Cholinergic Agents
Alkaloids Nicotine Lobeline Arecoline Muscarine Pilocarpine Synthetic Agents Dimethylphenylpiperazinium- (DMPP) Oxotremorine Methacholine Bethanechol Carbachol Cevimeline
Nicotine Nicotine mimics the actions of acetylcholine at nicotinic sites –Cell body of the postsynaptic neurons sympathetic and parasympathetic divisions –Chromaffin cells of the adrenal medulla –End plate of skeletal muscle fiber Affinity for N N sites versus N M sites Used as an insecticide
Muscarine Muscarine mimics the actions of acetylcholine at smooth muscles, cardiac muscles, and glands Poisoning by muscarine produces intense effects qualitative to those produced by cholinergic stimulation of smooth muscles, cardiac muscle, and glands Muscarine is found in various mushrooms –Amanita muscaria: content of muscarine is very low –Inocybe sp: content of muscarine is high –Clitocybe sp: content of muscarine is high
Pilocarpine Has muscarinic actions Used for xerostomia Used for glaucoma
Structure of Acetylcholine and its Derivatives AcetylcholineMethacholine BethanecholCarbachol
Therapeutic Uses of Cholinergic Agonists Dentistry –Pilocarpine –Cevimeline Ophthalmology –Pilocarpine –Carbachol Gastrointestinal tract –Bethanechol Urinary bladder –Bethanechol
Contraindications to the Use of Choline Esters Hyperthyroidism Asthma Coronary insufficiency Peptic ulcer Organic obstruction in bladder or gastrointestinal tract
Toxicity of Choline Esters Flushing SWEATING (diaphoresis) Abdominal cramps Spasm of the urinary bladder Spasm of accomodation Miosis Headache Salivation Bronchospasm Lacrimation Hypotension Bradycardia
Agents That Inhibit Acetylcholinesterase
Acetylcholinesterase (True Cholinesterase)
Acetylcholinesterase (1) Sites of location –Cholinergic neurons –Cholinergic synapses –Neuromuscular junction –Red blood cells Substrates –Acetylcholine is the best substrate –Methacholine is a substrate –Hydrolyzes ACh at greater velocity than choline esters with acyl groups larger than acetate or proprionate
Acetylcholinesterase (2) Esters that are not substrates –Bethanechol –Carbachol –Succinylcholine Its inhibition produces synergistic interaction with methacholine and additive actions with bethanechol and carbachol Drugs that block its hydrolysis of esters are called cholinesterase inhibitors
Drug Interactions of Choline Esters and Inhibitors of Acetylcholinesterase - Synergism versus Additivity Methacholine Carbachol Bethanechol
Butyrylcholinesterase (Plasma esterase, pseudocholinesterase, serum esterase, BuChE, PseudoChE)
Butyrylcholinesterase (1) Sites of location –Plasma, liver, glial cells, other tissues Substrates –Butyrylcholine is the best –Acetylcholine –Succinylcholine –Procaine
Butyrylcholinesterase (2) Esters that are not substrates –Methacholine, bethanechol, and carbachol Is inhibited by carbamyl and organophosphate inhibitors of acetylcholinesterase
Active Site of Acetylcholinesterase
Interaction of AChE and Acetylcholine
Acetylation of AChE and Release of Choline
Hydroxyl Group of Water Attacks the Carbonyl Group of Acetylated-AChE to Liberate AChE
Carbamyl Inhibitors of AChE
Their action promoting accumulation of ACh at muscarinic or nicotinic receptors is the basis of their pharmacological, therapeutic, and toxic actions Are derivatives of carbamic acid Bind covalently to the esteratic site of AChE, resulting in carbamylation of the enzyme Carbamyl Inhibitors of AChE (1) Carbamic acidCarbamic acid ester
Quaternary compounds bind to the ionic binding site of AChE Their induce accumulation of AChE at nicotinic and muscarinic sites, producing pharmacological responses qualitative to cholinergic stimulation Inhibition of AChE is reversible, in the order of hours Are metabolized in the plasma by plasma esterases Carbamyl Inhibitors of AChE (2)
High doses produce skeletal muscle weakness due to depolarizing blockade at the end plate of the neuromuscular junction High doses produce a profound fall in cardiac output and blood pressure Their inhibition of AChE is not reversed by pralidoxime Carbamyl Inhibitors of AChE (3)
Quaternary ammonium compounds do not cross the blood-brain barrier For oral administration, high doses must be given Carbamyl Inhibitors of AChE (4)
Neostigmine Carbamylates Acetylcholinesterase
Slow Hydrolysis of Carbamylated-AChE and Enzyme Liberation
Organophosphate Inhibitors of Acetylcholinesterase
Chemical characteristics Promote accumulation of ACh at –N M nicotinic receptor –N N nicotinic receptor –Muscarinic receptor Organophosphate Inhibitors of Acetylcholinesterase (1)
Their action promoting accumulation of ACh at the muscarinic receptor of the ciliary muscle is the basis of their therapeutic effectiveness in open angle glaucoma Only two of these agents are used for therapeutics –Echothiophate for glaucoma –Diisopropylflurophosphate (DFP) for glaucoma (?) Organophosphate Inhibitors of AChE (2)
Inhibition of AChE by these agents is irreversible –New enzyme synthesis is required for recovery of enzyme function They also inhibit pseudocholinesterase Metabolized by A-esterases (paroxonases) present in plasma and microsomes. They are metabolized by CYP450. Organophosphate Inhibitors of AChE (3)
Enzyme inhibition by these agents can be reversed by cholinesterase reactivators such as pralidoxime if administered before “aging” of AChE has occurred. Inhibition by agents that undergo rapid “aging” is not reversed. Except for echothiophate, these agents are extremely lipid soluble, and some are very volatile. Organophosphate Inhibitors of AChE (4)
Diisopropylflurophosphate (DFP) is a Substrate for AChE
The Extremely Slow Hydrolysis of Phosphorylated-AChE New enzyme synthesis is required for recovery of enzyme function
Various “States” of Acetylcholinesterase Clockwise: free AChE, acetylated AChE, carbamylated AChE, phosphorylated AChE
Acetylated-AChE Is Very Rapdily Hydrolyzed AChE + Acetylcholine AChE-acetylated + choline AChE-acetylated + H 2 O AChE + acetate Hydrolysis of AChE-acetylated is rapid, in the order of microseconds P
Carbamylated-AChE Is Hydrolyzed Slowly AChE + Carbamyl inhibitor AChE-carbamylated + noncarbamylated metabolite AChE-carbamylated + H 2 O AChE + carbamic acid derivative Hydrolysis of the AChE-carbamylated is slow, in the order of hours. The carbamylated enzyme is reversibly inhibited, and recovery of function is in the order of hours Enzyme after phosphorylation by neostigmine
Phosphorlylated-AChE Is Hydrolyzed Extremely Slowly AChE + organophosphate inhibitor AChE-phosphorylated + nonphosphorylated metabolite AChE-phosphorylated + H 2 O AChE + phosphorylated derivative Hydrolysis of the AChE-phosphorylated is extremely slow, in the order of days. The phosphorylated enzyme is considered to be irreversibly inhibited, and recovery of function is in the order of days. Pralidoxime, a reactivating agent, may be adminstered to a subject before the enzyme has “aged.” Enzyme after phosphorylation by DFP
AGING OF ACETYLCHOLINESTERASE
Loss of An Alkyl Group From Phosphorylated AChE “Ages” the Enzyme AChE, phosphorylated and inhibited by DFP “Aged” AChE
“Aging” of Phosphorylated- AChE
Cholinesterase Reactivation
Reactivation of Phosphorylated Acetylcholinesterase Oximes are used to reactivate phosphorylated AChE The group (=NOH) has a high affinity for the phosphorus atom Pralidoxime has a nucleophilic site that interacts with the phosphorylated site on phosphorylated-AChE
Pralidoxime Reacts Chemically with Phosphorylated-AChE The oxime group makes a nucleophilic attack upon the phosphorus atom
Oxime Phosphonate and Regenerated AChE
Limitations of Pralidoxime Pralidoxime does not interact with carbamylated-AChE Pralidoxime in high doses can inhibit AChE Its quaternary ammonium group does not allow it to cross the blood brain barrier “Aging” of phosphorylated-AChE reduces the effectiveness of pralidoxime and other oxime reactivators
Other Cholinesterase Reactivators Diacetylmonoxime –Crosses the blood brain barrier and in experimental animals, regenerates some of the CNS cholinesterase HI-6 is used in Europe –Has two oxime centers in its structure –More potent than pralidoxime
Edrophonium
Edrophonium is a Short Acting Inhibitor that Binds to the Ionic Site but Not to the Esteratic Site of AChE
Pharmacology of Acetylcholinesterase Inhibition
Inhibition of Acetylcholinesterase Produces Stimulation of All Cholinergic Sites
Carbamyl Inhibitors of AChE Physostigmine Neostigmine (N + ) Pyridostigmine (N + ) Ambenonium (N + ) Demecarium (N + ) Carbaryl
Pharmacology of Carbamyl Inhibitors of Acetylcholinesterase Eye Exocrine glands Cardiac muscle Smooth muscles Skeletal muscle Toxicity
Therapeutic Uses of Inhibitors of Acetylcholinesterase Glaucoma (wide angle) Atony of the bladder Atony of the gastrointestinal tract Intoxication by antimuscarinic agents (use physostigmine) Intoxication by tricyclic antidepressants (TCA’s) or phenothiazines (use physostigmine) Recovery of neuromuscular function after competitive blockade of N N receptor of skeletal muscle fibers Myasthenia gravis
Therapeutic Uses of Edrophonium Diagnosis of myasthenia gravis In conjunction with chosen therapeutic agent to determine proper dose of agent
Determining Proper Dose of AChE Inhibitor
Inhibitors of AChE Are Used for Therapy of Alzheimer’s Disease Tacrine Donepezil Rivastigmine Galantamine
Organophosphate Inhibitors of AChE
Some Organophosphate Inhibitors of Acetylcholinesterase Tetraethylpyrophosphate Echothiophate (N + ) Diisopropylflurophosphate (DFP) Sarin Soman Tabun Malathion Parathion Diazinon Chlorpyrifos Many others
Organophosphate Inhibitors - 2 Diisopropylfluorophosphate (DFP) Soman Sarin Tabun
Echothiophate Therapeutic use - local application to the eye for wide angle glaucoma
Conversion of Parathion to Paraoxon
Conversion of Malathion to Malaoxon
Malathion Is Hydrolyzed by Plasma Carboxylases in Birds and Mammals but Not Insects
Carboxyl Esterases Preferentially hydrolyzes aliphatic esters Malathion is a substrate Are inhibited by organophosphates May also be called aliesterases
Uses of Malathion Insecticide Therapeutics –Used as a lotion for Pediculus humanus capitis associated with pediculosis –0.5% solution in 78% isopropranolol is pediculicidal and ovicidal –Ovide is the brand name –Primoderm was the former brand name
Malathion Metabolism Rapidly metabolized by birds and mammals Plasma carboxylases are involved Insects do not possess the enzyme Organophosphates inhibit malathion metabolism Malathion is toxic to fish
Aryl Esterases Are found in the plasma and liver Hydrolyzes organophosphates at the – P-F bond – P-CN bond – Phosphoester bond – Anhydride bond
EPA And Organophosphates Diazinon –No longer allowed to be manufactured for indoor use in as of March 1, 2001 or for garden use as of June 3, 2001 –Found in Real Kill ®, Ortho ®, Spectracide ® –Limited agricultural use is allowed Chlorpyrifos (Dursban) has been phased out Parathion has been phased out for agricultural use in the United States
NERVE AGENT VX Chemical name: O-ETHYL-S-(2-DIISOPROPYLAMINOMETHYL)METHYL- PHOSHONOTHIOLATE Trade name: PHOSPHONOTHIOIC ACID
NERVE AGENT VX Chemical name: O-ETHYL-S-(2-DIISOPROPYLAMINOMETHYL)METHYL- PHOSHONOTHIOLATE Trade name: PHOSPHONOTHIOIC ACID
Organophosphates as Nerve Gas Agents in Chemical Warfare (1) Extremely volatile agents such as sarin, tabun, soman, and agent VX may be used as nerve agents in chemical warfare. Accumulation of ACh at cholinergic receptors produces effects reflecting stimulation of cardiac muscle, smooth muscles and glands. Such effects would be identical to those caused by muscarine poisoning. Bradycardia and hypotension occur. However, in some cases, tachycardia may be observed, due to intense sympathetic discharge in response severe hypoxemia.
Organophosphates as Nerve Gas Agents in Chemical Warfare (2) Irreversible inhibition of acetylcholinesterase by these agents produces accumulation of ACh at the end plate of skeletal muscle fibers. This in turn leads to depolarizing blockade of the N M nicotinic receptor. Skeletal muscle paralysis occurs. Movement is impossible. The diaphragm is also paralyzed. The individual eventually dies due to respiratory paralysis. Pralidoxime, atropine, and removal of the person from the source of exposure are all to be employed in cases of posioning.
Use of Pyridostigmine During the Gulf War