Cholinomimetics

Question 1

What are the main subtypes of muscarinic receptors?

Answer 1

M1:	Neural
 - Salivary glands
 - Stomach
 - CNS
M2: Cardiac	
 - Heart
M3: exocrine glands and smooth muscle
 - Salivary glands
 - Bronchial/visceral SM
 - Sweat glands
 - Eye
M4:	Periphery
 - CNS
M5: Striatal dopamine release	
 - CNS

General rule - muscarinic receptors are excitatory apart from M2 receptors in the heart which are inhibitory

Question 2

What type of receptor are muscarinic receptors?

Answer 2

Type 2 - G protein coupled

Distinguishing feature of type 2 receptors are the 7 transmembrane segments (alpha helices)

Question 3

What are the M1 and M3 subtype receptors linked to?

Answer 3

Gq protein –> increases IP3 and DAG

Question 4

What is M2 subtype receptor linked to?

Answer 4

Gi protein (inhibitory) –> decreases the production of cAMP

Question 5

How many subunits are there in nicotinic receptors and what subunits are in the different types of nicotinic receptors

Answer 5

5 subunits - alpha, beta, gamma, delta, epsilon

Muscle type: 2 alpha, beta, epsilon
Ganglion type: 2 alpha, 3 beta (CNS similiar)

The effect of ACh is relatively weak - you need more ACh to stimulate nicotinic than muscarinic receptors

Question 6

Where are muscarinic cholingeric receptors found?

Answer 6

Eye
Salivary glands
Lungs
Bladder
Gut
Heart
Vasculature (most vessels don't have parasympathetic innervation)
Sweat glands (sympathetic)

Question 7

What are the muscarinic effects of the eye?

Answer 7

Contraction of ciliary muscle: bulging of the lense accommodation for near vision

Contraction of the sphincter pupillae (circular muscle of the iris): Miosis and improves drainage of intraocular fluid

Lacrimation (tears)

Question 8

How does the contraction of the sphincter pupillae improve intraocular drainage?

Answer 8

AH is produced in the ciliary bodies, bathes the lens and cornea. Contraction opens the pathway for aqueous humour to drain into via the the canals of Schlemm and reducing intraoccular humour.

Question 9

What are the muscarinic effects on the heart?

Answer 9

M2 receptors in the atria and nodes:
Stimulation = decreased production of cAMP
Decreased Ca2+ –> decreased CO
Increased K+ efflux –> decreased HR

Question 10

What are the muscarinic effects on the vasculature?

Answer 10

Most blood vessels do not have parasympathetic innervation but they do have muscarinic receptors.

ACh acts on the M3 AChR on the vascular endothelial cells (not smooth muscle cells) to stimulate NO release.
NO induces vascular smooth muscle relaxation = decrease in TPR

See diagram

Question 11

Summarise the muscarinic effects on the CVS?

Answer 11

Decreased HR
Decreased CO (due to decreased atrial contraction)
Vasodilation (stimulation of NO production)

= Sharp drop in BP. (be careful when using muscarinic agonists)

Question 12

Muscurinic effects on non-vascular smooth muscle?

Answer 12

Smooth muscle that does have parasympathetic innervation responds in the opposite way to vascular smooth muscle. i.e it contracts

Lung: Bronchoconstriction
Gut: Increased peristalsis (motility)
Bladder: Increased bladder emptying

Question 13

What are the muscarinic effects on the exocrine glands?

Answer 13

Salvation
Increased bronchial secretion
Increased gastro-intestinal secretions (including gastric HCL)
Increased sweating (SNS-mediated)

Question 14

Summarise the muscarinic effects on the body?

Answer 14

See slides

Question 15

What are the two types of cholinomimteic drugs?

Answer 15

Directly acting

Indirectly acting

Question 16

What are the typical directly acting cholinomimetic drug agonists at muscarinic receptors?

Answer 16

1) Choline esters (bethanechol) (some degree of selectivity of M3 receptors)
2) Alkaloids (pilocarpine) (only targets muscarinic receptors)

Question 17

Describe pilocarpine

Answer 17

Non-selective muscarinic agonist
Good lipid solubility (good for eye use. Given locally)
Plasma half life; 3-4hrs

Question 18

What is pilocarpine useful for?

Answer 18

Effective local treatment of glaucoma - useful in opthalmology

Question 19

What are the side effects on pilocarpine?

Answer 19

If it does get into the systemic system you will see.

• blurred vision (effect on the lens)
• sweating
• GI disturbance and pain
• hypotension
• respiratory distress

Question 20

Describe bethanochol

Answer 20

Very similar to ACh
M3 selective agonist
Resistant to degradation, orally active and with limited access to the brain
Plasma half life; 3-4hrs

Question 21

What is the main use of bethanochol?

Answer 21

Assist bladder emptying and to enhance gastric motility post op

Question 22

What are the side effects of bethanochol?

Answer 22

• impaired vision
• sweating
• bradycardia
• hypotension
• respiratory difficulty

Question 23

What are the indirectly acting cholinomimetic drugs?

Answer 23

increase effect of normal parasympathetic nerve stimulation - effectively using ACh

Question 24

What are the types of indirectly acting cholinomimetic drugs?

Answer 24

Reversible anticholinesterases: physostigmine, neostigmine, donepezil (aricept)

Irreversible anticholinesterases: ecthiopate, dyflos, sarin

Question 25

What are the cholinesterase enzymes?

Answer 25

Metabolise ACh to choline and acetate

Acetylcholinesterase 
Butyrylcholinesterase (pseudocholinesterase)

Question 26

Describe acetylcholinesterase

Answer 26

Found in all cholinergic synapses
Very rapid action (hydrolysis; >10000 reactions per second)
Highly selective for ACh - active site has a serine residue.

Question 27

Describe butyrylcholinesterase

Answer 27

Found in the plasma and most tissues but not in cholinergic synapses.
Broad substrate specificity - hydrolyses other esters such as suxamethonium

This is reason why we gave low plasma ACh

Shows genetic variation

Question 28

Describe the effects o cholinesterase inhibitors

Answer 28

Low dose
Enhanced muscarinic activity (see above)

Moderate dose
Further enhancement of muscarinic activity
Increased transmission at ALL autonomic ganglia (nAChRs)

High dose (toxic)
Depolarising block at autonomic ganglia & NMJ (see PT9 NMJ lecture)

Question 29

What is the mechanism of action of revesible anticholinesterase drugs?

Answer 29

Physostigmine

Competes with ACh for the active site on the cholinesterase enzyme to prevent ACh from binding.

The carbamyl group is removed by slow hydrolysis (mins rather than msecs) which increases the duration of ACh activity in the synapse

Question 30

Describe physostigmine?

Answer 30

Primarily acts at the postganglionic PS synapse

Plasma half life; 30 mins

Question 31

What is physostigmine used for?

Answer 31

Treatment of glaucoma (aids in intraocular fluid drainage)

Also used to treat atropine poisoning (particularly in children)

Question 32

Describe the irreversible anticholinesterase drugs?

Answer 32

Organophosphate compounds - ecothiopate

Question 33

What is the mechanism of action of irreversible anticholinesterase drugs?

Answer 33

Rapidly react with the enzyme active site, leaving a large blocking group.

This is stable and resistant to hydrolysis - recovery may require the production of new enzymes (days/weeks)

Question 34

Describe ecothiopate

Answer 34

Potent inhibitor of ACh

Slow reactivation of the enzyme by hydrolysis takes several days

Question 35

What are the uses of ecothiopate?

Answer 35

Used as eye drops in treatment of glaucoma –> prolonged duration of action

Question 36

What are the side effects of ecothiopate?

Answer 36

Systemic side effects:

• sweating
• blurred vision, GI pain
• bradycardia
• hypotension
• respiratory difficulty

ALL PREDICTABLE SIDE EFFECTS OF THE STIMULATION OF MUSCARINIC RECEPTORS

Question 37

Describe antichoinesterase drugs and the CNS

Answer 37

Non-polar anticholinesterases (e.g. physostigmine; nerve agents) can cross the blood brain barrier

Low doses: Excitation with possibility of convulsions

High doses: Unconsciousness, respiratory depression, death

Question 38

Describe the treatment of organophosphate poisoning?

Answer 38

Accidental exposure to organophosphates used in insecticides, or deliberate use as nerve agents can cause severe toxicity ( muscarinic activity; CNS excitation; depolarising NM block)

Treatment: atropine (iv); artificial respiration; pralidoxime (iv) (only compound which can reverse irreversible inhibitors within the first coupe of hours)
NB: Phosphorylated enzyme ‘ages’ within few hours

See diagram