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Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS

Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS & ANTICHOLINESTERASES Part 1: Cholinergics & anticholinesterases. Contents Part 1: Cholinergics & anticholinesterases 1. Nerve Transmission (3 slides) 2. Neurotransmitter

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Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS

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  1. Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS & ANTICHOLINESTERASES Part 1: Cholinergics & anticholinesterases

  2. Contents Part 1: Cholinergics & anticholinesterases 1. Nerve Transmission (3 slides) 2. Neurotransmitter 3. Transmission process (10 slides) 4. Cholinergic receptors (2 slides) 4.1. Nicotinic receptor (2 slides) 4.2. Muscarinic receptor - G Protein coupled receptor (2 slides) 5. Cholinergic agonists 5.1. Acetylcholine as an agonist 5.2. Nicotine and muscarine as cholinergic agonists 5.3. Requirements for cholinergic agonists 6. SAR for acetlcholine (6 slides) 7. Binding site (muscarinic) (3 slides) 8. Active conformation of acetylcholine (2 slides) 9. Instability of acetylcholine 10. Design of cholinergic agonists (7 slides) 11. Uses of cholinergic agonists (2 slides) [46 slides]

  3. CHOLINERGIC NERVOUS SYSTEM

  4. 1. Nerve Transmission Peripheral nervous system CNS Brain Peripheral nerves Muscle Heart Gastro- intestinal tract (GIT) Spinal cord

  5. Skeletal muscle CNS (Somatic) CNS (Autonomic) Synapse Sympathetic Adrenaline Adrenal medulla AUTONOMIC Parasympathetic Smooth muscle Cardiac muscle 1. Nerve Transmission Peripheral nervous system Ach (N) Ach (N) NA Ach (N) Synapse Ach (M) Ach (N)

  6. 100-500A Receptors New signal Nerve impulse Nerve Nerve Vesicles containing neurotransmitters 1. Nerve Transmission Synapses Release of neurotransmitters Receptor binding and new signal

  7. O + C N M e 3 H C O 3 Acetyl Choline 2. Neurotransmitter Acetylcholine (Ach)

  8. . . . . . . Nerve 2 . . . Nerve 1 Signal . Acetylcholinesterase enzyme Acetylcholine Cholinergic receptor Vesicle 3. Transmission process Signal in nerve 1

  9. Nerve 2 Nerve 1 Signal 3. Transmission process Vesicles fuse with membrane and release Ach

  10. Nerve 2 3. Transmission process

  11. 2o Message Nerve 2 3. Transmission process • Receptor binds Ach • Induced fit triggers 2o message • Triggers firing of nerve 2 • Ach undergoes no reaction

  12. Nerve 2 3. Transmission process • Ach departs receptor • Receptor reverts to resting state • Ach binds to acetylcholinesterase

  13. Nerve 2 3. Transmission process Ach hydrolysed by acetylcholinesterase

  14. Choline Nerve 2 Nerve 1 Carrier protein for choline 3. Transmission process Choline binds to carrier protein

  15. Nerve 2 Nerve 1 3. Transmission process Choline transported into nerve

  16. Nerve 2 Nerve 1 E 1 = Choline acetyltransferase 3. Transmission process Ach resynthesised

  17. Nerve 2 Nerve 1 3. Transmission process Ach repackaged in vesicles

  18. Nicotine L-(+)-Muscarine 4. Cholinergic receptors • Receptor types • Not all cholinergic receptors are identical • Two types of cholinergic receptor - nicotinic and muscarinic • Named after natural products showing receptor selectivity Activates cholinergic receptors at nerve synapses and on skeletal muscle Activates cholinergic receptors on smooth muscle and cardiac muscle Acetylcholine is natural messenger for both receptor types

  19. Skeletal Muscle CNS (Somatic) SOMATIC CNS (Autonomic) Synapse Sympathetic Adrenaline Adrenal medulla AUTONOMIC Parasympathetic Smooth Muscle Cardiac Muscle Peripheral nervous system Ach (N) Ach (N) NA Ach (N) Synapse Ach (M) Ach (N)

  20. Binding site Receptor Messenger Cell membrane Cell Induced fit ‘Gating’ (ion channel opens) membrane Five glycoprotein subunits traversing cell membrane 4.1 Nicotinic receptor Control of Cationic Ion Channel:

  21. a g Binding sites a b d Ion channel a b g d a Cell membrane Two ligand binding sites mainly on a-subunits 4.1 Nicotinic receptor The binding sites 2xa, b, g, d subunits

  22. messenger induced fit closed open G-protein bound G-protein split 4.2 Muscarinic receptor - G Protein coupled receptor • Activation of a signal protein • Receptor binds messenger leading to an induced fit • Opens a binding site for a signal protein (G-protein)

  23. Enzyme Enzyme subunit 4.2 Muscarinic receptor - G Protein coupled receptor • Activation of membrane bound enzyme • G-Protein is split and subunit activates a membrane bound enzyme • Subunit binds to an allosteric binding site on enzyme • Induced fit results in opening of an active site • Intracellular reaction is catalysed active site (open) active site (closed) Intracellular reaction

  24. 5. Cholinergic agonists 5.1 Acetylcholine as an agonist • Advantages • Natural messenger • Easily synthesised • Disadvantages • Easily hydrolysed in stomach (acid catalysed hydrolysis) • Easily hydrolysed in blood (esterases) • No selectivity between receptor types • No selectivity between different target organs

  25. 5. Cholinergic agonists 5.2 Nicotine and muscarine as cholinergic agonists • Advantages • More stable than Ach • Selective for main cholinergic receptor types • Selective for different organs • Disadvantages • Activate receptors for other chemical messengers • Side effects

  26. 5. Cholinergic agonists 5.3 Requirements for cholinergic agonists • Stability to stomach acids and esterases • Selectivity for cholinergic receptors • Selectivity between muscarinic and nicotinic receptors • Knowledge of binding site • SAR for acetylcholine

  27. Ethylene bridge Ethylene bridge o Acetoxy 4 Nitrogen Acetoxy Nitrogen Bad for activity 6. SAR for acetlcholine Quaternary nitrogen is essential

  28. Ethylene bridge Ethylene bridge o Acetoxy 4 Nitrogen Acetoxy Nitrogen Bad for activity 6. SAR for acetylcholine • Distance from quaternary nitrogen to ester is important • Ethylene bridge must be retained

  29. Ethylene bridge Ethylene bridge o Acetoxy 4 Nitrogen Acetoxy Nitrogen Bad for activity 6. SAR for acetylcholine Ester is important

  30. Ethylene bridge Ethylene bridge o Acetoxy 4 Nitrogen o Acetoxy 4 Nitrogen Bad for activity Active 6. SAR for acetylcholine Minimum of two methyl groups on quaternary nitrogen

  31. Ethylene bridge Ethylene bridge o Acetoxy 4 Nitrogen Acetoxy Nitrogen Bad for activity 6. SAR for acetylcholine Methyl group of acetoxy group cannot be extended

  32. Ethylene bridge o Acetoxy 4 Nitrogen 6. SAR for acetylcholine • Conclusions: • Tight fit between Ach and binding site • Methyl groups fit into small hydrophobic pockets • Ester interacting by H-bonding • Quaternary nitrogen interacting by ionic bonding

  33. hydrophobic pocket Trp-307 Asp311 hydrophobic pockets Trp-616 Trp-613 hydrophobic pocket Asn-617 7. Binding site (muscarinic)

  34. vdw Trp-307 Asp311 vdw vdw Trp-616 Trp-613 Asn-617 7. Binding site (muscarinic) Ionic bond H-bonds

  35. d + d + d - d - 7. Binding site (muscarinic) • Possible induced dipole dipole interaction between quaternary nitrogen and hydrophobic aromatic rings in binding site • N+ induces dipole in aromatic rings

  36. 8. Active conformation of acetylcholine • Several freely rotatable single bonds • Large number of possible conformations • Active conformation does not necessarily equal the most stable conformation

  37. Muscarinic receptor Nicotinic receptor 8. Active conformation of acetylcholine Rigid Analogues of acetylcholine • Rotatable bonds ‘locked’ within ring • Restricts number of possible conformations • Defines separation of ester and N

  38. 9. Instability of acetylcholine • Neighbouring group participation • Increases electrophilicity of carbonyl group • Increases sensitivity to nucleophiles

  39. 10. Design of cholinergic agonists • Requirements • Correct size • Correct pharmacophore - ester and quaternary nitrogen • Increased stability to acid and esterases • Increased selectivity

  40. 10. Design of cholinergic agonists Use of steric shields • Rationale • Shields protect ester from nucleophiles and enzymes • Shield size is important • Must be large enough to hinder hydrolysis • Must be small enough to fit binding site

  41. hinders binding to esterases and provides a shield to nucleophilic attack asymmetric centre 10. Design of cholinergic agonists Methacholine • Properties • Three times more stable than acetylcholine • Increasing the shield size increases stability but decreases • activity • Selective for muscarinic receptors over nicotinic receptors • S-enantiomer is more active than the R-enantiomer • Stereochemistry matches muscarine • Not used clinically

  42. = 10. Design of cholinergic agonists • Use of electronic factors • Replace ester with urethane • Stabilises the carbonyl group

  43. Carbachol 10. Design of cholinergic agonists • Properties • Resistant to hydrolysis • Long lasting • NH2 and CH3 are equal sizes. Both fit the hydrophobic pocket • NH2 = bio-isostere • Muscarinic activity = nicotinic activity • Used topically for glaucoma

  44. Bethanechol 10. Design of cholinergic agonists Steric + Electronic factors • Properties • Very stable • Orally active • Selective for the muscarinic receptor • Used to stimulate GI tract and urinary bladder after surgery

  45. 10. Design of cholinergic agonists Nicotinic selective agonist

  46. 11. Uses of cholinergic agonists • Nicotinic selective agonists • Treatment of myasthenia gravis • - lack of acetylcholine at skeletal muscle causing weakness • Muscarinic selective agonists • Treatment of glaucoma • Switching on GIT and urinary tract after surgery • Treatment of certain heart defects. Decreases heart muscle activity and decreases heart rate

  47. Skeletal Muscle CNS (Somatic) SOMATIC CNS (Autonomic) Synapse Sympathetic Adrenaline Adrenal medulla AUTONOMIC Parasympathetic Smooth Muscle Cardiac Muscle Peripheral nervous system Ach (N) Ach (N) NA Ach (N) Synapse Ach (M) Ach (N)

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