Cholinomimetics

Question 1

what produces muscarinic effects?

how are they stopped?

Answer 1

replicated by muscarine
stopped by low doses of antagonist atropine

after atropine blockade, larger doses of ACh has similar effect like nicotine

Question 2

what are cholinomimetics?

Answer 2

ACh mimicking drugs acting almost exclusive on the PNS with the exception of the sweat glands that have sympathetic innervation

Question 3

what are the main types of muscarinic receptors and where are they located?

Answer 3

M1- CNS, salivary glands, stomach
M2- heart
M3- salivary, sweat glands, bronchial/visceral smooth muscle, eye

Question 4

which muscarinic receptors are stimulatory and inhibitory

Answer 4

M1, M3, (M5) are stimulatory

M2, (M4) are inhibitory

Question 5

what G protein and secondary messengers are involved in the muscarinic receptors>?

Answer 5

M1 and M3 have Gq- [PIP2–> IP3 +DAG]

M2 have Gi- [cAMP]

Question 6

nicotinic receptors

Answer 6

type 1 receptors with ion channel links

• they are faster, ligand gated
• located in muscle and ganglia
• 5 subunits
• ACh has weak effect on them

Question 7

how many and which subunits make up the nicotinic receptors?

Answer 7

alpha, beta, gamma, delta, epsilon
muscle type: 2 alpha, beta, delta, epsilon
ganglion type: 2 alpha, 3 beta

Question 8

what do the subunits determine

Answer 8

the different combinations of the subunits determine the ligand binding properties of the receptor
ACh has a weak effect on the receptors so a lot is required

Question 9

what are the muscarinic cholinergic target sites

Answer 9

the eye
salivary glands 
lungs
bladder
vasculature 
gut 
heart

Question 10

muscarinic effects on the eye(M3)

Answer 10

1) contraction of ciliary muscle for accommodation to near vision
2) contraction of sphincter pupillae- miosis and drainage of intraocular fluid (reduce intraocular pressure)
3) lacrimation- tears

Question 11

role of the sphincter papillae in preventing glaucoma

Answer 11

opens pathway for aqueous humour (produced by ciliary body), allowing its draining through the Canals of Schlemm thus reducing IOP, preventing glaucoma

Question 12

muscarinic effects on the heart (M2)

Answer 12

receptors are located mainly in the atria and the nodes
they have a depressing effect on the heart
mediated by cAMP

Question 13

effect of the reduction of cAMP on the heart

Answer 13

decreased Ca2+ entry –>reduces CO

increased K+ efflux–> decreased HR

Question 14

muscarinic effects on vasculature (M3)

Answer 14

does not have direct PNS innervation

ACh acts on endothelial to release NO via M3 AchR
NO acts on vascular smooth muscles and relaxes it

leads to decreased TPR

Question 15

muscarinic effects on CVS (M2)

Answer 15

decreased HR and CO
vasodilation

drop in BP

Question 16

muscarinic effects in non-vascular smooth muscle

Answer 16

smooth muscles with PNS innervation contract

lungs bronchoconstrict
gut- increased peristalsis
bladder- increased emptying

Question 17

muscarinic effects on exocrine glands

Answer 17

salivation
increased bronchial and GI secretions
increased sweating

Question 18

summary of muscarinic effects

Answer 18

	Decreased HR and BP.
	Increased sweating, salivation and lacrimation. 
	Difficulty breathing.
	Bladder contraction.
	GI pain.

Question 19

directly acting cholinomimetic drugs categories

Answer 19

1) choline esters e.g bethanechol –> bladder emptying

2) alkaloids e.g. pilocarpine–>glaucoma

Question 20

bethanechol

Answer 20

M3 AchR selective agonist
not metabolised readily by ACh esterase
limited access to brain (3-4 hr HL)
orally active

Question 21

bethanechol use and side effects

Answer 21

use: bladder emptying, enhance gastric motility

side effects: blurred vision, sweating, nausea, hypotension, respiratory distress, bradycardia

Question 22

pilocarpine

Answer 22

non-selective agonist
lipid soluble therefore locally administered as eye drops
3-4 hr HL

Question 23

pilocarpine use and side effects

Answer 23

use: treatment of glaucoma

side effects: blurred vision, sweating, GI pain, hypotension, respiratory distress

Question 24

new drug

Answer 24

Cevimeline

M3 selective, more than bethanechol

Question 25

indirectly acting cholinomimetics

Answer 25

they target ACh degrading enzymes i.e. ACh esterase
increase normal PNS stimulation as ACh remains

e. g. ecothiopate (irreversible) used for glaucoma
e. g. physostigmine (reversible) used for atropine poisoning

Question 26

ACh degrading enzymes

Answer 26

1) acetylcholinestrase

2) butyrylcholinesterase

Question 27

acetylcholinesterase

Answer 27

true/specific enzyme found only in synapses
rapid action
highly selective for ACh

Question 28

butyrylcholinesterase

Answer 28

found in plasma and most tissues , not in synapses
broad substrate specificity
leads to the low conc of ACh in the plasma
shows genetic variation

Question 29

effects of cholinesterase inhibitors at different doses

Answer 29

low dose- enhanced muscarinic activity

moderate dose- further enhancement and increased transmission at all ANS ganglia

high dose- becomes toxic having a depolarising block effect on ANS ganglia and NMJ

Question 30

examples of reversible anticholinesterases

Answer 30

physostigmine
neostigmine
donepezil

Question 31

what is the MoA of reversible anticholinesterases?

Answer 31

donate carbamyl group to enzyme active site to block it (competitive)
carbamyl group is hydrolysed slowly (mins) therefore longer acting

Question 32

physostigmine

Answer 32

non selective mAChR agonist:

• acts on postganglionic PNS synapse
• non-polar so it crosses BBB readily
• treat glaucoma
• treat atropine poisoning

Question 33

examples of irreversible anticholinesterases

Answer 33

ecothiopate, dyflos, sarin

these are organosphate compounds

Question 34

irreversible anticholinesterases

Answer 34

rapidly react with enzyme active site leaving a large blocking group
stable and resistant to hydrolysis

Question 35

ecothiopate

Answer 35

potent inhibitor
slow reactive of the enzymes it binds to (several days)
treatment of glaucoma

side effects: sweating, blurred vision, GI pain, bradycardia, hypotension, respiratory difficulty

Question 36

what drugs are used to treat Alzheimers

Answer 36

donepezil and tacrine

Question 37

low dose and high dose effects of physostigmine

Answer 37

low- excitations with possibility of convulsions

high- unconsciousness, respiratory depression, death

Question 38

organophosphate poisoning treatment

Answer 38

IV atropine, artificial respiration, IV pralidoxine (causes unbinding)

caused by nerve gas like sarin that caused a depolarising NMJ block

phosphorylated enzyme ages within a few hours so the patient needs to be kept alive till then

Question 39

what is the difference between acetylcholinesterase and butrylcholinesterases?

Answer 39

Acetylcholinesterase: Is found in all cholinergic synapses in the periphery

Butyrylcholinesterase is not associated with cholinergic synapses but is found in many tissues (e.g. liver, skin) and in plasma.

Question 40

Butyrylcholinesterase selectivity and effect on drug action

Answer 40

broader substrate specificity than AChE and hydrolyses other esters such as suxamethonium

shows genetic variance which influences the duration of action of the drugs it normally metabolises.

Question 41

what is the mechanisms by which ACh is broken down by acetylcholinesterase?

Answer 41

ACh binds to enzyme so enzymes becomes acetylated

the acetylated enzyme breaks down choline

leaves with acetate and free enzyme

Question 42

how do reversible anticholinesterases inhibit the enzyme?

Answer 42

carbamyl esters like physostigmine and neostigmine inactivate the enzyme by transferring their carbamyl group

the carbamylated enzyme is slowly reactivated by hydrolysis

Question 43

how do irreversible anticholinesterases inhibit the enzyme?

Answer 43

organophosphorus compounds like ecothiopate

labile group (fluoride or organic) can inactivate the enzyme by phosphorylation

the inactive enzyme is in a stable state and therefore reactivation can take weeks

its better off synthesising new enzymes