Sympatholytic drugs (Adrenergic blockers) bind to the adrenergic receptors and prevent the action of adrenergic drugs.
These are drugs which block the actions of sympathetic division or catecholamines (adrenaline and noradrenaline).
They are competitive antagonists at both α and β adrenergic receptors.
1. SYMPATHOLYTICS
Prof. Amol B. Deore
• Department of Pharmacology
• MVP’s Institute of Pharmaceutical Sciences, Nashik
2. SYMPATHOLYTICS
•Sympatholytic drugs (Adrenergic blockers) bind to
the adrenergic receptors and prevent the action of
adrenergic drugs.
•These are drugs which block the actions of
sympathetic division or catecholamines (adrenaline
and noradrenaline).
•They are competitive antagonists at both α and β
adrenergic receptors.
3. Adrenergic Receptors
•Adrenaline and noradrenaline are the
neurotransmitters release at the sympathetic post
ganglionic nerve endings.
•The adrenergic receptors are categorized into alpha
and beta adrenergic receptors. Adrenaline acts on both
alpha and beta receptors.
4. Alpha Sympatholytics
• Alpha adrenergic blocking agents
• Alpha receptor antagonists block the adrenergic
responses mediated through alpha adrenergic
receptors.
• Some of them have selectivity for α1 or α2 receptors.
5. • Pharmacological actions of adrenaline and alpha Sympatholytics
Receptor Location
Pharmacological actions
of Adrenaline
Pharmacological actions
of α- Sympatholytics
α1
• Veins, arterioles,
arteries, capillaries
• Urinary sphincter
• Eye Radial muscles
Vasoconstriction and
rise in blood pressure
Contraction
Mydriasis
Vasodilation and fall in
blood pressure
Relaxation
Miosis
α2
• Presynaptic
membrane
• Blood vessels
Control release of NA in
nerve endings
Vasoconstriction and
rise in blood pressure
Increase release of NA
Vasodilation and fall in
blood pressure
7. Pharmacological actions of alpha sympatholytics
• The important effects of α receptor stimulation are α1
mediated vasoconstriction and α2- (presynaptic) receptor
mediated inhibition of NA release.
• α1-blockade—inhibits vasoconstriction --leading to
vasodilation and thereby ↓ BP. This fall in BP is opposed by
the baroreceptor reflexes which tend to ↑ heart rate and
cardiac output.
• α2-blockade—enhances release of NA which stimulates β
receptors (α are already blocked) - β1 stimulation in heart
results in tachycardia and increased cardiac output.
8. Selective α1-blockade—results in hypotension without significant tachycardia.
Selective α2-blockade—↑NA release resulting in hypertension.
α-blockade also results in miosis and nasal stuffiness.
α-blockade in the bladder and prostate leads to decreased resistance to the flow
of urine.
9. Therapeutic uses of alpha sympatholytics
• Hypertension: Selective alpha -blockers like prazosin are used in
the treatment of hypertension. Phenoxybenzamine or
phentolamine can be used in hypertensive crisis.
• Pheochromocytoma: Pheochromocytoma is an adrenal medullary
tumour which secretes large amounts of catecholamines resulting
in hypertension. The tumour has to be removed surgically.
• Phenoxybenzamine and phentolamine are used for the
preoperative management of the patient and during the
operation. Inoperable cases are put on long-term treatment with
phenoxybenzamine.
10. Therapeutic uses of alpha sympatholytics
• Raynaud's disease: A patient with Raynaud's disease experiences
pain in the extremities, for example, the fingers, when temperatures
drop. In Raynaud's disease, smaller arteries that supply blood to your
skin undergo vasoconstriction, restrictive blood circulation to
affected areas.
• Migraines are severe, recurring, and painful headaches. Symptoms
may include nausea, vomiting, difficulty speaking, numbness or
tingling, and sensitivity to light and sound.
12. Therapeutic uses of alpha sympatholytics
• Frostbite may occur when skin is exposed to extreme cold, at
times combined with high winds, resulting in vasoconstriction. The
associated decrease in blood flow does not deliver sufficient heat
to the tissue to prevent the formation of ice crystals.
• Benign prostatic hypertrophy (BPH) Blockade of α1 receptors in
the bladder, prostate and urethra reduce resistance to urine
outflow. Prazosin, tamsulosin and alfuzosin are useful in patients
who cannot be operated upon.
16. Adverse effects of α-blockers
•Postural hypotension, palpitation, nasal stuffiness,
miosis, impaired ejaculation and impotence.
Postural hypotension— is when your blood pressure drops when you
go from lying down to sitting up, or from sitting to standing
17. DALES ADRENALINE REVERSAL PHENOMENON
• Henry Dale was demonstrated adrenaline reversal phenomenon in
1906 by using extract of Ergotoxin on anaesthetized experimental
cat. A characteristic series of changes observed in arterial blood
pressure if adrenaline administered intravenously in anaesthetized
cat.
18. • We should also keep in mind that-
• At higher concentration, adrenaline acts on all receptors (α1, α2,
β1,β2, β3).
• But at lower concentration, adrenaline acts selectively on β2 –
receptors (because β2 are more sensitive)
Receptors Location
Pharmacological action of
Adrenaline
α1
Blood vessels (Veins, Arteries,
Arterioles, Capillaries)
Vasoconstrictions
(increases blood pressure)
β2 Blood vessels (Arteries)
Vasodilatation
(fall in blood pressure)
19. Phase 1:
• If adequate dose of adrenaline is given intravenously in anaesthetized
cat, then there will be rise in blood pressure due vasoconstriction
(α1, β2 effect). The cardiac output, heart rate, conduction velocity
and excitability of heart also increased. This is because initially the
concentration of adrenaline is high. So adrenaline will act on both α1,
β2 receptors.
• Within few second level of adrenaline will decrease due to its rapid
metabolism and neuronal re-uptake. At lower concentration only
action of β2 will predominant. So only fall in Blood pressure seen. So
at this level you can observe initially rise in blood pressure and then
after fall in blood pressure. This is called Biphasic response. (refer
figure)
20. Phase 2:
• After biphasic response, if we administer non-selective alpha
blocker-Ergotoxine intravenously in anaesthetized cat, then it
blocks the α1 receptors on blood vessels (veins, arteries,
arterioles, capillaries).
• Hence Ergotoxine shows vasodilation and fall in blood pressure
i.e. hypotensive action. (refer figure)
21.
22. Phase 3:
• After alpha blocking action, if adequate dose of adrenaline is given
intravenously in same anaesthetized cat, then there will be fall in blood
pressure due vasodilation (β2 effect).
• This is because Ergotoxine already blocks the α1 receptors on blood
vessels. So adrenaline will act only on β2 receptors located on blood
vessels (arteries) to show vasodilation and fall in blood pressure i.e.
hypotensive action. (refer figure)
23. So as We have seen in adrenaline reversal phenomenon-
• 1. First give adrenaline and observe biphasic response
2. Second We give non-selective alpha blocker
3. At last We give adrenaline again and observe only
fall in BP due to unopposed β2 action.
28. • β blockers competitively block the actions of adrenaline on beta
receptors innervated organs especialy heart.
• β1 Blocking action reduces heart rate (-ve chronotropic effect),
myocardial contractility (-ve ionotropic effect), conduction velocity and
excitability of the heart.
• Beta blockers decrease myocardial oxygen consumption by decreasing
heart rate, blood pressure and contractility.
29. • β blockers also inhibit the Renin secretion from the kidney nephrons.
Thereby they produce vasodilation and fall in blood pressure.
• β blockers decrease outflow of the sympathetic impulses from
sympathetic nerves.
• β blockers produce resetting of baroreceptors on the aortic body on the
aorta.
• Therefore β blockers shows antihypertensive activity.