Anxiolytic , Sedative and Hypnotic Drugs-2
Benzodiazepines are the most widely used anxiolytic drugs.They have largely replaced barbiturates because:
The benzodiazepines are safer (have a wide therapeutic index) and more effective
Not cause drug – drug interaction(not induce hepatic microsomal enzyme)
Produce tolerance and psychological dependence but physical dependence and withdrawal symptom are less marked
Benzodiazepines are classified according to their duration of action into:
Short – acting : Oxazepam, Triazolam (3-8) hours Intermediate – acting : Alprazolam, Lorazepam , Temazepam (10-20) hours
Long-acting : Chlordiazepoxide, Diazepam, Flurazepam
Benzodiazepines
ANXIOLYTIC: Alprazolam, chlordiazepoxide , diazepam, lorazepam HYPNOTIC: Triazolam, temazepam, flurazepam.
Mechanism of action:
Binding of GABA (the major in hibitory neurotransmitter in the central nervous system) to its receptor triggers an opening of a chloride channel, which leads to an increase in chloride conductance Benzodiazepines increase the frequency of channel openings produced by GABA.
The influx of chloride ions causes hyperpolarization of the cell making it more difficult to depolarize and there for reduces neural excitability
Actions:
The benzodiazepines have neither antipsychotic activity nor analgesic action
Reduction of anxiety: At low doses, the benzodiazepines are anxiolytic.
Sedative and hypnotic actions: All of the benzodiazepines used to treat anxiety have some sedative properties, and some can produce hypnosis (artificially produced sleep) at higher doses.
Anticonvulsant: some are used to treat epilepsy (status epilepticus) and other seizure disorders.
Muscle relaxant: At high doses, the benzodiazepines relax the spasticity of skeletal muscle
Therapeutic uses:
Anxiety disorders: Benzodiazepines are effective for the treatment of the anxiety.generalized anxiety disorder, specific phobias, such as fear of flying.
Muscular disorders: Diazepam is useful in the treatment of skeletal muscle spasms, multiple sclerosis and cerebral palsy.
The shorter-acting agents are used as premedication for anxiety-provoking and unpleasant procedures, such as endoscopic, bronchoscopic, dental procedures.
They cause a form of conscious sedation, allowing the person to be receptive to instructions during these procedures.
Midazolam is an injectable-only benzodiazepine also used for the induction of anesthesia
Seizures: Clonazepam is occasionally used in the treatment
of certain types of epilepsy Diazepam and lorazepam are the drugs of choice in terminating grand mal epileptic seizures and status epilepticus.
chlordiazepoxide,, diazepam, and oxazepam are useful in the acute treatment of alcohol withdrawal
Sleep disorded :Flurazepam has a long-acting effect and causes no rebound insomnia.
Temazepam: This drug is useful in patients who experience frequent wakening.
the peak sedative effect occurs 1 to 3 hours after an oral dose; and
should be given 1 to 2 hours before bedtime.
Triazolam: short duration of action and, therefore, is used to induce sleep in patients with recurring insomnia.
Whereas temazepam is useful forinsomnia caused by the inability to stay a sleep
triazolam is effective in treating individuals who have difficulty in going to sleep
Pharmacokinetics
• lipophilic,
• rapidly and completely absorbed after oral administration
• distribute throughout the body .
The half-lives of the benzodiazepines are very important clinically, because the duration of action may determine the therapeutic usefulness, The longer-acting agents form active metabolites with long half-lives.
However, with some benzodiazepines, the clinical durations of action do not always correlate with actual half-lives.
Most benzodiazepines, including chlordiazepoxide and diazepam, are metabolized by the hepatic microsomal system to compounds that are also active.
The benzodiazepines are excreted in the urine as glucuronides or oxidized metabolites.
All the benzodiazepines cross the placental barrier and may depress the CNS of the newborn if given before birth.
Nursing infants may also become exposed to the drugs in breast milk
Adverse effects
Drowsiness and confusion: Psychological and physical dependence on benzodiazepines can develop if high doses of the drugs are given over a prolonged period
withdrawal symptoms, including confusion, anxiety, insomnia, tension, and rarely, seizures.
• a short elimination half-life(rapidly eleminated), such as triazolam, induce more abrupt severe withdrawal reactions than drugs that are slowly eliminated, such as flurazepam
Precautions:
In treating patients with liver disease. In patients with acute narrow-angle glaucoma.
Alcohol and other CNS depressants enhance the sedative-hypnotic effects of the Benzodiazepine.
Benzodiazepine Antagonist
Flumazenil (is a GABA-receptor antagonist) that can rapidly reverse the effects of benzodiazepines(competitively occupies a GABA-receptor without causing a functional change in CL channel) .
• for intravenous administration only.
• rapid Onset of action
• short duration, with a half-life of about 1 hour.
Frequent administration may be necessary to maintain reversal of a long-acting benzodiazepine
Side effects:
1.Dizziness, nausea, vomiting, and agitation
2.withdrawal in dependent patients
3. seizures
• If a benzodiazepine is used to control seizure activity
• If the patient ingests tricyclic antidepressants
Other anxiolytic drugs:
Buspirone , hydroxyzine
Buspirone
• Is useful in the treatment of generalized anxiety disorder• has efficacy comparable to that of the benzodiazepines.
• Mode of action differs from that of the benzodiazepines
because:
• The actions of buspirone appear to be mediated by
• Serotonin (5-HT1A) receptors, buspirone displays some affinity for DA2 dopamine receptors and 5-HT2A serotonin receptors
• undergoes metabolism by CYP3A4; thus, its half-life is shortened if taken with rifampin (an inducer of the enzyme)
• lengthened if taken with erythromycin (an inhibitor of the enzyme)
• Adverse effects: Headaches, dizziness ,nervousness
• Disadvantage: Buspirone has the slow onset of action
Hydroxyzine:
is an antihistamine with antiemetic activity. It has a low tendency for habituation and, thus, is useful for patients with anxiety who have a history of drug abuse.It is also often used for sedation prior to dental procedures or surgery. Drowsiness is a possible adverse effect
Antidepressants: many antidepressants have proven efficacy in managing the long-term symptoms of chronic anxiety disorders and should be considered as first-line agents, especially in patients with concerns for addiction or dependence or a history of addiction or dependence to other substances.
The SSRIs, TCAs, venlafaxine, duloxetine and MAOIs all have potential usefulness in treating anxiety
Other Hypnotic Agents
Zolpidem
• Is not a benzodiazepine in structure, but it acts on a subset of the benzodiazepine receptor family, BZ1.
• Zolpidem has no anticonvulsant or musclerelaxing properties
• It shows few withdrawal effects, and minimal rebound insomnia, and little or no tolerance occurs with prolonged use.
• Zolpidem is rapidly absorbed from the gastrointestinal tract, and it has a rapid onset of action and short elimination half-life (about 2 to 3 hours).
• . Zolpidem undergoes hepatic oxidation by the cytochrome p450 system to inactive products.
• Drugs such as rifampin, which induce this enzyme system, shorten the half-life of zolpidem,
• Drugs that inhibit the CYP3A4 isoenzyme may increase the half life
this drug.
• Adverse effects of zolpidem include nightmares, agitation, headache,
gastrointestinal upset, dizziness, and daytime drowsiness.
Ramelteon: is a selective agonist at the MT1 and MT2 subtypes of melatonin receptors stimulation of MT1 and MT2 receptors by melatonin the hypothalamus is able to induce and promote sleep
Ramelteon is indicated for the treatment of insomnia in which falling asleep (increased sleep latency) is the primary complaint.
The potential for abuse of ramelteon is minimal, and no evidence of dependence or withdrawal effects has been observed. Therefore, ramelteon can be administered long-term.
• Adverse effects of ramelteon include dizziness, fatigue .
• Ramelteon may also increase prolactin level .
Chloral hydrate
• The drug is an effective sedative and hypnotic that
• Induces sleep in about 30 minutes and the duration of sleep is about 6 hours.
• Chloral hydrate is irritating to the gastrointestinal tract and causes epigastric distress
• It also produces an unusual, unpleasant taste sensation.
• It synergizes with ethanol.
Antihistamines: diphenhydramine
• They are effective in treating mild types of insomnia.• They have numerous undesirable side effects (such as anticholinergic effects) that make them less useful than the benzodiazepines.
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