Cholinergic System Drugs PDF

Summary

This document provides an overview of the autonomic nervous system in relation to pharmacology, and specifically focusing on cholinergic system drugs.. It details the different components of the system and the roles acetylcholine plays, including the excitatory and inhibitory functions of acetylcholine on different parts of the body.

Full Transcript

Pharmacology of the Autonomic Nervous System:
Cholinergic System Drugs
Dr. Eman Milad Maddy

Introduction

The autonomic nervous system (ANS) is a branch of the peripheral nervous
system (PNS) that regulates the function of the viscera. It innervates smooth muscle
as well as glands and is further divided into;

the parasympathetic and sympathetic systems.

The ANS has an essential role in controlling internal organ function, regulating
heart rate, blood pressure, micturition, sweating, sexual function and gastrointestinal
transit (digestion and defecation).

Broadly speaking the two branches of the ANS can be thought of as opposing or
antagonistic systems, with the sympathetic arm acting as the exciter (eliciting the
“fight or flight” response) and the

parasympathetic as the suppressor (eliciting the “rest and digest” response).

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Parasympathetic nervous system

The parasympathetic nervous system consists of many pathways that connect its
craniosacral components with the peripheral tissues.

Each parasympathetic pathway consists of two neurons, the presynaptic
(preganglionic) and postsynaptic (postganglionic) neurons, which are connected by
the axons of the presynaptic neurons.

The presynaptic neurons of the parasympathetic system are located within
the medulla oblongata and sacral spinal cord. They give off long axons (presynaptic
fibers) that leave the CNS and travel towards the postsynaptic neurons. Once they
reach them, the presynaptic fibers synapse with the bodies of the postsynaptic
neurons.

This synapse uses the acetylcholine as a neurotransmitter, which is why the
parasympathetic pathways are referred to as the cholinergic pathways. The presynaptic
neurons of the parasympathetic pathways are located within the two major parts of the
central nervous system:

The postsynaptic neurons are found within the parasympathetic ganglia, which
typically lie near or within the target organs.

After receiving the impulse from the presynaptic neuron, the postsynaptic neuron
conveys the neural impulse further down its axon (postsynaptic fiber).

The postsynaptic fibers are significantly shorter than the presynaptic ones, given that
the postsynaptic neuronal bodies lie in the close proximity of their target organs.

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What is acetylcholine (ACh)?

Acetylcholine (ACh) is a neurotransmitter, a chemical that carries messages from your
brain to your body through nerve cells. It’s an excitatory neurotransmitter.

This means it “excites” the nerve cell and causes it to “fire off the message.”

Acetylcholine gets its name from the two substances that it’s made from — an acetyl
group (acetyl coenzyme A, which comes from the sugar molecule glucose) and the
nutrient choline.

Acetylcholine is involved in many important functions in your body.

It plays a major role in voluntary muscle movement all over your body.

Nerve cells stimulate muscle nerve cells, causing muscles to contract.

It also plays an important role in brain nerve cells, in such processes as memory,
thinking and learning.

Acetylcholine synthesis

An enzyme called choline acetyltransferase causes a reaction between choline and the
acetyl group to create acetylcholine.

It’s made at the end of nerve cells.

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How does acetylcholine (ACh) work?

Acetylcholine is stored at the end of nerve cells until it’s triggered to be released.

Once released from the end of the nerve cell, it moves into a space called the synaptic
cleft.

The synaptic cleft is between the nerve cell from which acetylcholine was released
(the presynaptic nerve cell) and the next nerve cell acetylcholine is going to (the
postsynaptic nerve cell).

Once acetylcholine moves across the synapse, it can bind to two types of receptors:
nicotinic receptors and muscarinic receptors. There are two subtypes of nicotinic
receptors and five types of muscarinic receptors.

After binding to the receptors, the chemical message moves along to the next nerve
cell and then the process repeats until the message arrives at its destination.

Acetylcholine in the synapse is broken down by an enzyme called acetylcholinesterase
into choline and acetate. These products are reabsorbed and recycled so they can be
used again in transmitting another chemical message.

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What does acetylcholine (ACh) do?

When it binds to muscarinic receptors, it:

Regulates heart contractions and blood pressure and decreases heart rate.

Moves food through your intestine by contracting intestinal muscles and increasing
stomach and intestine secretions.

Causes glands to secrete substances such as tears, saliva, milk, sweat and digestive
juices.

Controls the release of urine.

Contracts muscles that control near vision.

Causes an erection.

Acetylcholine Receptors

There are two types of Ach receptors: nicotinic and muscarinic.

They are named this way because the muscarinic receptors can get activated by a
substance called muscarine (mushroom poison) but not by nicotine, while the nicotinic
receptors can get activated by nicotine.

Acetylcholine can activate both of these receptors. Although both are ligand-gated
(Ach-gated), the nicotinic and muscarinic receptors differ in structure, location and
signal transduction mechanisms.

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Nicotinic receptors

Nicotinic receptors are found on the neurons of the central and peripheral nervous
systems, as well as on the muscle cells within the neuromuscular junctions.

There are two types of nicotinic receptors, namely N1 and N2.

The NM receptors are those found within the neuromuscular junctions, while
the NN are found on the postganglionic neurons of the ANS. the N1 receptors are
often called the muscle nicotinic receptors, and their function is to elicit voluntary
muscle movement in the skeletal muscle.

The function of N2 receptors is to transmit signals from the preganglionic to
postganglionic nerves in both sympathetic and parasympathetic systems.

By the type of signal transduction, the nicotinic receptors are ion-channel receptors,
or ionotropic receptors. As such, upon the binding of Ach, the nicotinic receptors
specifically induce the formation of an ion channel on the cell membrane of the
effector cell (called ligand-gated ion channel), through which positively
charged ions (cations) can enter into the cell. The influx of ions leads to the

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 depolarization of the cell membrane and generation of an action potential, which is
observed as e.g. muscle contraction

When it binds to nicotinic receptors, it:

Allows skeletal muscle to contract.

Causes the release of adrenaline and norepinephrine from your adrenal glands.

Activates your sympathetic system with the release of norepinephrine.

Both types of receptors are involved in memory, including long-term and working
memory, memory formation and consolidation and retrieval.

Within your brain, acetylcholine is also involved in motivation, arousal, attention,
learning and promoting rapid eye movement (REM) sleep.

Muscarinic receptors

Muscarinic receptors. There are five types of them, termed M1, M2, M3, M4 and
M5.

M1 receptors are mostly found in the cerebral cortex, gastric, and salivary glands

M2 receptors are located on the cell membranes of the smooth and cardiac muscle

M3 are also found on the smooth muscle cells, but also on the gastric and salivary
glands
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 M4 and M5 are found predominantly in the substantia nigra and hippocampus

The type of signal transduction, the muscarinic receptors are G-protein coupled
receptors (GPCRs)

As such, they produce effects through second messenger system

The response may be either stimulatory or inhibitory in respect to the cell’s function.
In particular, the M1, M3 and M5 receptors are excitatory, meaning that their
activation increases the activity of the cell.

On the other hand, the M2 and M4 receptors are inhibitory, as their activation results
in the inhibition of the target cell.

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Muscles of iris & pupil:

A-sphincter pupillae (circular Muscle)
B- dilator pupillae (radial muscle)

The sphinctor pupillae →receive only parasympathetic innervations (M3)
leading to miosis →iris stretched →filtration angle widens→↑drainage of
aqueous humor →↓IOP

The dilator papillae → receive only sympathetic innervations(α1)→ contraction
of muscle → active mydriasis

Accommodation

The accommodation reflex is the visual response for focusing on near objects.

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 The ciliary ms receive only parasympathethtic innervations →contraction of
ciliary ms therefore suspensory ligament become loose → convex lens fixing eye
on near vision → accommodation

cycloplegia

Parasymptholytic →ciliary ms relaxed the ligament get taught & lens become less
convex paralysis of accommodation (cycloplegia)

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Effects of Drugs on Cholinergic Transmission

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Muscarinic agonists (parasympathomimetics)

muscarinic agonists divide into two groups: direct agonist and indirect agonist.

Direct agonists resist acetylcholinesterase, thus preventing its breakdown.

Indirect agonists work by inhibiting the acetylcholinesterase enzyme preventing the
degradation of acetylcholine.

Direct and indirect agonists both increase acetylcholine concentration in the synapse,
prolonging acetylcholine effects on the receptor.

Direct Agonists

Bethanechol

Choline esters

indications include postoperative ileus, neurogenic ileus, and urinary retention.

Bethanechol increases the smooth muscle tone of the gastrointestinal tract to promote
motility and restores peristalsis in the absence of obstruction.

Bethanechol also increases the tone of the detrusor muscle to increase bladder
emptying.

Carbachol

Choline esters is indicated to treat open-angle glaucoma, acute angle-closure
glaucoma, and increased intraocular pressure.

Carbachol contracts the ciliary body muscle and opens the trabecular meshwork.

Opening the meshwork increases aqueous humor outflow from the eye to reduce
intraocular pressure.

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Pilocarpine

Cholinomimic Alkaloids

is indicated for open-angle glaucoma, acute angle-closure glaucoma, and ocular
hypertension. When given topically, pilocarpine contracts the ciliary body muscle and
opens the trabecular meshwork to increase the outflow of aqueous humor.

Oral pilocarpine can be used to increase secretion of the salivary glands to treat dry
mouth in patients with Sjogren's syndrome or salivary gland dysfunction.

Methacholine

Choline esters

is most commonly used to diagnose asthma or bronchial hyperactivity. Methacholine
stimulates the muscarinic receptor in the airway when inhaled and induces
bronchoconstriction, and increases tracheobronchial secretions.

The lower the dose it takes for methacholine to induce bronchoconstriction, the more
reactive the bronchial airway is.

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Indirect Agonists
Anticholinesterases drugs
Cholinesterase inhibitors (also called acetylcholinesterase inhibitors) are a group of
medicines that block the normal breakdown of acetylcholine.

Cholinesterase inhibitors block the action of the enzyme cholinesterase, which is
responsible for breaking down acetylcholine.

This increases levels of acetylcholine in the synaptic cleft (the space between two
nerve endings).

Anticholinesterases drugs

Classification:

1. Reversible anticholinesterases

2. Irreversible anticholinesterases

Reversible Acetylcholinesterase Inhibitors

Reversible AChE inhibitors play an important role in pharmacological manipulation of
the enzyme activity. These inhibitors include compounds with different functional
groups (carbamate, quaternary or tertiary ammonium group), and have been applied in
the diagnostic and/or treatment of various diseases such as: myasthenia gravis, AD,
post-operative ileus, bladder distention, glaucoma, as well as antidote to
anticholinergic overdose.

Edrophonium used in diagnosis of myasthenia gravis because of it has short duration
of action (5- 15min.)

Neostigmine used in treatment of myasthenia gravis, paralytic ileus

Reverse neuromuscular block (1- 2hr.)
Pyridostigmine used in treatment of myasthenia gravis, better absorbed than
neostigmine and longer duration of action (3- 6hr.)
Ambenonium used in treatment of myasthenia gravis
Physostigmine used in treatment of glucoma

myasthenia gravis
a chronic autoimmune disorder in which antibodies destroy the communication between
nerves and muscle, resulting in weakness of the skeletal muscles. Myasthenia gravis
affects the voluntary muscles of the body, especially those that control the eyes, mouth, throat
and limbs.

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 Myasthenia gravis is a chronic (long-lasting) neuromuscular condition (it affects the
junction between your nerves and muscles). There isn’t a cure, but effective treatment
can help you manage your symptoms and function well.

Tacrine

Galantamine, donepezil, and rivastigmine are indicated for Alzheimer disease. The
medications help with memory loss as well as decrease plaque build-up. Galantamine,
donepezil, and rivastigmine do not cure Alzheimer disease and can only delay the
progression of the disease.

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 Irreversible anticholinesterases(Organophosphates
Parathion

Malathion

Both used as insecticides

Echothiophat
Used in treatment of glucoma

All has long duration of action

Effects of Muscarinic Agonists
Muscarinic agonists are agents that activate the muscarinic acetylcholine receptor.
There are five different muscarinic receptors labeled M1-M5. Muscarinic agonists are
parasympathomimetics, and their mechanism of action is different depending on
which receptor is activated.

The M1, M3, and M5 are transmembrane receptors that couple to a Gq protein. The
Gq protein upregulates phospholipase C (PLC). PLC cleaves phosphatidylinositol 4,5-
bisphosphate (PIP2) into 1,2- diacylglycerol (DAG) and inositol 1,4,5-triphosphate
(IP3).

DAG activates protein kinase C, which activates downstream protein and causes
calcium influx. IP3 causes the sarcoplasmic reticulum to release stored calcium.
Increased intracellular calcium causes smooth muscle contraction and exocrine
glandular secretions.

The M2 and M4 receptors are Gi receptor, which inhibits adenylyl cyclase. Inhibition
of adenylyl cyclase decreases cyclic adenosine 3’,5’-monophosphate (cAMP)
production from ATP. The decrease in cAMP concentration subsequently decreases
the activation of protein kinase A.

The clinically significant muscarinic receptors are the M1, M2, and M3 receptors.

The M1 muscarinic receptor is clinically significant in the central nervous system,
and it influences neurologic functions.

Muscarinic agonists play an important role in the treatment of Alzheimer
disease(AD).

The M2 muscarinic receptor is the predominant receptor found in the sinoatrial and
atrioventricular nodal cells of the heart.

The downstream effect, once the M2 receptor is activated, allows potassium efflux.
Potassium efflux results in hyperpolarization and reduction of the action potential

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 duration in the nodal cells. Therefore, the activation of the M2 receptor in the heart
causes decreased heart rate and atrial contractility.

The M3 muscarinic receptor is clinically significant in the intestine's smooth muscle,
bladder, airway, eye, exocrine glands, and blood vessels. Smooth muscle of the
intestine, bladder, airway, and the eye.

contracts when calcium concentration increase within the cell. Calcium binds with
calmodulin to form a complex that can now activate the enzyme myosin light chain
kinase. Myosin light chain kinase phosphorylates myosin resulting in contraction.

Muscarinic agonists' action on blood vessels results in vasodilatation rather than
vasoconstriction. Calcium in the endothelial cells activates nitric oxide synthase,
converting L-arginine into nitric oxide. Nitric oxide diffuses into the underlying
smooth muscle causing an increase in cGMP. cGMP activates myosin light chain
phosphatase resulting in smooth muscle relaxation. When the endothelium is
damaged, it does not produce nitric oxide and acetylcholine results in smooth muscle
contraction

Administration

Bethanechol is administered orally on an empty stomach two to four times a day to
prevent stomach upset and nausea.

Carbachol is commonly administered topically ocularly.

Pilocarpine is administered topically, ocularly, or orally.

Methacholine is administered through inhalation.

Neostigmine is administered through intramuscular, intravenous, and subcutaneous
injection.

Physostigmine is administered intravenously.

Galantamine, donepezil, and rivastigmine are administered orally.

Edrophonium is administered through intramuscular injection.

Pyridostigmine is administered orally.

Adverse Effects

Adverse effects of muscarinic agonists can be memorized using the mnemonic
"DUMBBELSS."

Diarrhea

Urination

Miosis
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 Bronchospasm

Bradycardia

Excitation of skeletal muscle and CNS

Lacrimation

Sweating

Salivation

Contraindications

Asthma or Chronic Obstructive Pulmonary Disease (COPD)

Peptic Ulcer

Coronary Vascular Disease

Hyperthyroidism

Toxicity
Organophosphate agents are used for insecticides and work by irreversibly inhibiting
acetylcholine esterase. Excess acetylcholine act on muscarinic and nicotinic receptors
and present with signs of acetylcholine toxicity. Toxicity characteristically
demonstrates overactive parasympathetic stimulation and presents with symptoms of
diarrhea, urination, miosis, bronchospasm, bradycardia, excitation of skeletal muscle
and CNS, lacrimation, sweating, and salivation.

Cholinergic crisis, sometimes known by the mnemonic "SLUDGE syndrome"
(Salivation, Lacrimation, Urination, Defecation, Gastrointestinal distress and Emesis)

Organophosphate poisoning antidotes are atropine and pralidoxime. Atropine is a
muscarinic antagonist, and pralidoxime can regenerate acetylcholinesterase

What medical conditions are associated with low levels of
acetylcholine (ACh)?
Low levels (deficiency) of acetylcholine play an important role in several diseases, the
most common being:

Alzheimer’s disease. People who have Alzheimer’s disease don’t have enough
acetylcholine in their brains.

Lambert-Eaton myasthenic syndrome. This disorder is caused by a reduction in the
release of acetylcholine from nerve cells.

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 Myasthenia gravis. This is an autoimmune disorder in which there’s a rapid
weakening of skeletal muscles after repeated use. Some of the body’s antibodies
interfere with acetylcholine receptors at the neuromuscular junction.

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Cholinergic Antagonists (Parasympatholytic)

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Musscarinic Antagonists(Parasympatholytics)
atropine belladonna alkaloids

Hyoscine

glycopyrrolate

Propantheline selective action on GIT Antispamodic

Atropine

Homatropine passive mydrsis, cycloplegia

cyclopentolate used in ophthalmology examination

benztropine

Orphenadrine used in parkinsonism

benzhexol

ipratropium
tiotropium used in bronchial asthma and COPD

oxybutynin
Tolterodine used in urinary incontinence

Hyoscine used in motion sickness, preanethetic medication , it produce
amnesia and drowsiness

Pirenzepine and Telenzepine used in treatment of peptic ulcer

Antagonists at M1 receptors

Atropine used in treatment of sinus bradycardia

Mechanism of Action
Muscarinic receptors are predominately present on glandular cells, smooth muscle
cells, and cardiac muscle cells. The parasympathetic nervous system releases ACh,
which binds to and activates muscarinic receptors. Muscarinic receptor antagonists
function by competitively blocking the binding of ACh to muscarinic receptors
resulting in an anticholinergic response.

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 Muscarinic receptor antagonists function by acting as competitive inhibitors on the
numerous muscarinic receptors.

There are five different muscarinic receptors: M1, M2, M3, M4, and M5. The M1,
M4, and M5 receptors are in the central nervous system (CNS), and the action of these
agents on these receptors can manifest as cognitive impairment.

The M2 receptors are found in cardiac tissue and are predominately in the
atrioventricular (AV) and sinoatrial (SA) nodal cells, resulting in decreased heart rate
and reduced atrial contractility. Therefore, muscarinic receptor antagonist binding
to M2 receptors leads to an increase in heart rate.

M3 receptors are on the smooth muscle of the gastrointestinal tract, urinary tract,
airway, and blood vessels.

Muscarinic receptor antagonist binding to M3 receptors reduces intestinal
peristalsis and bladder contraction, reduces salivary and gastric secretions,
reduces bronchial secretions, and increases bronchodilation

Adverse Effects
adverse effects of confusion and disorientation.

The action of muscarinic receptor antagonists on M2 receptors in cardiac tissue leads
to tachycardia.

Muscarinic receptor antagonists acting on M3 receptors in exocrine glands can lead to
dry mouth, dry skin, and sore throat. Moreover, muscarinic receptor antagonists act
on receptors in the eyes resulting in mydriasis and photophobia.

Muscarinic receptor antagonists also cause decreased smooth muscle tone, resulting
in constipation, ileus, urinary retention, and gastroesophageal reflux

Contraindications
myocardial infarction

hyperthyroidism

paralytic ileus

benign prostatic hyperplasia

urinary retention

narrow-angle glaucoma

myasthenia gravis.

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 Toxicity
Clinical features of muscarinic receptor antagonist toxicity include dry mouth,
blurry vision, hyperthermia, tachycardia, mydriasis, delirium, and
hallucinations.

Physostigmine, an acetylcholinesterase inhibitor, is used as the antidote for
muscarinic antagonist toxicity.

Ganglion Stimulating Drugs
Nicotine, Lobeline.
These drugs act only on nicotinic receptors, and cause generalized stimulation of
autonomic ganglia.
They have no clinical use, used only experimentally.

Ganglion Blocking Drugs
Trimetaphan
Mecamylamine, Hexomethonium
Act by competitive inhibition of Ach receptors, at postsynaptic membrane.
These drugs were used as antihypertensive but now only Trimetaphan is used
During general anesthesia to produce controlled hypotension to decrease bleeding
during surgery,
Also used in emergency in case of malignant hypertension

Side Effects of ganglion Blocking Drugs
Hypotension results mainly from block of sympathetic ganglia causes arterial
vasodilatation.
Moderate Tachycardia due to parasympathetic inhibition at S A node
Constipation due to inhibition of parasympathetic effects
Urinary retention
Sexual function impaired.

Neuromuscular Blocking Drugs (Muscle Relaxants)
They are classifed in to two groups:
1. Non depolarizing blocking drugs.
2. Depolarizing blocking drugs.

Non depolarizing blocking drugs.
Curare
Metocurare
Gallamine
Pancuronium
Rocuronium

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 Vecuonium
Atracurium
Hivacurium
Cisatracurium (most common used clinically)
They act by competitive block of Ach receptors at post junctional membrane
They do not cross BBB, and also do not cross placenta
All are quarterly ammonium compounds.
Their effects are mainly due to motor paralysis
The first muscle affected are small muscles of eyes, then larger muscle of the body.
The last muscles affected and first to recover are respiratory muscles.

Side Effects:
Hypotension and broncospasm due to ganglion block and histamine release specify
with Tubacurarine.
Less common with other drugs.

Depolarizing blocking drugs.
Succinylcholine (Suxamethonium) (used clinically)
Decamethoium
(agonists at Ach receptors)
Mechanism of action
Phase I Block (Depolarizing)
First these drugs depolarize membranes by opening Na-K channels leading to
repetitive excitation which might lead to muscle fasciculation.
This phase followed by block of neuromuscular transmission and flaccid paralysis.

Phase II Block (Desensitization)
This phase not well understood
Continues exposure to Succinylcholine will lead to repolarization of membrane and
this is thought may lead to receptors desensitization.

Side Effects of Depolarizing Drugs:
1. Bradycarbia
2. Hyperkalemia
3. Malignant Hyperthermia
4. Muscle pain
5. Prolonged paralysis
6. Increased intraocular pressure

Malignant Hyperthermia

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 This is congenital (autosomal dominant) condition leads to muscle spasm and increase
in body temperature ,this case occur with exposure to cretin drugs such as
Succinylcholine and Halothane.
This condition causes excessive release of Ca from sarcoplasmic reticulum.
Treatment with Dantrolene (dirct acting muscle relaxant) this drug inhibit ca release
from sarcoplsmic reticulum.

Clinical use of Muscle Relaxants:
The main use of neuromuscular blocking drugs is in surgical anesthesia to obtain
muscular relaxation such as;
Abdominal wall relaxation to facilitate surgical operation
Muscle relaxation during orthopedic surgery.
To prevent trauma during electroshock therapy in psychiatric diseases

Best of luck

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