The Autonomic Nervous System

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The Autonomic Nervous System

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Title: The Autonomic Nervous System

1
The Autonomic Nervous System

ISRAA OMAR

2
Autonomic drugs

Autonomic drugs Drugs that produce their
primary therapeutic effect by mimicking or
altering the functions of the autonomic nervous
system .
The autonomic nervous system is composed of
efferent neurons.
These innervate smooth muscle, cardiac muscle
and the exocrine glands, thereby controlling
digestion, cardiac output, blood flow, and
glandular secretions.

3
Activity of the Sympathetic Nervous System

Prepares body for physical action
Fight or Flight
Increased heart rate
Increased blood pressure
Redistribution of blood flow - ? flow to skeletal
muscle, ? flow to skin and organs
? GI activity
Dilation of pupils and bronchioles
? blood glucose

4
Activity of the Parasympathetic Nervous System

Opposite effects to SNS
Prepares the body for feeding and digestion
Slows heart rate
Lowers blood pressure
Promotes GI secretions
Stimulates GI movement
Constricts the pupil
Empties bladder and rectum

In general, the parasympathetic division and the
sympathetic division of the ANS are antagonistic
in their effects on organ systems.

6
The enteric division of the ANS

It is a very large and highly organized
collection of neurons located in the walls of the
gastrointestinal (GI) system.
It regulates and coordinates the motor activity
and secretory functions of the GI system.

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Anatomy of the ANS

Afferent nerve fibers (sensory nerves)
Non-myelinated information is carried to the CNS
by the vagus, pelvic, splanchnic and somatic
nerves.
Efferent nerve fibers (motor nerves)
Sympathetic division
Thoracolumbar division (T1 L2)
Parasympathetic division
Craniosacral division (cranial nerves III, VII,
IX, and X) and sacral region of spinal cord (S2
S4)

Consists of 2 neurons arranged in series
Preganglionic nerve fiber
Postganglionic nerve fiber
Adrenal Medulla is the exception to the two
neuron arrangement (a modified ganglion that
mainly secretes adrenaline hormone)

10
The Peripheral Nervous System
11
PRE-GANGLIONIC
12
GANGLIA
13
POST-GANGLIONIC
14
Cholinergic Agonists

The cholinergic drugs act on receptors that
are activated by acetylcholine.
Location of cholinergic neurons (releases Ach)
Preganglionic fibers terminating in the adrenal
medulla
Preganglionic fibers terminating in autonomic
ganglia (both parasympathetic and sympathetic),
The postganglionic fibers of the parasympathetic
division .
Cholinergic neurons innervate the muscles of the
somatic nervous system
also found in the central nervous system (CNS).

15
Neurotransmission at cholinergic neurons

Involves sequential six steps.
Synthesis, Choline acetyltransferase catalyzes
the reaction of choline with acetyl coenzyme A
(CoA) to form acetylcholine.
Choline acetyl coenzyme A (CoA)
? Choline
acetyltransferas
Acetylcholine
Storage

Release, When an action potential arrives at a
nerve ending, voltage-sensitive calcium channels
on the presynaptic membrane open, causing an
increase in the concentration of intracellular
calcium.
Elevated calcium levels promote the release of
acetylcholine into the synaptic space.
This release can be blocked by botulinum toxin.
Binding of acetylcholine to a receptor
Degradation of the neurotransmitter in the
synaptic gap by acetylcholinesterase enzyme to
choline and acetic acid.
Reuptake of choline by the cholinergic neurons
for synthesis of new ACh.

17
Cholinergic Receptors (Cholinoceptors)

The postsynaptic cholinergic receptors on the
surface of the effector organs are divided into
two classes muscarinic and nicotinic.

18
A. Muscarinic receptors

There are five subclasses of muscarinic
receptors M1, M2, M3, M4, and M5
Only M1, M2 and M3, receptors have been
functionally characterized.

19
Mechanisms of Acetylcholine Signal Transduction

Activation of the M1 or M3 receptors the
receptor undergoes a conformational change and
interacts with Gq protein, which in turn
activates phospholipase C. This leads to an
increase in intracellular Ca2.
Ca2 can then interact to produce the response
(e.g. Secretion, contraction, etc.)
Activation of M2 subtype on the cardiac muscle
stimulates Gi protein,
Gi protein inhibits adenylyl cyclase and
increases K conductance, to which the heart
responds with a decrease in rate and force of
contraction.

20
Selective Muscarinic antagonists

Pirenzepine, a tricyclic anticholinergic drug,
selective M1 muscarinic receptor antagonist
(such as those of the gastric mucosa).
Darifenacin is a competitive muscarinic receptor
antagonist at M3 receptor. The drug is used in
the treatment of overactive bladder.

21
B. Nicotinic receptors

The nicotinic receptor is composed of five
subunits, and it functions as a ligand-gated ion
channel.
Binding of two acetylcholine molecules elicits a
conformational change that allows the entry of
sodium ions, resulting in the depolarization of
the effector cell.

Nicotine (or high doses of acetylcholine)
initially stimulates and then blocks the
receptor.
Nicotinic receptors are located in the CNS,
adrenal medulla, autonomic ganglia, and the
neuromuscular junction.
The nicotinic receptors of autonomic ganglia
(called nicotinic neuronal) differ from those of
the neuromuscular junction (which are called
nicotinic muscular) .

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I. Direct-Acting Cholinergic Agonists

Cholinergic agonists (also known as
parasympathomimetics) mimic the effects of
acetylcholine by binding directly to
cholinoceptors.
Classified into two groups
Choline esters, which include acetylcholine and
synthetic esters of choline, such as carbachol
and bethanechol.
Naturally occurring alkaloids, such as
pilocarpine constitute the second group .

All direct-acting drugs have longer durations of
action than acetylcholine.
Drugs (e.g. pilocarpine and bethanechol) which
bind to muscarinic receptors are also referred to
as muscarinic agents.

25
1. Acetylcholine

Acetylcholine is a quaternary ammonium compound
that cannot penetrate membranes.
It is not useful therapeutically because of its
multiplicity of actions and its rapid
inactivation by the cholinesterases (unstable).

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Major Actions of Acetylcholine

Acetylcholine has both muscarinic and nicotinic
activity. Its actions include
CVS
Decrease in heart rate (negative chronotropic
effect) and cardiac output
The actions of acetylcholine on the heart mimic
the effects of vagus nerve stimulation.

Decrease in blood pressure
Acetylcholine activates M3 receptors found on
endothelial cells lining the smooth muscles of
blood vessels. This results in the production of
nitric oxide from arginine.
Note nitric oxide is also known as
endothelium-derived relaxing factor and is a
vasodilator

Other actions
In the gastrointestinal tract, acetylcholine
increases salivary secretion and stimulates
intestinal secretions and motility.
In the lungs, Bronchiolar secretions are also
enhanced.
In the genitourinary tract, the tone of the
detrusor urinae muscle is increased, causing
expulsion of urine.

In the eye, acetylcholine is involved in
stimulating ciliary muscle contraction for near
vision and in the constriction of the pupillae
sphincter muscle (circular muscle), causing
miosis (marked constriction of the pupil).

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2. Bethanechol

Bethanechol is not hydrolyzed by
acetylcholinesterase
It posses strong muscarinic activity, but lacks
nicotinic activity.
It is used to treat urinary retention. as well
as megacolon.
Adverse effects sweating, salivation, flushing,
decreased blood pressure, nausea, abdominal pain,
diarrhea, and bronchospasm.

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3. Carbachol

Carbachol has both muscarinic as well as
nicotinic actions .
It is a poor substrate for acetylcholinesterase
Therapeutic uses carbachol is rarely used
therapeutically except in the eye as a miotic
agent to treat glaucoma by causing pupillary
constriction and a decrease in intraocular
pressure.

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4. Pilocarpine

The alkaloid pilocarpine is a tertiary amine and
is stable to hydrolysis by acetylcholinesterase .
Pilocarpine is the drug of choice in both
narrow-angle (also called closed-angle) and
wide-angle (also called open-angle) glaucoma.

33
II. Indirect-Acting Cholinergic
Agonsists(Anticholinesterases)

These drugs can provoke a response at all
cholinoceptors in the body, including
- both muscarinic and nicotinic receptors of
the autonomic nervous system,
- nicotinic receptors of skeletal muscle
- and muscarinic and nicotinic receptors in
the brain.

34
A. Reversible anticholinesterases 1.
Physostigmine

Used in treatment of atony of intestine and
bladder as it increases motility of either
organ.
It is used to treat glaucoma
Used in the treatment of overdoses of drugs with
anticholinergic actions, such as atropine,
phenothiazines, and tricyclic antidepressants.

Adverse effects (shown by high doses)
Convulsions .
Bradycardia and a fall in cardiac output
Accumulation of acetylcholine and, ultimately,
paralysis of skeletal muscle.

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2. Neostigmine

Similar actions to that of physostigmine.
Unlike physostigmine, neostigmine has a
quaternary nitrogen hence, it is more polar and
does not enter the CNS.
Neostigmine is used to stimulate the bladder and
GI tract, and it is also used as an antidote for
tubocurarine

Also used in symptomatic treatment of myasthenia
gravis ( an autoimmune disease caused by
antibodies to the nicotinic receptor at
neuromuscular junctions. This causes their
degradation and, thus, makes fewer receptors
available )
Adverse effects include salivation, flushing,
decreased blood pressure, nausea, abdominal pain,
diarrhea, and bronchospasm.

39
3. Pyridostigmine and ambenomium

Cholinesterase inhibitors that are used in the
chronic management of myasthenia gravis.
Their durations of action are longer than that of
neostigmine.
Adverse effects of these agents are similar to
those of neostigmine.

40
4. Demecarium

Cholinesterase inhibitor used to treat chronic
open-angle glaucoma (primarily in patients
refractory to other agents) and closed-angle
glaucoma after irredectomy.
Mechanism of actions and side effects are similar
to those of neostigmine.

41
5. Edrophonium

Prototype short-acting agent (duration of action
is 10 to 20 minutes).
The actions are similar to those of neostigmine,
except that it is more rapidly absorbed and has a
short duration of action
Edrophonium is used in the diagnosis of
myasthenia gravis. Intravenous injection of
edrophonium leads to a rapid increase in muscle
strength.

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6. Other reversible anticholinesterases

Tacrine, donepezil, rivastigmine, and
galantamine
Are useful in patients with Alzheimer's disease
(they have a deficiency of cholinergic neurons in
the CNS).
Gastrointestinal distress is their primary
adverse effect.

43
B. Irreversible Anticholinesterases

Some synthetic organophosphate compounds have
the capacity to bind covalently to
acetylcholinesterase. The result is a
long-lasting increase in acetylcholine at all
sites where it is released.
Many of these drugs are extremely toxic and were
developed by the military as nerve gases (sarin,
soman, tabun).
Related compounds, such as parathion, are
employed as insecticides.

44
1. Echothiophate

Echothiophate is an organophosphate.
It is an irreversible anticholinesterase
The enzyme becomes permanently inactivated, and
restoration of acetylcholinesterase activity
requires the synthesis of new enzyme molecules.
Echothiophate is used in treatment of open-angle
glaucoma.
Atropine in high dosage can reverse many of the
muscarinic and some of the central effects of
echothiophate.
Pralidoxime can reactivate inhibited
acetylcholinesterase enzyme.

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2. Other irreversible anticholinesterases

Nerve gases sarin, soman, tabun
These are organophosphorus compounds
Used as chemical warfare
Malathion and Parathion
These are organophosphorus compounds
Used as insecticides
Toxic effects could be treated with immediate
administration of pralidoxime and atropine

46
Cholinergic Antagonists

The cholinergic antagonists (also called
cholinergic blockers, parasympatholytics or
anticholinergic drugs) bind to cholinoceptors.
Include
Antimuscarinic Agents block muscarinic synapses
of the parasympathetic nerves.
The ganglionic blockers, which block the
nicotinic receptors of the sympathetic and
parasympathetic ganglia.
The skeletal neuromuscular blocking agents

47
A. Antimuscarinic Agents

Antimuscarinic drugs have little or no action at
skeletal neuromuscular junctions or autonomic
ganglia.

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1. Atropine

Atropine, a tertiary amine belladonna alkaloid,
that binds competitively to muscarinic receptors,
preventing acetylcholine from binding to those
sites.
Atropine acts both centrally and peripherally.

Pharmacological action
Eye
Persistent mydriasis and cycloplegia (inability
to focus for near vision).
In patients with narrow-angle glaucoma
intraocular pressure may rise dangerously.
Gastrointestinal (GI)
Antispasmodic, gastric motility is reduced but
hydrochloric acid production is not significantly
affected.
Urinary system
Reduces hypermotility states of the urinary
bladder.

Cardiovacular
With higher doses of atropine, the M2 receptors
on the sinoatrial node are blocked, and the
cardiac rate increases (tachycardia).
Secretions
Atropine blocks the salivary glands, producing a
drying effect on the oral mucous membranes
(xerostomia).
Sweat and lacrimal glands are also affected.
Note Inhibition of secretions by sweat glands
can cause elevated body temperature.

Therapeutic uses of atropine
Ophthalmic for eye examination. Atropine may
induce an acute attack of eye pain due to sudden
increases in eye pressure in individuals with
narrow-angle glaucoma.
Antispasmodic to relax the GI tract and bladder.
For the treatment of overdoses of cholinesterase
inhibitor insecticides and some types of mushroom
poisoning (muscarine poisoning).
As preanesthetic medication to block secretions
in the upper and lower respiratory tracts prior
to surgery.

Pharmacokinetics
Atropine is readily absorbed, partially
metabolized by the liver, and eliminated
primarily in the urine. It has a half-life of
about 4 hours.
Adverse effects
Dry mouth, blurred vision, tachycardia, and
constipation.
Effects on the CNS include restlessness,
confusion, hallucinations, and delirium
Contraindications
In older individuals, the use of atropine may
exacerbate an attack of glaucoma and / or
urinary retention.

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2. Scopolamine

Tertiary amine belladonna alkaloid,
Used prophylactically for treatment of motion
sickness.
Produces sedation (atropine causes excitation).
Scopolamine may produce euphoria and is subject
to abuse.

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3. Ipratropium

Inhaled ipratropium, a quaternary derivative of
atropine, is useful in treating asthma.
Ipratropium is also useful in chronic
obstructive pulmonary disease(COPD).

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4. Tropicamide and cyclopentolate

Used as ophthalmic solutions as mydriatics.
Their duration of action is shorter than that of
atropine.

56
B. Ganglionic Blockers

Ganglionic blockers act on the nicotinic
receptors of both parasympathetic and sympathetic
autonomic ganglia.
These drugs are not effective as neuromuscular
blockers

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1. Nicotine

A component of cigarette smoke and a poison with
many undesirable actions.
Nicotine is available as patches, lozenges,
gums, and other forms.
The drug is effective in reducing the craving
for nicotine in people who wish to stop smoking.

Pharmacological action
Nicotine initially stimulates, then blocks all
sympathetic and parasympathetic ganglia.
The stimulatory effects include increased blood
pressure and cardiac rate (due to release of
noradrenaline from adrenergic terminals and
adrenaline hormone from the adrenal medulla)
Nicotine causes increased peristalsis and
secretions

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2. Mecamylamine and trimethaphan

These are ganglion blockers.
They are used to lower blood pressure in
emergency situations.

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Drugs affecting the sympathetic nervous system

Drugs that act directly on the adrenergic
receptor (adrenoceptor) and activate them are
said to be sympathomimetics.
Blockers of adrenoceptors are called
sympatholytics
There are drugs which affect presynaptic
adrenergic function.

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Adrenergic neurons

Adrenergic neurons synthesize, store and release
norepinephrine (noradrenalin).
Adrenergic neurons are found in the sympathetic
nervous system (postganglionic sympathetic
neurons) and in the central nervous system (CNS).

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Neurotransmission At Adrenergic Neurons

The process involves five steps
Synthesis,
Storage,
Release,
Receptor binding of norepinephrine
Removal of the neurotransmitter from the synaptic
cleft.

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Synthesis of norepinephrine

Tyrosine is transported into the axoplasm of the
adrenergic neuron, where it is hydroxylated to
DOPA by tyrosine hydroxylase.
This is the rate-limiting step in the formation
of norepinephrine.
DOPA is then decarboxylated by dopa
decarboxylase to form dopamine.
Dopamine is hydroxylated to form norepinephrine
by the enzyme, dopamine ß-hydroxylase.
In the adrenal medulla, norepinephrine is
methylated to yield epinephrine (adrenaline).

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Binding with adrenoceptors

Binding of norepinephrine to the membrane
receptors triggers a cascade of events, resulting
in the formation of intracellular second
messengers.
Adrenergic receptors use both the cyclic
adenosine monophosphate (cAMP) second-messenger
system, and the phosphatidylinositol cycle, to
transduce the signal into an effect.

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Termination of norepinephrine actions

Norepinephrine may
Diffuse out of the synaptic space and enter the
general circulation,
Be metabolized by catechol o-methyltransferase
(COMT) in the synaptic space,
Be recaptured by an uptake system that pumps the
norepinephrine back into the neuron. Uptake of
norepinephrine into the presynaptic neuron is the
primary mechanism for termination of
norepinephrine's effects.

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Fate of reuptaken norepinephrine

Norepinephrine may be released by another action
potential, or it may stored,
Alternatively, norepinephrine can be oxidized by
monoamine oxidase (MAO) present in neuronal
mitochondria.

68
Adrenergic receptors (adrenoceptors)

Adrenoceptors are designated a and ß.
For a receptors, the rank order of potency is
epinephrine gtnorepinephrine gtgt isoproterenol
(isoprenaline).
For ß receptors, the rank order of potency is
isoproterenol gt epinephrine gt norepinephrine.

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A. a adrenoceptors

The a adrenoceptors are subdivided into two
subgroups, a1 and a2
a1 Receptors
Found on the postsynaptic membrane of the
effector organs
Activation of a1 receptors initiates a series of
reactions through a G protein resulting in the
generation of inositol-1,4,5-trisphosphate (IP3)
and diacylglycerol (DAG) from phosphatidylinositol
.
IP3 initiates the release of Ca2 from the
endoplasmic reticulum into the cytosol, and DAG
turns on other proteins within the cell.
The a 1 receptors are further divided into a 1A,
a 1B, a 1C, and a 1D

a2 Receptors
are located primarily on presynaptic nerve
endings.
The stimulation of a2 receptor causes
inhibition of further release of norepinephrine.
a2 Receptors are also found on presynpatic
parasympathetic neurons. Norepinephrine can
diffuse and interact with these receptors,
inhibiting acetylcholine release.
The effects of binding at a2 receptors are
mediated by inhibition of adenylyl cyclase and a
fall in the levels of intracellular c-AMP.
a 2 receptors are further divided into a 2A, a
2B, a 2C, and a 2D.

Tamsulosin
is a selective a 1A antagonist
is used to treat benign prostate hyperplasia. The
drug is clinically useful because it targets a1A
receptors found primarily in the urinary tract
and prostate gland.

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B. ß-adrenoceptors

The ß-adrenoceptors can be subdivided into three
major subgroups, ß1, ß2, and ß3,.
ß1 Receptors
Have approximately equal affinities for
epinephrine and norepinephrine (mainly found in
the heart)
ß2 receptors
Have a higher affinity for epinephrine than for
norepinephrine (mainly found in the bronchioles)
ß3 receptors
Are involved in lipolysis.

Binding of a neurotransmitter at any of the three
ß receptors results in activation of adenylyl
cyclase and, therefore, increased concentrations
of cAMP within the cell.

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Distribution of receptors

Tissues such as the vasculature skeletal muscle
have both ß1 and ß2 receptors, but the ß2
receptors predominate.
The heart contains predominantly ß1 receptors.

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Effects mediated by the adrenoceptors

Stimulation of ß1 receptors characteristically
causes cardiac stimulation,
Stimulation of ß2 receptors produces
vasodilatation (in skeletal vascular beds) and
bronchiolar relaxation.

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Desensitization of receptor

Prolonged exposure to the catecholamines reduces
the responsiveness of these receptors, a
phenomenon known as desensitization.

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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
High potency
Rapid inactivation by COMT and by MAO .
Poor penetration into the CNS because they are
polar

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Adrenergic agonists

Classification of the adrenergic agonists
Direct-acting agonists include
epinephrine, norepinephrine, isoproterenol, and
phenylephrine.
Indirect-acting agonists include
amphetamine, cocaine and tyramine.
Mixed-action agonists include
ephedrine, pseudoephedrine and metaraminol, may
act directly and indirectly.

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A. Direct-Acting Adrenergic Agonists

1. Epinephrine
Is a catecholamine.
Interacts with both a and ß receptors.
At low doses, ß effects (vasodilatation)
predominate, whereas at high doses, a effects
(vasoconstriction) are strongest.

Pharmacological effects
Epinephrine strengthens the contractility of the
myocardium (positive inotropic ß1 action) and
increases the heart rate (positive chronotropic
ß1 action).
Epinephrine increases systolic blood pressure,
coupled with a slight decrease in diastolic
pressure.
Epinephrine causes powerful bronchodilation (ß2
action).

Epinephrine inhibits the release of allergy
mediators such as histamines from mast cells.
Epinephrine has a significant hyperglycemic
effect because of increased glycogenolysis in the
liver (ß2 effect), increased release of glucagon
(ß2 effect), and a decreased release of insulin
(a2 effect).
Lipolysis Epinephrine initiates lipolysis
through its agonist activity on the ß receptors
of adipose tissue

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Metabolism of Epinephrine

Epinephrine is metabolized by two enzymatic
pathways MAO, and COMT.
The final metabolites found in the urine are
metanephrine and vanillylmandelic acid.

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Therapeutic uses

Treatment of acute asthma and anaphylactic
shock, epinephrine is the drug of choice.
Glaucoma in open-angle glaucoma. It reduces the
production of aqueous humor.
Cardiac arrest Epinephrine may be used to
restore cardiac rhythm.
Anesthetics Local anesthetic solutions usually
contain 1100,000 parts epinephrine. The effect
of the drug is to greatly increase the duration
of the local anesthesia. It does this by
producing vasoconstriction at the site of
injection.

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Adverse effects

CNS disturbances include anxiety, fear,
tension, headache, and tremor.
Cerebral hemorrhage as a result of a marked
elevation of blood pressure.
Cardiac arrhythmias
Pulmonary edema.

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Interactions

Hyperthyroidism Epinephrine may have enhanced
cardio-vascular actions in patients with
hyperthyroidism.
Cocaine In the presence of cocaine, epinephrine
produces exaggerated cardiovascular actions.
Diabetes Epinephrine increases the release of
endogenous stores of glucose. In the diabetic,
dosages of insulin may have to be increased.

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2. Norepinephrine

Cardiovascular actions
Vasoconstriction Both systolic and diastolic
blood pressures increase
Norepinephrine is used to treat shock, because
it increases vascular resistance and, therefore,
increases blood pressure. However, metaraminol is
favored.

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3. Isoproterenol

Isoproterenol is a direct-acting synthetic
catecholamine that predominantly stimulates both
ß1- and ß2-adrenergic receptors
Therapeutic uses
It can be employed to stimulate the heart in
emergency situations.

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4. Dobutamine

Dobutamine is a synthetic, selective ß1 agonist.
Dobutamine is used to increase cardiac output in
congestive heart failure.

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5. Oxymetazoline

Oxymetazoline is a direct-acting synthetic
adrenergic agonist that stimulates both a1- and
a2-adrenergic receptors.

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6. Phenylephrine

Phenylephrine is a direct-acting, synthetic a 1
receptors agonist.
It is not a catechol derivative and, therefore,
not a substrate for COMT.
Phenylephrine is a vasoconstrictor that raises
both systolic and diastolic blood pressures.
Phenylephrine acts as a nasal decongestant and
produces prolonged vasoconstriction.

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7. Methoxamine and clonidine

Methoxamine is a direct-acting, synthetic a1
receptor agonist.
Clonidine is an a2 agonist that prevents further
release of noradrenaline.
It is used in hypertension as it acts on a2
receptors in the CNS..
It can be used in withdrawal from opiates or
benzodiazepines.

8. Metaproterenol
The drug is an agonist at ß2 receptors,
producing little effect on ß1 receptors of the
heart.
The drug is useful as a bronchodilator in the
treatment of asthma
9. Albuterol, pirbuterol, and terbutaline
are short-acting ß2 agonists used primarily as
bronchodilators .
10. Salmeterol and formoterol
are selective ß2-agonists, long-acting
bronchodilators.
These agents are highly efficacious when combined
with a corticorsteroid.

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B. Indirect-Acting Adrenergic Agonists

They potentiate the effects of norepinephrine
produced endogenously, but these agents do not
directly affect postsynaptic receptors.

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1. Amphetamine

Central stimulant, abused drug
Its peripheral actions are mediated primarily
through the release of stored norepinephrine and
the blockade of norepinephrine uptake.

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2. Tyramine

It is not a clinically useful drug, but it is
important because it is found in fermented foods,
such as cheese.
Normally, it is oxidized by MAO in the
gastrointestinal tract, but if the patient is
taking MAO inhibitors, it can precipitate a
hypertensive crisis in him.

96
3. Cocaine

Cocaine is a local anesthetic (sodium channel
blocker) and is a CNS stimulant (blocks the
reuptake of norepinephrine, thus potentiating NA
effects).
Drug of abuse.

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C. Mixed-Action Adrenergic Agonists

Mixed-action drugs induce the release of
norepinephrine, and they activate postsynaptic
adrenergic receptors.
Ephedrine, and pseudoephedrine are plant
alkaloids, that are now made synthetically.
Ephedrine produces bronchodilation
Pseudoephedrine is used to treat nasal and sinus
congestion.

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D. Adrenergic Antagonists (also called blockers
or sympatholytic agents)

A. a-Adrenergic Blocking Agents
The a-adrenergic blocking agents,
phenoxybenzamine and phentolamine, have limited
clinical applications, they are nonselective a
blockers

1. Phenoxybenzamine
is used in the treatment of pheochromocytoma, a
catecholamine-secreting tumor of the adrenal
medulla.
Adverse effects Phenoxybenzamine can cause
postural hypotension, nasal stuffiness, nausea,
and vomiting.
2. Phentolamine
Phentolamine is also used for the short-term
management of pheochromocytoma.

100

3. Prazosin terazosin, doxazosin, and tamsulosin
are selective competitive blockers of the a1
receptor.
The first three drugs are useful in the treatment
of hypertension.
Tamsulosin is indicated for the treatment of
benign prostatic hyperplasia.
Doxazosin is the longest acting of these drugs.

101

The first dose of these drugs produces an
exaggerated orthostatic hypotensive response that
can result in syncope (fainting). This action,
termed first-dose effect.
Tamsulosin is a more potent inhibitor of the a1A
receptors found on the smooth muscle of the
prostate. This selectivity accounts for
tamsulosin's minimal effect on blood pressure.

102

4. Yohimbine
Is a selective a2 blocker.
It is found as a component of the bark of the
yohimbe tree and is sometimes used as a sexual
stimulant (aphrodisiac) or cardiovascular
stimulant.

103
B. ß-Adrenergic Blocking Agents

Nonselective ß-blockers act at both ß1 and ß2
receptors, whereas cardioselective ß antagonists
block ß1 receptors
Note There are no clinically useful ß2
blockers.
Although all ß-blockers lower blood pressure in
hypertension, they do not induce postural
hypotension, because the a-adrenoceptors remain
functional.

104

ß-Blockers are also effective in treating
Angina,
Cardiac arrhythmias,
Myocardial infarction,
Congestive heart failure,
Hyperthyroidism,
Glaucoma, as well as serving in the prophylaxis
of migraine headaches.

105
1. Propranolol

A nonselective ß blocker
Sustained-release preparations for once-a-day
dosing are available.
Actions
Cardiovascular Propranolol diminishes cardiac
output, having both negative inotropic and
chronotropic effects.
Cardiac output, work, and oxygen consumption are
decreased by blockade of ß1 receptors these
effects are useful in the treatment of angina.
The reduction in cardiac output leads to
decreased blood pressure.

106

Bronchoconstriction Blocking ß2 receptors in the
lungs of susceptible patients causes contraction
of the bronchiolar smooth muscle.
Non-selective ß-blockers, are contraindicated in
patients with COPD or asthma.
ß-blockade leads to decreased glycogenolysis and
decreased glucagon secretion, thus pronounced
hypoglycemia may occur after insulin injection in
a patient using propranolol.
ß-Blockers also mask the normal physiologic
response to hypoglycemia.

107
Mechanisms of action

Propranolol lowers blood pressure in hypertension
by
Decreased cardiac output is the primary
mechanism,
Inhibition of renin release from the kidney and
decreased sympathetic outflow from the CNS also
contribute to propranolol's antihypertensive
effects

108

Adverse effects
Bronchoconstriction
Arrhythmias Treatment with ß-blockers must never
be stopped quickly because of the risk of
precipitating cardiac arrhythmias, which may be
severe.
Sexual impairment

109

Drug interactions
Drugs that interfere with the metabolism of
propranolol, such as cimetidine, fluoxetine,
paroxetine, and ritonavir, may potentiate its
antihypertensive effects.
Conversely, those that stimulate its metabolism,
such as barbiturates, phenytoin, and rifampin,
can decrease its effects.

110

2. Timolol and nadolol
Nonselective ß blockers,
are more potent than propranolol.
3. Acebutolol, atenolol, metoprolol, and esmolol
Selective ß1 blockers
Esmolol has a very short lifetime. It is only
given intravenously if required during surgery or
management of poisoning.
4. Pindolol and acebutolol
blockers with partial agonist activity

111

5. Labetalol and carvedilol
blockers of both a- and ß- adrenoceptors
Carvedilol also decreases lipid peroxidation and
vascular wall thickening, effects that have
benefit in heart failure.
Labetalol may be employed as an alternative to
methyldopa in the treatment of pregnancy-induced
hypertension.
Intravenous labetalol is also used to treat
hypertensive emergencies, because it can rapidly
lower blood pressure.

112
Drugs Affecting Neurotransmitter Release or Uptake

Some agents act on the adrenergic neuron, either
to interfere with neurotransmitter release or to
alter the uptake of the neurotransmitter.
1. Reserpine
Reserpine, a plant alkaloid that causes the
depletion of biogenic amines.
Sympathetic function, in general, is impaired
because of decreased release of norepinephrine.

113

2. Guanethidine
Guanethidine blocks the release of stored
norepinephrine as well as displaces
norepinephrine from storage vesicles (thus
producing a transient increase in blood
pressure).
This leads to gradual depletion of norepinephrine
in nerve endings except for those in the CNS.
Guanethidine commonly causes orthostatic
hypotension and interferes with male sexual
function.

114

3. Alpha methyl dopa
Antihypertensive
Mechanism Transformed to alpha methyl
noradrenaline in adrenergic neuron,
When released, alpha methyl noradrenaline acts as
agonist on presynaptic alpha2 receptors. Thus
further release of transmitter is inhibited.

The Autonomic Nervous System - PowerPoint PPT Presentation

The Autonomic Nervous System

The Autonomic Nervous System ISRAA OMAR – PowerPoint PPT presentation