PHAR 736 Midterm 2 (Antagonists)

Question 1

General purpose of B-blockers in CHF

Answer 1

CHF is cycle of sympathetic activation. Goal of pharmacological intervention is to inhibit progressive deterioration of cardiac function.

Question 2

B1-selevtive antagonists (general)

Answer 2

All are competitive (antagonists, inverse agonists, or partial agonists)

Effects most pronounced under conditions of stress or exercise

Question 3

B1-selective antagonists therapeutic indications

Answer 3

Post MI therapy, Ischemic heart disease, Angina (decrease O2 demand on heart, decrease workload on cardiac muscle)

Prevention of ventricular tachycardic arrhythmias (decrease heart rate, decrease AV nodal conduction, and increase refractory period; classified as Class 2 anti-arrhythmic agents)

Compensatory cardiac hypertrophy (block the overgrowth of the heart muscle - cardiac remodeling - due to excess SNS activity)

Hypertension (see hypertension notecard)

Question 4

B1-selective antagonists and hypertension

Answer 4

NOT FIRST LINE

Decrease in cardiac output (b1 blockade) resulting in decreased systolic BP

Decrease in renin secretion (b1 blockade in kidney) resulting in vasodilation

Other less understood factors may contribute to decrease in BP with use of B receptor antagonists

Question 5

Contraindications for B1-selective antagonists

Answer 5

Insulin-dependent diabetes:
>masks symptoms of hypoglycemia (increased HR, tremors) of vital importance to diabetics

• *hyperglycemia is the main problem in diabetics and is toxic in the long-term
• *hypoglycemia, a side effect of insulin treatment, can kill quickly

Question 6

B1-selective or non-selective antagonists in those with asthma/COPD?

Answer 6

B1-Selective

blocking B2 adrenergic receptors would inhibit pulmonary relaxation

Question 7

B1-selective antagonists side effects

Answer 7

Bradycardic arrhythmias (block of B1 in heart, particularly a problem for those with inadequate myocardial reserve)

Fatigue and exercise intolerance (blockade of B1 receptors in the heart)

Withdrawal syndrome

Question 8

Describe B1-selective antagonists withdrawal syndrome

Answer 8

Rebound tachycardia upon abrupt withdrawal due to receptor supersensitization.

MI may ensure in susceptible patients.

Problematic for up to 2 weeks following cessation of therapy.

Discontinue by tapering the dose.

Question 9

Metoprolol, Atenolol

Answer 9

Reduce basal activity of cardiac B1 receptors

Inverse agonists (awful super-sensitization)

Question 10

Acebutolol

Answer 10

Weak B1 partial agonist (and partial antagonist) - used by itself has ~20% efficacy

Moderately decreases cardiac output and heart rate

Very little receptor supersensitivity, better withdrawal profile

Effects of blockade are more apparent under conditions of stress or exercise

Question 11

Acebutolol is particularly useful in patients that can…

Answer 11

Tolerate changes in cardiac output

Question 12

How does Acebutolol work in the presence of a full agonist?

Answer 12

Acts like an antagonist in presence of full agonist (e.g. NE)

Weak partial agonist as NE presence diminishes

Question 13

Esmolol

Answer 13

Very short duration B1 blocker

Used to treat ventricular tachycardic arrythmias and in other situations where brief cardiac blockade is warranted

Question 14

Pharmacogenomic considerations for B1 blockers

Answer 14

People with two Arg alleles more responsive in terms of cardiac stimulation to sympathomimetics than those with at least one Gly allele.

Bucindolol acts as an inverse agonist in patients with the Arg alleles. Acts as a neutral antagonist in patients with at least one Gly allele.
**Effective in HF only if patient has Arg alleles

Question 15

B2-selective antagonists

Answer 15

NONE of therapeutic value currently marketed

Question 16

Non-selective B adrenergic antagonists therapeutic indications

Answer 16

Chronic glaucoma (decrease aqueous humor production by blocking B1 and B2 in eye)

Hyperthyroidism symptoms (blocks symptoms mimicking SNS over-activity, no effect on the disease itself)

Performance anxiety (reduced nervousness through CNS effects and fine motor tremors)

Tremors (drug induced tremors, such as accompany lithium carbonate treatment; Familial palsy (NOT PARKINSONS)

Prophylactic Treatment of migraines (MOA unknown; does not work acutely)

Hypertension

Ventricular tachycardic arrhythmias, Post MI therapy, angina, HF (same as B1 selective blockers, which are generally preferred now for these indications)

Question 17

B non-selective and hypertension

Answer 17

Decrease in cardiac output (B1 blockade) resulting in decreased systolic BP

Decrease in renin secretion (B1 blockade in kidney) resulting in vasodilation

Paradoxical effects:
>short term B2 blockade in normotensives will cause a little bit of vasoconstriction (expected)
>B2 blockade in hypertensives leads to decreased systolic AND diastolic BP (may have to do with adrenergic receptors playing a role in tissue remodeling)

Question 18

B Non-selective antagonists contraindications

Answer 18

Asthma/COPD (blocks bronchodilation)

Insulin-dependent diabetes (should work by decreasing glucagon release and aiding in lowering blood sugar, BUT can mask symptoms of hypoglycemia)

Question 19

B non-selective antagonists side effects

Answer 19

Exercise intolerance:
Reduced airflow, restriction of blood flow to skeletal muscles, reduced cardiac output

Hyperkalemia (generally only a problem for those prone to electrolyte imbalance, but can be a problem during exercise as skeletal muscle uptake of potassium is reduced)

Mast cell degranulation

Bradycardic arrhythmias (blockade of B1 receptors in heart, particularly in patients with inadequate myocardial reserve)

Malaise (sedation, fatigue, depression) - due to CNS effects
**depression may occur in susceptible population

Withdrawal syndrome

Question 20

Describe B non-selective antagonists withdrawal syndrome

Answer 20

Rebound tachycardia upon abrupt withdrawal due to receptor supersensitization.

MI may ensue in susceptible patients.

Problematic for up to 2 weeks following cessation of therapy.

Discontinue by tapering the dose.

Question 21

Propranolol

Answer 21

Precursor of all B-antagonists

CNS penetrating (decreases nervousness and tremors for performance anxiety, familial and drug-induced tremors)

MOST COMMON agent for performance anxiety.

Decreases HR and cardiac output; decreases systolic BP, inhibits renin production, and peripheral resistance with chronic use to treat hypertension

Used topically to treat glaucoma by inhibiting aqueous humor production

Question 22

Sotalol

Answer 22

Little or no blood/brain barrier permeability (no sedation)

Used predominantly for cardioprotective effects

Question 23

Pindolol

Answer 23

Partial agonist (partial antagonist in presence of full agonist)

Similar advantages to acebutolol

Question 24

Timolol

Answer 24

Used topically to treat glaucoma

Be careful in asthmatics, systemically absorbed

Question 25

A-1 selective antagonists indications

Answer 25

Benign prostatic hyperplasia (urinary retention and outflow difficulties; blocks a-1 mediated constriction of bladder sphincter and prostate capsule; longterm, may block hypertrophy of the prostate capsule)

Hypertension (blocks a-1 mediated vasoconstriction; decrease peripheral resistance)

Congestive heart failure (decreased peripheral resistance leads to less workload and increases cardiac output; patient MUST be able to tolerate an increase in heart rate)

Frostbite and Reynaud’s syndrome (increased blood flow to the extremities)

Off-label for nightmares in PTSD patients (Prazosin crosses BBB)

Question 26

a-1 selective antagonist side effects

Answer 26

Tachycardia (reflex tachycardia due to decrease in MABP)

Syncope and orthostatic or postural hypotension (blocks ability to respond to gravitational effects on BP; dose at bedtime and remain supine for 2 hours to avoid syncope; remind patients to be careful after taking a hot shower or hot tub)

Nasal congestion

Sexual side effect in men (inhibition of ejaculation)

Question 27

Prazosin, Terazosin, Alfuzosin

Answer 27

a-1 selective

Antihypertensives, decrease peripheral resistance

Treatments for benign prostatic hyperplasia

Question 28

Unique quality of Prazosin

Answer 28

Crosses BBB

Question 29

Unique quality of Alfuzosin

Answer 29

Less sexual side effects

Question 30

Tamsulosin, Silodosin

Answer 30

a-1 selective (selective for a1A over a1B)
**70% of receptors in the prostate are a1A

treatment for benign prostatic hyperplasia

Not very effective anti-hypertensive, but dizziness and fainting are possible side effects

Question 31

Nebivolol

Answer 31

B1 antagonist (10 fold more selective than metoprolol)

Metabolites promote endothelial NO-dependent vasorelaxation (metabolites may have partial B2 agonist properties or act at serotonin receptors on endothelium)

Summative effects include a reduction in HR and a reduction in BP

Question 32

Labetolol

Answer 32

Mix of 4 stereoisomers, each with unique properties
>RR: B1 antagonist and B2 partial agonist
>SR,SS: a1 antagonist
>RS: no activity

Uptake 1 inhibitor (indirect agonist)

Overall effect:
>block a1 receptors, decrease peripheral resistance
>block B1 receptors, decrease cardiac output, renin secretion
>partial B2 agonist, increased vasodilation in skeletal muscle

Very effective antihypertensive agent

Question 33

Carvedilol

Answer 33

Mix of 2 enantiomers
>S: B antagonist
>R and S: a1 antagonist

Good antihypertensive agent

Additional antioxidant and antiproliferative effects on vascular smooth muscle protect against atherosclerotic complications of hypertension

Question 34

Non-selective a1/a2 antagonists

Answer 34

Used to manage pheochromocytoma in combination with propranolol

Considered “dirty” drugs - block serotonin receptors, histamine and muscarinic activity which makes for complex pharmacology

Question 35

Non-selective a1/a2 antagonist side effects

Answer 35

Much more tachycardia than with a1 selective agents (block of a2 inhibition of baroreflex leads to greater baroreflex response; blockade of a2 inhibition of NE release onto heart leads to greater NE release)

Question 36

Phentolamine

Answer 36

Competitive a-antagonist

Quick reversal of numbness following dental anesthetics (vasodilates to disperse the local anesthetic more quickly)

GI side effects

Question 37

Phenoxybenzamine

Answer 37

Irreversible a-antagonist, alkylating agent

Long duration antagonist (effective longer than 24 hours)

Reversal requires synthesis of new receptors

Question 38

How does a1 mediate urinary retention?

Answer 38

Controls constriction of prostate smooth muscle and constriction of bladder sphincter