological effects of terbutaline and albuterol

Answer 90

1. Bronchodilation
2. Uterine relaxation
3. Negligible cardiovascular effects (can cause some beta agonist-like responses)

Question 91

What are the toxicities of terbutaline and albuterol?

Answer 91

1. Tachycardia (beta1)*
2. Muscle tremor (beta2)*
3. Tolerance (beta2)*

Question 92

What are the indications of terbutaline and albuterol?

Answer 92

1. Bronchospasm*

2. Chronic treatment of obstructive airway disease*

Question 93

What is phenylephrine?

Answer 93

Selective alpha1 adrenergic receptor agonist

Question 94

Phenylephrine is not a catecholamine; why is this important?

Answer 94

It is not subject to COMT degradation.

Question 95

What are the physiological effects of phenylephrine?

Answer 95

1. Increase TPR and MAP
2. Decrease HR (baroreflex)
3. Pupillary dilation
4. Decrease bronchiole and sinus secretions

Question 96

What are the toxicities of phenylephrine?

Answer 96

1. Hypertension*

Question 97

What are the indications of phenylephrine?

Answer 97

1. Hypotension during anesthesia
2. SV tachycardia*
3. Mydriatic agent in ophthalmic issues*
4. Nasal congestion*

Question 98

What are the contraindications of phenylephrine?

Answer 98

1. Hypertension

2. V. tach.

Question 99

What is clonidine?

Answer 99

Selective alpha2 adrenergic receptor agonist

Question 100

What are the physiological effects of clonidine?

Answer 100

1. Acute increase in BP (peripheral effect)

2. Reduced BP (central effect by crossing BBB)

Question 101

What are the toxicities of clonidine?

Answer 101

1. Dry mouth*
2. Sedation
3. Bradycardia
4. Hypertensive crisis after acute withdrawal*

Question 102

What are the indications of clonidine?

Answer 102

1. Hypertension due to sympathetic activation*

Question 103

What are indirect acting sympathomimetics?

Answer 103

Drugs that increase [endogenously released catecholamines] at site of release

Question 104

Upon what do the effects of indirect acting sympathomimetics depend?

Answer 104

Whether the drug can cross the BBB

Question 105

What are the 6 major indirect acting sympathomimetics (releasing agents)?

Answer 105

1. Amphetamine
2. Methamphetamine
3. Methylphenidate
4. Ephedrine
5. Pseudoephedrine
6. Tyramine

Question 106

What are the physiological effects of the indirect acting sympathomimetics (releasing agents)?

Answer 106

1. Increased TPR and diastolic BP (alpha1, alpha2)
2. Positive inotropic/chronotropic effects, increased systolic BP (beta1)
3. CNS stimulant (increased NE)
4. Anorexia (increased DA)

Question 107

What are the toxicities of the indirect acting sympathomimetics (releasing agents)?

Answer 107

1. Tachycardia (beta1)*

2. Anxiety (?)

Question 108

What are the indications of the indirect acting sympathomimetics (releasing agents)?

Answer 108

1. ADD*
2. Narcolepsy*
3. Nasal congestion*

Question 109

What are the contraindications of the indirect acting sympathomimetics (releasing agents)?

Answer 109

1. Hypertension
2. Severe atherosclerosis
3. History of drug abuse
4. Treatment with MAO inhibitors within 2 weeks*

Question 110

What are the three main categories of beta-blockers?

Answer 110

1. Non-selective (beta1, beta2)
2. Cardioselective (beta1)
3. Partial agonist (beta1, beta2)

Question 111

What are the three classic non-selective beta-blockers?

Answer 111

1. Propranolol
2. Timolol
3. Nadolol

Question 112

What are the two classic cardioselective beta blockers (plus 1 new one)?

Answer 112

1. Atenolol
2. Metoprolol
3. Esmolol (new)

Question 113

What is the one classic partial agonist beta blocker?

Answer 113

Pindolol

Question 114

Compare the effects of the three categories of beta-blockers on heart rate and force of contraction.

Answer 114

All 3 decrease the rate and force of contraction; however, the partial agonist has a limited bradycardic response due to the partial agonist activity

Question 115

Compare the effects of the three categories of beta-blockers on peripheral resistance.

Answer 115

1. Non-selective: increased, due to unopposed vasoconstriction by alpha1-receptors
2. Cardioselective: little effect, as beta-receptors are not blocked
3. Partial agonist: slight decrease because of partial beta2 agonist properties

Question 116

Compare the effects of the three categories of beta-blockers on renin release.

Answer 116

All three decrease release of renin

Question 117

Compare the effects of the three categories of beta-blockers on the bronchioles.

Answer 117

1. Non-selective: bronchoconstriction, particularly in asthmatics
2. Cardioselective: Less bronchoconstriction, but still not recommended in asthmatics
3. Ditto

Question 118

Compare the effects of the three categories of beta-blockers on glucose metabolism.

Answer 118

1. Non-selective: inhibits effects of EPI; use caution with diabetics using insulin, as it masks symptoms of hypoglycemia
2. Little effect
3. Reduced response to EPI because of partial agonist, but still not as potent as endogenously-released EPI

Question 119

What are the physiological effects of the non-selective beta-blockers?

Answer 119

1. Decreased HR
2. Decreased contractility
3. Decreased renin release
4. Reduced sympathetic activation
5. Inhibition of aqueous humor producttion

Question 120

What are the toxicities of the non-selective beta-blockers?

Answer 120

1. Bronchospasm*
2. Mask symptoms of hypoglycemia*
3. Insomnia
4. Depression
5. Bradycardia*
6. Increased triglycerides*

Question 121

What are the indications of the non-selective beta-blockers?

Answer 121

1. Hypertension*
2. Angina*
3. Glaucoma*
4. Early to moderate heart failure*
5. Arrhythmia*
6. Thyrotoxicosis
7. Anxiety

Question 122

What are the contraindications of the non-selective beta-blockers?

Answer 122

1. Bronchospasm during asthma*
2. Sinus bradycardia*
3. 2nd and 3rd degree heart block*
4. Cardiogenic shock*

Question 123

What are the physiological effects of the cardioselective beta-blockers?

Answer 123

1. Decreased HR
2. Decreased contractility
3. Decreased renin release
4. Reduced sympathetic activation

Question 124

What are the toxicities of the cardioselective beta-blockers?

Answer 124

1. Dizziness
2. Depression
3. Insomnia
4. Hypotension*
5. Bradycardia*

Question 125

What are the indications of the cardioselective beta-blockers?

Answer 125

1. Hypertension*
2. Angina*
3. Arrhythmia*

Question 126

What are the contraindications of the cardioselective beta-blockers?

Answer 126

1. Sinus bradycardia*
2. 2nd and 3rd degree heart block*
3. Cardiogenic shock*

Question 127

When is it beneficial to use a partial agonist beta blocker?

Answer 127

When symapthetic activity is high

Question 128

What are the physiological effects of the partial agonist beta-blockers?

Answer 128

1. Decreased BP
2. Decreased contractility
3. Decreased renin release
4. Reduced sympathetic activation

Question 129

What are the toxicities of the partial agonist beta-blockers?

Answer 129

1. Dizziness
2. Depression
3. Insomnia
4. Hypotension*

Question 130

What are the indications of the partial agonist beta-blockers?

Answer 130

1. Hypertension when other beta blockers are less well-tolerated*

Question 131

What are the contraindications of the partial agonist beta-blockers?

Answer 131

1. Sinus bradycardia*
2. 2nd and 3rd degree heart block*
3. Cardiogenic shock*

Question 132

What are the two classic non-selective alpha-receptor antagonists (classify as reversible/irreversible)?

Answer 132

1. Phenoxybenzamine (irreversible)

2. Phentolamine (reversible)

Question 133

What are the physiological effects of the non-selective alpha-blockers?

Answer 133

1. Decreased BP (alpha blockade unmasks beta effect)

2. Increased inotropy and chronotropy

Question 134

What are the toxicities of the non-selective alpha-blockers?

Answer 134

1. Prolonged hypotension*
2. Reflex tachycardia*
3. Nasal congestion

Question 135

What are the indications of the non-selective alpha-blockers?

Answer 135

1. Hypertension associated w/pheochromocytoma*

2. Vasoconstrictor-induced extravasation*

Question 136

What are the contraindications of the non-selective alpha-blockers?

Answer 136

1. Coronary artery disease

Question 137

What are the selective alpha1 adrenergic blockers?

Answer 137

1. Prazosin
2. Doxazosin
3. Terazosin

Question 138

What are the physiological effects of the alpha1 adrenergic blockers?

Answer 138

1. Inhibits vasoconstriction

2. Prostate smooth muscle relaxation

Question 139

What are the toxicities of the alpha1 adrenergic blockers?

Answer 139

1. Syncopy

2. Orthostatic hypotension*

Question 140

What are the indications of the alpha1 adrenergic blockers?

Answer 140

1. Hypertension*

2. Bengin prostatic hyperplasia (BPH)*