11/2 Adrenergic Antagonists_2/2- Corbett

Question 1

alpha adrenergic antagonists

Answer 1

two general types:

• nonselective: block both alpha1 and alpha2
• ​alpha1-selective

can be reversible or irreversible

CARDIOVASCULAR EFFECTS

• decr peripheral vascular resistance (alpha1 effect)
• decr bp
• cause orthostatic hypotension and reflex tachycardia

other effects

• miosis, nasal stuffiness
• decr resistance to urinary flow

Question 2

non-selective alpha antagonists

Question 3

non-selective alpha antagonists: phenoxybenzamine

route

mech

effect

use

adv effects

Answer 3

PHENOXYBENZAMINE (oral)

• nonselective alpha1 and alpha2 blockade (alpha1>2)
• irreversible receptor blockade lasting 14-48hr
  
  • only irrev agent among alpha blockers! (also only oral)
• blocks NE reuptake at presyn terminals

effect: blocks catecholamine-mediated vasoconst\

use: tx of pheochromocytoma (tumor of adrenal medulla → excessive catecholamine production), often with paroxysmal HTN

• point of premedication: block the alpha effects to allow actual blood volume to rise to a level where it’s safe to operate

adverse effects: postural hypotension, reflex tachycardia, nasal stuffiness, fatigue, nausea

Question 4

non-selective alpha antagonists: phentolamine

route

mech

effect

use

adv effects

Answer 4

PHENTOLAMINE (IV or IM)

• nonselective alpha1 and alpha2 blockade (alpha1=2)
• reversible receptor blockade lasting 4hr

​​effect: decr peripheral resistance, cardiac stimulation

use: tx of pheochromocytoma, in cases of NE extravasation

​adverse effects: severe tachycardia, arrhytmias, myocardial ischemia

Question 5

selective alpha antagonists

4 ex and uses

adverse effects

Answer 5

1. PRAZOSIN

• highly selective alpha1 effects (1000:1 alpha1:2 effect)
  
  • not much effect on heart
• relaxes arterial and venous smooth muscle
• relaxes smooth muscle in prostate

metabolized in liver w/ 3hr half-life

uses: HTN (not first line) and BPH

2. TERAZOSIN: HTN and BPH

3. DOXAZOSIN: HTN and BPH (22h half-life)

4. TAMULOSIN: “uroselective”

• blocks alpha1A and 1D receptors in prostate → selective for BPH

adverse effects

• orthostatic hypotension (esp with first dose)
• dizziness, headache
• drowsiness
• ejaculation issues

Question 6

selective alpha2 antagonists

Answer 6

yohimbine

• used for ED (largely displaced by sudenefil - Viagra)
• works in CNS to increase SNS outflow to periphery
• contraindicated in CVD

mirtazapine

• antidepressant
• central presyn alpha2 antagonist effects → stimulate NE and 5HT release

Question 7

beta-adrenergic antagonists

Answer 7

1. nonselective
2. beta1-selective antagonists: cardio selective
3. antagonists with action against beta1, beta2, alpha1

Question 8

PK of beta blockers

absorption

distribution

excretion

Answer 8

• limited bioavailability when taken orally
  
  • implications for IV admin (much higher availability!)
• large volume of distribution
• most metabolized in liver (except nadolol)

Question 9

esmolol

Answer 9

v v v short acting!

10 min metabolism

only given parenterally

quick metabolism distinguishes it from others

Question 10

CV effects of beta blockers

Answer 10

lowers high blood pressure

• suppression of renin release
• effective ONLY if you have high bp!

negative chronotrope (slowed AV conduction, incr PR interval)

negative inotrope (decr CO, workload, VO2)

beta2 blockade in periphery → acutely increased PVR

Question 11

other effects of beta blockers

Answer 11

respiratory system

• bronchoconstriction (even with beta1 selective drugs)
  
  • contraindicated with severe obstructive disease (FEV1 <50% PV)

metabolic/endocrine effects

• lipolysis blocked → incr VLDL, decr HDL
• impaired glucose tolerance

effects on eye

• reduce intraocular pressure

Question 12

therapeutic effects of beta blockers

Answer 12

1. hypertension (not first line!)

• lowers bp in pt with HTN
• decr CO, renin, systemic vasc resistance over time
• not recommended as 1st line tx

2. myocardial infarction
   * WHY CARDIOPROTECTIVE IN THIS SETTING? reduces myocardial oxygen consumption!!!
3. heart failure

• metoprolol in symptomatic heart failure (reduced EF) - has to be stable!
• same reason as above: decreases oxygen consumption

4. hyperthyroidism
   * high SNS tone of hyperthyroidism can be blocked by beta blockers
5. glaucoma
6. migraine

Question 13

beta blockers: adverse CARDIAC events

Answer 13

1. drug rebound

• can precipitate acute MI in pt with CAD
• ventricular tachyarrhythmia

2. CHF exacerbation (if pt in acute decomp heart failure)
3. bradyarrythmia (pt has AV conduction defect →→→ serious bradyarrhythmia!)

Question 14

beta blockers: adverse NONCARDIAC events

Answer 14

• bronchoconstriction
• worse glycemic control in DM2
• depression, fatigue, sexual dysfx (low risk)
• affects lipid metabolism
• weight gain

Question 15

beta-adrenergic antagonists

non-selective drugs and hallmarks

Answer 15

NONSELECTIVE BETA ANTAGONISTS

• propranolol - prototypical beta blocker
• pindolol - partial agonist activity
• nadolol - v LONG duration action
• timolol - opthalmic, along with betaxolol, carteolol

Question 16

beta-adrenergic antagonists

beta1 selective drugs and hallmarks

Answer 16

BETA1 SELECTIVE ANTAGONISTS - preferred in pt with asthma/COPD/DM

• atenolol, metoprolol, betaxolol, bisoprolol
• acebutolol - partial agonist activity
• esmolol - parenteral, ultrashort action
• nebivolol - most highly beta1 selective agent
  
  • vasodilatory effects via NO release (beta3 receptors)
  • no effect on lipid profile or glycemic control

Question 17

beta-adrenergic antagonists

mixed (beta1/beta2 AND alpha1) drugs and hallmarks

Answer 17

MIXED ANTAGONISTS - beta1, beta2, and alpha1

• carvedilol - used in CHF and HTN
  
  • prob best choice beta blocker (along with nebivolol) in diabetics
  • no alteration in HbA1c noted for DM2 pts
• labetalol

Question 18

summary table

Answer 18