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By: Dr.S.Kameshwaran
Sedative & Hypnotics
Sedative:
A drug that subdues excitement and calms the subject without
inducing sleep, though drowsiness may be produced.
Sedation refers to decreased responsiveness to any level of
stimulation; is associated with some decrease in motor activity and
ideation.
Hypnotics:
A drug that induces and/or maintains sleep, similar to normal
arousable sleep.
• A hypnotic at lower dose may act as sedative.
• Sedation—hypnosis—general anaesthesia may be regarded as
increasing grades of CNS depression.
• Hypnotics given in high doses can produce general anaesthesia.
SLEEP
Sleep
• The duration and pattern of sleep varies considerably among individuals.
• Age has an important effect on quantity and depth of sleep.
• The different phases of sleep and their characteristics
Stage 0 (Awake)
• From lying down to falling asleep and occasional nocturnal awakenings;
• constitutes 1–2% of sleep time.
• Eye movements are irregular or slowly rolling.
Stage 1 (Dozing)
• Eye movements are reduced but there may be rolling.
• Neck muscles relax. Occupies 3–6% of sleep time.
Stage 2 (Unequivocal sleep)
• Little eye movement;
• Subjects are easily arousable.
• This comprises 40–50% of sleep time.
Stage 3 (deep sleep transition)
• Eye movements are few;
• subjects are not easily arousable;
• comprises 5–8% of sleep time.
Stage 4 (cerebral sleep)
• Eyes are practically fixed;
• Subjects are difficult to arouse.
• It comprises 10–20% of sleep time.
• During stage 2, 3 and 4 heart rate, BP and respiration are steady and muscles are
relaxed.
• Stages 3 and 4 together are called slow wave sleep (SWS).
REM sleep (paradoxical sleep)
• There are marked, irregular eye movements;
• Dreams and nightmares (disturbing dream associated with negative
feelings, such as anxiety or fear that awakens) occur, Which may be
recalled if the subject is aroused.
• Heart rate and BP fluctuate; respiration is irregular.
• Muscles are fully relaxed, but irregular body movements occur
occasionally.
• Erection occurs in males.
• About 20–30% of sleep time is spent in REM.
Normally stages 0 to 4 and REM occur in succession over a period
of 80–100 min.
Then stages 1–4–REM are repeated cyclically.
CLASSIFICATION
Barbiturates
• Long acting : Phenobarbitone
• Short acting: Butobarbitone, Pentobarbitone
• Ultra-short acting: Thiopentone Methohexitone
Benzodiazepines
• Hypnotic: Diazepam, Flurazepam, Nitrazepam, Alprazolam, Temazepam
• Antianxiety: Diazepam, Chlordiazepoxide, Oxazepam, Lorazepam, Alprazolam
• Anticonvulsant: Diazepam, Lorazepam, Clonazepam Clobazam, Triazolam
Newer non benzodiazepine hypnotics
• Zopiclone Zolpidem Zaleplon
BARBITURATES:
• Barbiturates have been popular hypnotics and sedatives of the last
century upto 1960s,
• But are not used now to promote sleep or to calm patients.
PHARMACOLOGICAL ACTIONS
• Barbiturates are general depressants for all excitable cells, the
CNS is most sensitive
CNS
• Barbiturates produce dose-dependent effects:
• Sedation → sleep → anaesthesia → coma.
• Hypnotic dose shortens the time taken to fall asleep and increases
sleep duration.
• The sleep is arousable, but the subject may feel confused and
unsteady if waken early. Night awakenings are reduced.
• Hangover (dizziness, distortions of mood, irritability and lethargy) may occur in
the morning after a nightly dose.
• Barbiturates can impair learning, shortterm memory and judgement.
MECHANISM OF ACTION
BARBITURATES
↓
BINDS TO ITS RECEPTOR PRESENT IN THE ΑLPHA SUB UNIT OF GABA-A
RECEPTOR
↓
IT INCREASE THE BINDING OF GABA TO THE GABA-A RECEPTOR
↓
INCREASES THE INFLUX OF MORE Cl- IONS IN TO INTRACELLULAR SITE
↓
HYPERPOLARIZATION
↓
SEDATION/HYPNOSIS
PHARMACOKINETICS
• Barbiturates are well absorbed from the g.i. tract.
• They are widely distributed in the body.
• The rate of entry into CNS is dependent on lipid solubility.
• Highly-lipid soluble thiopentone enters instantaneously,
• less lipid-soluble pentobarbitone take longer;
• Plasma protein binding thiopentone 75%, phenobarbitone
20%.
• Barbiturates cross placenta and are secreted in milk
• Metabolized in liver by oxidation, dealkylation and
conjugation.
• Significantly excreted unchanged in urine.
ADR:
• Hangover
• Tolerance and dependence.
• Mental confusion,
• Impaired performance
• Traffic accidents may occur
USES:
• Except - phenobarbitone in epilepsy and thiopentone in
anaesthesia no other barbiturate is used now.
• As hypnotic and anxiolytic they have been superseded by
BZDs.
• They are occasionally employed as adjuvants in
psychosomatic disorders.
BENZODIAZEPINES (BZDs)
• Chlordiazepoxide and diazepam were introduced around 1960 as
antianxiety drugs.
• Since then this class has proliferated and has replaced barbiturates
• BZDs produce a lower degree of neuronal depression than
barbiturates.
• They have a high therapeutic index.
• Ingestion of even 20 hypnotic doses does not usually endanger
life—there is no loss of consciousness (though amnesia occurs) and
patient can be aroused; respiration is mostly not so depressed as to
need assistance.
• Hypnotic doses do not affect respiration or cardiovascular
functions.
• They have lower abuse liability: tolerance is mild, psychological
and physical dependence, drug seeking and withdrawal
syndrome are less marked.
• A specific BZD antagonist flumazenil is available which can be used
in case of poisoning.
• In contrast to barbiturates, bZDs are not general
depressants,
• exert relatively selective anxiolytic, hypnotic, muscle
relaxant and anticonvulsant effects
• Time spent in stage 2 is increased while that in stage 3
and 4 is decreased.
• BZDs produce centrally mediated skeletal muscle
relaxation without impairing voluntary activity
• Clonazepam, diazepam, nitrazepam, lorazepam and
flurazepam have more prominent anticonvulsant activity
MECHANISM OF ACTION:
BENZODIAZEPINES
↓
BINDS TO BZD RECEPTOR PRESENT IN THE ΑLPHA SUB UNIT OF GABA-A
RECEPTOR
↓
IT INCREASE THE BINDING OF GABA TO THE GABA-A RECEPTOR
↓
INCREASES THE INFLUX OF MORE Cl- IONS IN TO INTRACELLULAR SITE
↓
HYPERPOLARIZATION
↓
SEDATION/HYPNOSIS
PHARMACOKINETICS
• Absorbed orally
• Plasma protein binding also varies markedly (flurazepam 10% to
diazepam 99%).
• BZDs are widely distributed in the body.
• Benzodiazepines are metabolized in liver mainly by CYP3A4 and
CYP2C19
• Some BZDs (e.g. diazepam) undergo enterohepatic circulation.
• BZDs and their phase I metabolites are excreted in urine as
glucuronide conjugates.
• BZDs cross placenta and are secreted in milk.
ADR:
• Benzodiazepines are relatively safe drugs. Side effects of hypnotic doses
are
• dizziness,
• vertigo,
• ataxia,
• disorientation,
• amnesia,
• prolongation of reaction time—impairment of psychomotor skills
(should not drive).
Uses:
• As hypnotic
• As anxiolytic
• As anticonvulsant,
• As centrally acting muscle relaxant
• In preanaesthetic medication,
• In Alcohol withdrawal
NON-BENZODIAZEPINE HYPNOTICS
• This lately developed group of hypnotics are chemically different from
BZDs,
• Act as agonists on a specific subset of BZD receptors.
• They have lower abuse potential than hypnotic BZDs.
Zopiclone
• This is the first of the non-BZD hypnotics,
• Which acts as an agonist at a subtype of BZD receptor involved in the
hypnotic action.
• The effect on sleep resemble those of BZDs, but it does not alter REM
sleep and tends to prolong stages 3 and 4.
• It is reported not to disturb sleep architecture, but some degree of next
morning impairment can occur.
THANK
YOU

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Sedatives & Hypnotics B.Pharm & Pharm.D - CNS

  • 2. Sedative & Hypnotics Sedative: A drug that subdues excitement and calms the subject without inducing sleep, though drowsiness may be produced. Sedation refers to decreased responsiveness to any level of stimulation; is associated with some decrease in motor activity and ideation.
  • 3. Hypnotics: A drug that induces and/or maintains sleep, similar to normal arousable sleep. • A hypnotic at lower dose may act as sedative. • Sedation—hypnosis—general anaesthesia may be regarded as increasing grades of CNS depression. • Hypnotics given in high doses can produce general anaesthesia.
  • 5. Sleep • The duration and pattern of sleep varies considerably among individuals. • Age has an important effect on quantity and depth of sleep. • The different phases of sleep and their characteristics Stage 0 (Awake) • From lying down to falling asleep and occasional nocturnal awakenings; • constitutes 1–2% of sleep time. • Eye movements are irregular or slowly rolling. Stage 1 (Dozing) • Eye movements are reduced but there may be rolling. • Neck muscles relax. Occupies 3–6% of sleep time. Stage 2 (Unequivocal sleep) • Little eye movement; • Subjects are easily arousable. • This comprises 40–50% of sleep time.
  • 6. Stage 3 (deep sleep transition) • Eye movements are few; • subjects are not easily arousable; • comprises 5–8% of sleep time. Stage 4 (cerebral sleep) • Eyes are practically fixed; • Subjects are difficult to arouse. • It comprises 10–20% of sleep time. • During stage 2, 3 and 4 heart rate, BP and respiration are steady and muscles are relaxed. • Stages 3 and 4 together are called slow wave sleep (SWS).
  • 7. REM sleep (paradoxical sleep) • There are marked, irregular eye movements; • Dreams and nightmares (disturbing dream associated with negative feelings, such as anxiety or fear that awakens) occur, Which may be recalled if the subject is aroused. • Heart rate and BP fluctuate; respiration is irregular. • Muscles are fully relaxed, but irregular body movements occur occasionally. • Erection occurs in males. • About 20–30% of sleep time is spent in REM. Normally stages 0 to 4 and REM occur in succession over a period of 80–100 min. Then stages 1–4–REM are repeated cyclically.
  • 8.
  • 9. CLASSIFICATION Barbiturates • Long acting : Phenobarbitone • Short acting: Butobarbitone, Pentobarbitone • Ultra-short acting: Thiopentone Methohexitone Benzodiazepines • Hypnotic: Diazepam, Flurazepam, Nitrazepam, Alprazolam, Temazepam • Antianxiety: Diazepam, Chlordiazepoxide, Oxazepam, Lorazepam, Alprazolam • Anticonvulsant: Diazepam, Lorazepam, Clonazepam Clobazam, Triazolam Newer non benzodiazepine hypnotics • Zopiclone Zolpidem Zaleplon
  • 10. BARBITURATES: • Barbiturates have been popular hypnotics and sedatives of the last century upto 1960s, • But are not used now to promote sleep or to calm patients. PHARMACOLOGICAL ACTIONS • Barbiturates are general depressants for all excitable cells, the CNS is most sensitive CNS • Barbiturates produce dose-dependent effects: • Sedation → sleep → anaesthesia → coma. • Hypnotic dose shortens the time taken to fall asleep and increases sleep duration. • The sleep is arousable, but the subject may feel confused and unsteady if waken early. Night awakenings are reduced.
  • 11. • Hangover (dizziness, distortions of mood, irritability and lethargy) may occur in the morning after a nightly dose. • Barbiturates can impair learning, shortterm memory and judgement. MECHANISM OF ACTION BARBITURATES ↓ BINDS TO ITS RECEPTOR PRESENT IN THE ΑLPHA SUB UNIT OF GABA-A RECEPTOR ↓ IT INCREASE THE BINDING OF GABA TO THE GABA-A RECEPTOR ↓ INCREASES THE INFLUX OF MORE Cl- IONS IN TO INTRACELLULAR SITE ↓ HYPERPOLARIZATION ↓ SEDATION/HYPNOSIS
  • 12.
  • 13. PHARMACOKINETICS • Barbiturates are well absorbed from the g.i. tract. • They are widely distributed in the body. • The rate of entry into CNS is dependent on lipid solubility. • Highly-lipid soluble thiopentone enters instantaneously, • less lipid-soluble pentobarbitone take longer; • Plasma protein binding thiopentone 75%, phenobarbitone 20%. • Barbiturates cross placenta and are secreted in milk • Metabolized in liver by oxidation, dealkylation and conjugation. • Significantly excreted unchanged in urine.
  • 14. ADR: • Hangover • Tolerance and dependence. • Mental confusion, • Impaired performance • Traffic accidents may occur USES: • Except - phenobarbitone in epilepsy and thiopentone in anaesthesia no other barbiturate is used now. • As hypnotic and anxiolytic they have been superseded by BZDs. • They are occasionally employed as adjuvants in psychosomatic disorders.
  • 15. BENZODIAZEPINES (BZDs) • Chlordiazepoxide and diazepam were introduced around 1960 as antianxiety drugs. • Since then this class has proliferated and has replaced barbiturates • BZDs produce a lower degree of neuronal depression than barbiturates. • They have a high therapeutic index. • Ingestion of even 20 hypnotic doses does not usually endanger life—there is no loss of consciousness (though amnesia occurs) and patient can be aroused; respiration is mostly not so depressed as to need assistance. • Hypnotic doses do not affect respiration or cardiovascular functions. • They have lower abuse liability: tolerance is mild, psychological and physical dependence, drug seeking and withdrawal syndrome are less marked. • A specific BZD antagonist flumazenil is available which can be used in case of poisoning.
  • 16. • In contrast to barbiturates, bZDs are not general depressants, • exert relatively selective anxiolytic, hypnotic, muscle relaxant and anticonvulsant effects • Time spent in stage 2 is increased while that in stage 3 and 4 is decreased. • BZDs produce centrally mediated skeletal muscle relaxation without impairing voluntary activity • Clonazepam, diazepam, nitrazepam, lorazepam and flurazepam have more prominent anticonvulsant activity
  • 17. MECHANISM OF ACTION: BENZODIAZEPINES ↓ BINDS TO BZD RECEPTOR PRESENT IN THE ΑLPHA SUB UNIT OF GABA-A RECEPTOR ↓ IT INCREASE THE BINDING OF GABA TO THE GABA-A RECEPTOR ↓ INCREASES THE INFLUX OF MORE Cl- IONS IN TO INTRACELLULAR SITE ↓ HYPERPOLARIZATION ↓ SEDATION/HYPNOSIS
  • 18.
  • 19. PHARMACOKINETICS • Absorbed orally • Plasma protein binding also varies markedly (flurazepam 10% to diazepam 99%). • BZDs are widely distributed in the body. • Benzodiazepines are metabolized in liver mainly by CYP3A4 and CYP2C19 • Some BZDs (e.g. diazepam) undergo enterohepatic circulation. • BZDs and their phase I metabolites are excreted in urine as glucuronide conjugates. • BZDs cross placenta and are secreted in milk.
  • 20. ADR: • Benzodiazepines are relatively safe drugs. Side effects of hypnotic doses are • dizziness, • vertigo, • ataxia, • disorientation, • amnesia, • prolongation of reaction time—impairment of psychomotor skills (should not drive). Uses: • As hypnotic • As anxiolytic • As anticonvulsant, • As centrally acting muscle relaxant • In preanaesthetic medication, • In Alcohol withdrawal
  • 21. NON-BENZODIAZEPINE HYPNOTICS • This lately developed group of hypnotics are chemically different from BZDs, • Act as agonists on a specific subset of BZD receptors. • They have lower abuse potential than hypnotic BZDs. Zopiclone • This is the first of the non-BZD hypnotics, • Which acts as an agonist at a subtype of BZD receptor involved in the hypnotic action. • The effect on sleep resemble those of BZDs, but it does not alter REM sleep and tends to prolong stages 3 and 4. • It is reported not to disturb sleep architecture, but some degree of next morning impairment can occur.
  • 22.