Autonomic nervous system II. - PowerPoint PPT Presentation

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Autonomic nervous system II.

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Effect similar to stimulation of cholinergic nervous system ... GIT muscles atonia. miosis and decreases intraocular pressure. CI - obstruction GIT ... – PowerPoint PPT presentation

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Title: Autonomic nervous system II.


1
Autonomic nervous system II.
  • MUDr. Martin Votava

2
Main functions
  • contraction and relaxation of smooth muscles
  • function of all exocrine and some endocrine
    glands
  • heart beat
  • some metabolic pathways

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Homotropic and heterotropic inhibition
6
AUTONOMIC NERVOUS SYSTEM II.
  • Parasympatomimetics
  • Parasympatolytics

7
  • Parasympatomimetics
  • Parasympatolytics
  • Drugs affecting autonomic ganglia

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10
Cholinomimetics
  • Effect similar to stimulation of cholinergic
    nervous system
  • Act on muscarinic (M) a nicotinic (N) receptors

11
M1, M3, M5 receptors
muscarinic receptor
12
M2, M4 receptors
muscarinic receptor
13
Muscarinic and nicotinic (cholinergic) receptors
14
Stimulation of muscarinic receptor
15
Nicotinic effects
  • Ganglial receptors
  • Depends on autonomic stimulation. When
    sympathetic nervous system outweighs (vessels),
    then their stimulation stimulates sympathetic
    neurons.
  • When parasympathetic system outweighs (heart,
    GIT), then their stimulation stimulates
    parasympathetic neurons.
  • Adrenal medula - adrenalin and noradrenalin
    release
  • Neuromuscular junction - spasms and convulsions
    of skeletal muscles

16
Cholinomimetics
  • 1. direct
  • M receptor agonists
  • N receptor agonists
  • (most of them are nonspecific)
  • 2. indirect (AChE inhibitors)
  • short acting-edrofonium
  • intermediate acting - carbamates
  • long acting (irreversible blockers) -
    organophosphates

17
Direct cholinomimetics
  • Acetylcholine - direct endogenous
    cholinomimetics, which is released in
  • sympathetic and parasympathetic ganglias
    (N-effects)
  • postganglial parasympathetic neurons (M-effects)
  • neuromuscular junction (N-effects)
  • adrenal medula (N-effect, adrenaline secretion)
  • CNS (N-effect)
  • Very fast hydrolysis by acetylcholinesterase.

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Acetylcholine
  • poor absorption p.o. and s.c., does not cross HEB
  • rapid hydrolysis by AChE
  • BP decrease, bradycardia, heart arrest
  • sweating, salivation, lacrimation, glands
    secretion
  • nauzea, cough, dyspnoe
  • vessels dilatation EDRF (NO) release
  • effect

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Pilocarpine
  • tercial N atom - increased lipofility, cross HE
    barrier and enters cornea
  • M and N effect
  • miosis and decreases intraocular pressure

22
Carbachol
  • quartery N atom, does not cross HEB, resistance
    to AChE
  • secretion GIT glands
  • GIT muscles atonia
  • miosis and decreases intraocular pressure
  • CI - obstruction GIT

23
Metacholine, betanechol
  • quartery N atom, does not cross HEB, resistance
    to AChE
  • GIT motility increasing, urinary retention after
    anesthesia or vagotomia
  • examination of exocrine pancreas secretion
  • CI - obstruction GIT

24
Intoxication
  • M receptors CNS stimulation, miosis,
    accommodation, dyspnoe, (bronchoconstriction,
    hypersecretion of bronchial glands), diarrhoea
    (hypermotility and hypersecretion), hypotension
    (vazodilatation), bradycardia.
  • N receptors convulsions, BP increase (adrenal
    and ganglia N receptor stimulation).

25
Indication
  • postoperative and neurogenic ileus, urinary
    retention.
  • glaucoma (carbachol, pilokarpine).

26
Reversible (competitive) AChE inhibitors
27
Indications
  • Postoperative and neurogenic ileus, urinary
    retention neostigmine
  • Glaucoma- physostigmine
  • Myastenia gravis neostigmine, pyridostigmine,
    edrophonium
  • Treatment of neuromuscular blocks
  • Alzheimer disease
  • rivastigmine, donezepil

28
Ireversible AChE inhibitors - organphosphates
  • M and N effect
  • AChE activity 70 - mild intoxication
  • AChE activity ? 30 - severe intoxication

29
Toxicology importance
  • agriculture - herbicids and pesticids
  • chemical weapons tabun, sarin, soman (cross skin
    and mucos membranes)
  • Intoxication - nausea, vomitus, cephalea,
    weakness, sweating, salivation, bradycardia,
    dyspnoe, breathing arrest
  • Pharmacotherapy
  • Very rare glaucoma echothiophtate
  • scabies malathione

30
Therapy of intoxication
  • avoid absorption
  • atropine - blocks muscarinic effects
  • ventilation
  • AChE reactivators- pralidoxime
  • short acting AChE inhibitors - save AChE, which
    is not affected by poison

31
Parasympatolytics
  • tercial amonium basis (tercial amonium atom)
  • natural alkaloids. Atropin (Atropa belladonna) or
    (Datura stramonium) and scopolamine (Hyosciamus
    niger).
  • synthetic analogs - esterification of natural
    basis with organic acids
  • Quartery amonium basis (quartery amonium atom)

32
Pharmacokinetics
  • absorption
  • tercial basis - good GIT and corneal absorption
  • Quartery basis - GIT absorption only 10-30
  • distribution
  • tercial basis - very wide distribution (HEB)
    after 1 hour - many CNS side effects
  • Quartery basis - dont cross HEB

33
Atropine - competitive reversible inhibitor
34
CNS effects
  • Antiemetic properties (scopolamine) - kinetosis,
    vestibular apparatus disorders
  • tremor attenuation in Parkinson disease
    (Acetylcholine increased release)
  • n. vagus center stimulation - bradycardia (after
    low doses of atropine), after high doses direct
    antimuscarinic effect - tachycardia

35
Eye effect
  • m. sphincter pupillae - inhibition of m.
    sfincter pupillae, m. dilatator pupillae indirect
    activation - mydriasis
  • m. ciliaris paralysis - cycloplegia.
    accommodation attenuation
  • cave - acute glaucoma attack
  • lacrimation decrease

36
GIT effect
  • Attenuation of GIT motility (M receptors), then
    gland secretion
  • Relaxation of GIT smooth muscles
  • Contraction of sphincters, GIT paralyis
  • Stomach secretion is attenuated after relatively
    high doses of parasympatolytics

37
Termoregulation
  • atropine attenuated sweating, one of the most
    important termoregulatory mechanism. It causes
    body temperature increase, but only after high
    doses. Children can have atropine fewer after
    lower doses of artropine

38
Indications I.
  • Parkinson disease, symptomatic therapy, (first
    line therapy are dopaminergic drugs)
  • Kinetosis - scopolamine, transcutal form, (24-48
    h.), side effects
  • Bradycardia
  • Eyes
  • mydriasis for diagnostic examination
  • synechia prevention when inflammation is present
    (uveitis, iritis)

39
Indications II.
  • Gastrointestinal disorders (Quartery bases)
  • peptic ulcer disease. (Antimuscarinic effect to
    the parietal cells - pirenzepine, poldine)
  • spasmolytics - GIT - urolithiasis, cholelythiasis
  • diarrhoea with cramps (combination with opiates)
    (e.g. atropine with diphenoxylate REASEC)
  • bronchodilatation and inhibition of secretion
  • asthma bronchiale therapy ipratropium
    (ATROVENT), or combination with fenoterole
    (BERODUAL)
  • sweating

40
Indications III.
  • therapy of AChE irreversible inhibitors poisoning
    (organophaosphates). Atropinsulphate in high
    doses(1-2 mg) i.v. after 5-15 min. until atropine
    side effect are present (dry mouth, miosis)
  • Mushroom poisoning
  • Amanita muscarina - after 30 - 60 minutes -
    nausea, vomitus, diarrhoea, tachycardia,
    sweating, salivation, bronchoconstriction -
    atropine (1-2 mg parenteral)

41
Side effects
  • peripheral - dry skin, tachycardia, mydriasis,
    cycloplegia
  • Stimulation, CNS excitation (hallucinations,
    delirium, convulsions, coma)
  • Warm and red, dry skin, increased body
    temperature
  • Quartery bases - mostly antimuscarinic affects,
    minimal central effects
  • Antinicotinic effects - hypotension
  • Therapy - neostigmine, sympatomimetics
    (fenylefrine)

42
Contraindications
  • glaucoma, (closed angle)
  • prosthatic hypertrophy

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44
Drugs affecting autonomic ganglia
  • Ganglion stimulants
  • (acetylcholine)
  • Nicotine (drug of abuse)
  • Lobeline (found in tabacco leaves as well)
  • Dimethylphenylpiperazinium (DMPP)
  • Tetramethylamonium
  • Used as experimental tools

45
Ganglion-blocking drugs
  • Interference with acetylcholine release
  • Botulinum toxin, hemicholinium
  • Prolonged depolarization
  • Nicotine
  • Competitive antagonist
  • Hexamethonium, tetraethylamonium
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