(Ch 19) Sedative-Hypnotic and Anxiolytic

Question 1

What are CNS Depressants?

Answer 1

CNS depressants are medications that suppress the transmission of information throughout the central nervous system.

Question 2

What are the 7 Classifications of CNS Depressants

Answer 2

There are 7 classifications of CNS depressants.

They are:

1. Sedative-hypnotics
2. General and local anesthetics
3. Analgesics
4. Narcotic analgesics 5. Anticonvulsants
5. Antipsychotics
6. Antidepressants

Question 3

Define anxiety:

Ex of symptoms involved:

Answer 3

An unpleasant emotional state consisting of apprehension, tension, and feelings of danger without a real or logical cause

Tachycardia- Tachypnea -Sweating -Trembling Weakness

Question 4

What are the 4 major classes of drugs used to treat anxiety?

Answer 4

1. Benzodiazepines—the most frequently used drugs for anxiety, most important group, used as sedative and hypnotic agents.

2. Azapirones—(5-HT 1a receptor agonist, ex: Buspirone) are a class of drugs used as anxiolytics, antidepressants, and antipsychotics.

They are commonly used as add-ons to other antidepressants, such as selective serotonin reuptake inhibitors (SSRIs

3. Barbiturates—rarely used today because of severe side effects and a low therapeutic index. These drugs have generally been replaced by the benzodiazepines.

4. β -adrenoceptor antagonists (e.g. propranolol). They are used to treat some forms of anxiety,

where physical symptoms (sweating, tremor, and tachycardia), are troublesome. They are not used as hypnotics.

Question 5

Ex: Benzodiazepines and their approximate duration of action:

Short-Acting

Answer 5

Short-Acting (2 to 8 hr):

1. Triazolam (Halcion)
2. Oxazepam (Serax)
3. Midazolam (Versed)
4. Clonazepam (Klonopin)

Question 6

Ex: Benzodiazepines and their approximate duration of action:

Intermediate-Acting

Answer 6

Intermediate-Acting (10 to 20 hr):

1. Temazepam (Restoril)
2. Lorazepam (Ativan)
3. Alprazolam (Xanax)
4. Alprazepam

Question 7

Ex: Benzodiazepines and their approximate duration of action:

Long-Acting

Answer 7

Long-Acting (1 to 3 days):

1. Chlordiazepoxide (Librium)

2. Diazepam (Valium)

3. Flurazepam (Dalmane)

4. Clonazepam

Question 8

Benzodiazepines:

Bind strongly to what ?

Are inactivated by what ?

Answer 8

Benzodiazepines are well absorbed when given orally.

1. They bind strongly to plasma proteins, however, many of them accumulate gradually in the body fat (i.e. they are highly lipid soluble).
2. Benzodiazepines are inactivated by the liver and excreted in the urine.

Question 9

Benzodiazepines:

Pharmacodynamics ?

Answer 9

Pharmacodynamics

Act by binding to a specific regulatory site on the GABAA receptor, thus enhancing the inhibitory effects of GABA. Central nervous system effects of benzodiazepines include:

1. Reduction of anxiety and aggression.
2. Sedation and induction of sleep.
3. Reduction of muscle tone and coordination.
4. Anticonvulsant effects

Question 10

Benzodiazepines

Clinical Uses:

Answer 10

Clinical Uses

Treatment insomnia

Anxiety

Preoperative mediations

Acute alcohol withdrawal

As anticonvulsants

Chronic muscle spasm and spasticity

Question 11

Benzodiazepines:

Side-effects

Answer 11

Side-effects

Toxic effects due to acute overdosage causes prolonged sleep.

Side-effects occurring during normal therapeutic use includes:

drowsiness, confusion, amnesia, and impaired motor coordination.

Tolerance and dependance: Pharmacokinetic and tissue tolerance and also cause physical dependance.

i.e. stopping benzodiazepines treatment after weeks or months causes an increase in symptoms of anxiety.

Question 12

Benzodiazepine

Pharmacokinetic:

Answer 12

Pharmacokinetic:

Absorbed from GI tract; crosses blood– brain barrier; metabolized in liver, and excreted in urine

Question 13

What is GABA?

Answer 13

GABA (γ-aminobutyric acid) is the major inhibitory neurotransmitter of the CNS.

Question 14

How do benzodiazepines work?

Answer 14

1. When benzodiazepines bind to specific receptors that are separate from but adjacent to the GABAA receptor, they potentiate the binding of GABA to its own receptor.
2. The binding of GABA to its own receptor results in increased chloride ion conductance, cell membrane hyperpolarization, and decreased initiation of action potentials.

Remember that benzodiazepines do not bind to GABA receptors—they bind adjacent to them

Question 15

What are the therapeutic indications for benzodiazepines?

Name 4

Answer 15

These drugs are used clinically as muscle relaxants and in the treatment of the following:

1. Anxiety disorders

2. Panic disorders—alprazolam is the drug of choice.
Status epilepticus—diazepam is the drug of choice.
3. Sleep disorders—flurazepam or temazepam.
4. Alcohol withdrawal—diazepam is most commonly used.

Question 16

Are benzodiazepines effective for controlling pain as well as anxiet?

Answer 16

No. They have little analgesic effect.

Question 17

Benzodiazepine:

What is their route of administration?

Answer 17

PO, IV, or IM

Question 18

Where are benzodiazepines metabolized?

Answer 18

They are metabolized in the liver and excreted in the urine. Many of the benzodiazepines have active metabolites.

Question 19

Does dependence occur?

Answer 19

Yes. Prolonged use can result in dependence. Abrupt discontinuation can result in withdrawal symptoms, including confusion, anxiety, and agitation.

Question 20

What types of symptoms may a patient taking benzodiazepines experience?

Answer 20

• Drowsiness and confusion—the most common side effects: Ataxia (loss of full controll of bodily movements) Dizziness
• Respiratory depression and death if taken with other CNS depressants such as ethanol

Question 21

What are Sedative-hypnotics?

Ex:

Answer 21

Sedative-hypnotics (Benzodiazepines) , the mildest form of central nervous system depressant, are given in low doses to diminish physical and mental responses without affecting consciousness.

Short-acting sedative-hypnotics are prescribed to help fall asleep, allowing the patient to awake early without a lingering after effect.

Intermediate-acting sedative-hypnotics are used for sustaining sleep and have residual drowsiness after waking.

NOTE: Sedative-hypnotics are not prescribed for patients who have severe respiratory disorders or who are pregnant.

Sedative-hypnotics are prescribed for short-term use because the patient can develop a tolerance of and dependency on the medication. Avoid chronic use of sedative-hypnotics.

Question 22

5 - HT1A receptor agonist

• Provide Ex:*
• Define:*
• SE:*

Answer 22

Buspirone

is a potent agonist of. 5 - HT1A receptors. Anxiolytic effects take days to weeks to develop.

• Buspirone does not cause sedation*, motor incoordiation and withdrawal effects.
• The main side effects*: are nausea, dizziness, headache, and restlessness.

Question 23

Schedule IV: Drugs

• Benzodiazepine’s:*
• Examples? 5*

Answer 23

1. Flurazepam hydrochloride (Dalmane)
2. Diphenhydramine (Benadryl)
3. Temazepam (Restoril)
4. Triazolam (Halcion)
5. Zolpidem (Ambien)

Question 24

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV:

Use:

Answer 24

• Short-term treatment of insomnia* (up to 4 weeks); a. a. reduces sleep induction time
  b. reduces number of nocturnal awakenings; increases length of sleep.

Question 25

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV:

How it works:

Answer 25

• Enhances action of inhibitory neurotransmitter gamma-aminobutyric acid (GABA), producing hypnotic effect caused by CNS depression

Question 27

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV:

Adult dose

Answer 27

1• Flurazepam hydrochloride (Dalmane) 15–30 mg at bedtime (15 mg for elderly)

2• Zolpidem (Ambien): PO 10 mg at bedtime (elderly, debilitated 5 mg)
3• Triazolam (Halcion): PO 0.125–0.5 mg at bedtime (elderly 0.0625–0.125 mg)

4• Temazepam (Restoril): PO 15–30 mg at bedtime (elderly 7.5–15 mg)

Question 28

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV:

Administration

Answer 28

• Give without regard to meals.
• Capsules may be emptied and mixed with food.
• Triazolam (Halcion): Tablets may be crushed and grapefruit juice may alter absorption.
• Zolpidem (Ambien): For faster sleep onset, do not give with or immediately after a meal.

Question 30

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV:

Contraindications:

Answer 30

• Narrow-angle glaucoma, acute alcohol intoxication, and pregnancy. Use with caution with impaired liver or kidney function.

Question 31

SEDATIVE–HYPNOTIC–BENZODIAZEPINE–SCHEDULE IV: (control substances)

Side effects / Adverse reactioins

Answer 31

SE• Drowsiness, dizziness, ataxia, sedation. Morning drowsiness may occur initially. Occasionally GI disturbances, nervousness, blurred vision, dry mouth, headache, confusion, skin rash, irritability, and slurred speech

AR• Hangover, REM Rebound, dependence, tolerance, excessive depression, respiratory depression, hypersensitivity

Question 32

What is flumazenil’s MOA?

Answer 32

Flumazenil is a competitive antagonist of benzodiazepines at the GABAA receptor.

Question 33

Describe the clinical use of Flumazenil drug.

Answer 33

Reversal of benzodiazepine sedation or overdose

Question 34

How is Flumazenil administered to the patient

Answer 34

IV use only

Question 35

How long do the effects of flumazenil last?

Answer 35

Only 1 hr—Repeat doses may be necessary for a heavily sedated patient to remain alert.

Question 36

AZAPIRONES: BUSPIRONE (BuSpar)

How does buspirone work?

Answer 36

It acts as a partial agonist at serotonin (5- HT1A) receptors.

Question 37

AZAPIRONES: BUSPIRONE (BuSpar)

What are the indications for this drug?

Answer 37

Buspirone is used for generalized anxiety;

however, unlike benzodiazepines,

its effects may take 1 to 2 weeks to become apparent.

Question 38

AZAPIRONES: BUSPIRONE (BuSpar)

What are the pharmacokinetic properties of buspirone?

Answer 38

This drug is metabolized by the liver and excreted in the urine;

its half-life is 2 to 11 hr.

Question 39

AZAPIRONES: BUSPIRONE (BuSpar)

How do the actions of buspirone differ from those

of the benzodiazepines?

Answer 39

Buspirone lacks the muscle relaxant and anticonvulsant properties of the benzodiazepines.

Question 40

AZAPIRONES: BUSPIRONE (BuSpar)

What advantages does buspirone have over benzodiazepines?

Answer 40

1. Minimal sedation
2. Low abuse potential
3. No overdose fatalities reported
4. No withdrawal symptoms

Question 41

AZAPIRONES: BUSPIRONE (BuSpar)

What toxic effects are associated with buspirone?

Answer 41

Headache, nausea, dizziness

Question 42

Define Barbituates:

Answer 42

They are non-selective CNS depressants, which produce effects ranging from sedation and reduction of anxiety, to unconsciousness and death from respiratory and cardiovascular failure.

Question 43

BARBITURATES act by:

Answer 43

Barbiturates act by enhancing action of GABA,

• but less specific than benzodiazepines.
• They are potent inducers of hepatic drug metabolizing enzymes, hence likely to cause drug interaction.
• Tolerance and dependance occur, more than benzodiazepines

Question 44

BARBITURATES are classified as?

Specifically USED for WHAT and are able to control WHAT condition?

Answer 44

Classified as type of Sedative-Hypnotic

Use: to induce sleep and as an anesthetic.

-In high doses barbiturates control epileptic seizures.

Question 45

Barbiturates are considered what Class of Drugs and by duration of Action.

Class of Drugs?

Name the Durations of Action?

Answer 45

Barbiturates are Class II controlled substances prescribed for no more than two weeks because of adverse side effect such as CNS depression in the elderly.

Barbiturates are classified by duration of action.

1. Ultrashort-acting: Ultra–short-acting barbiturates (thiopental sodium; Pentothal) are an anesthetic
2. Short-acting: Short-acting barbiturates (Secobarbital; Seconal), pentobarbital (Nembutal) induce sleep
3. Intermediate-acting: Intermediate-acting barbiturates (amobarbital; Amytal), aprobarbital (Alurate) and butabarbital (Butisol)) induce longer sleep periods
4. Long-acting: Long-acting barbiturates (phenobarbital and mephobarbital) control epileptic seizures

Question 46

Give 4 ex of barbiturates and their duration of action.

Answer 46

1. Phenobarbital (Luminal)—long- acting/1–2 days.
2. Pentobarbital (Nembutal)—short- acting/2–8 hours.
3. Amobarbital (Amytal)—short-acting
4. Thiopental (Pentothal)—ultra–short-acting/10–20 minutes.

Question 47

Barbiturates

How do these drugs work?

Answer 47

Like benzodiazepines, barbiturates increase the duration of GABA action on Cl– entry into the cell, which results in membrane hyperpolarization and a decrease in neuron excitability.

Barbiturates do not bind to benzodiazepine receptors.

Question 48

What are the therapeutic indications for barbiturate administration?

Answer 48

• Induction of anesthesia—thiopental
• Anticonvulsants—eg: phenobarbital
• TX of Anxiety—rarely
• Induction of Hypnosis

Question 49

Why are benzodiazepines favored over barbiturates for the treatment of anxiety?

Answer 49

Benzodiazepines have a much higher therapeutic index, cause less physiological dependence, and do not induce hepatic enzymes

Question 50

By what routes can barbiturates be administered?

Answer 50

IV, PO, or IM

Question 51

What are the pharmacokinetic properties of barbiturates?

Answer 51

They are metabolized in the liver and excreted in the urine.

Question 52

What determines the duration of action of thiopental?

Answer 52

Redistribution to the other tissues

Question 53

Does barbiturate dependency occur?

Answer 53

Yes. Abrupt cessation can lead to severe withdrawal symptoms (tremor, restlessness, nausea, seizures, and cardiac arrest).

Question 54

For whom are barbiturates contraindicated?

Answer 54

For patients who have acute intermittent porphyria, because they increase porphyrin synthesis

Acute intermittent porphyria (AIP) is one of the porphyrias, a group of hereditary diseases that involve defects in heme metabolism and result in excessive secretion of porphyrins and porphyrin precursors.

-AIP manifests as episodes of abdominal pain, neuropathies, and constipation, but, unlike most types of porphyria, patients with AIP do not have a rash

Question 55

What are the adverse effects of Barbituates drugs?

Answer 55

• -Drowsiness* and decreased motor control
• Induction of the P-450 system, which can therefore decrease the effect of other drugs metabolized by these enzymes
• -*Addiction-

In high doses, respiratory depression and coma

-Allergic reactions-

especially in patients with asthma

Question 56

SEDATIVE-HYPNOTIC: BARBITURATES and Others

USE:

Answer 56

Treat insomnia; use for sedation, preoperative medication, barbiturate
coma (for controlled increased intracranial pressure)

Question 57

SEDATIVE-HYPNOTIC: BARBITURATES and Others

Example:

Answer 57

pentobarbital sodium (Nembutal Sodium)

-short-acting barbiturate

Question 58

SEDATIVE-HYPNOTIC: BARBITURATES and Others

How it works:

Answer 58

• Depression of the CNS, including the motor and sensory activities

Question 59

SEDATIVE-HYPNOTIC: BARBITURATES and Others

Adult Dose:

Answer 59

• PO 20–30 mg TID
• Hypnotic: PO 100–200 mg
• Preoperative PO/IM/IV: 100 mg, repeat if needed

Question 60

SEDATIVE-HYPNOTIC: BARBITURATES and Others

Administration:

Answer 60

• IV pentobarbital at a rate of less than 50 mg/min. • Do NOT mix with other medications.
• IM should be given into a large muscle.
• PO give 30 minutes before bedtime

Question 61

SEDATIVE-HYPNOTIC: BARBITURATES and Others

After administrations: Safety steps

Answer 61

• Maintain a safe environment after administration (side rails up; proper lighting; toileting before medicating).

• Monitor vital signs.
• Observe for adverse reactions.
• Observe for signs of withdrawal if taken over a prolonged period of time and then abruptly discontinued.

Question 62

SEDATIVE-HYPNOTIC: BARBITURATES and Others

Contraindications

Answer 62

• Respiration depression, severe liver disease, pregnancy (fetal immaturity), nephrosis

Nephrosis: kidney disease, especially when characterized by edema and the loss of protein from the plasma into the urine due to increased glomerular permeability. Also called nephrotic syndrome.

Question 63

SEDATIVE-HYPNOTIC: BARBITURATES and Other

Side Effects-Adverse Reactions

Answer 63

SE• Nausea, vomiting, diarrhea, lethargy, drowsiness, hangover, dizziness, rash
• Drug dependence or tolerance, urticaria (hives), hypotension if given rapidly IV

AE• Respiratory distress, laryngospasm

Question 64

SEDATIVE-HYPNOTIC: BARBITURATES and Other

Short Acting EX:

1. Class:
2. Use:
3. ROA:

Answer 64

Secobarbital sodium

1. (Seconal Sodium) class II
2. Preoperative sedation / Used to induce sleep
3. PO 100–200 mg before surgery / hypnotic PO/IM 100–200 mg

Question 65

SEDATIVE-HYPNOTIC: BARBITURATES and Other

Intermediate-acting: Name Ex

Class:

Use:

ROA:

Answer 65

Amobarbital sodium

Class: (Amytal Sodium)

Use: Sleep sustainers

ROA:

Status epilepticus: IV; 5.5 mg/kg; reappear in 3–4 hours; with spinal anesthesia IV; 50–100 mg.; infused over 30 seconds; maximum dose of 250/mg

PB 50%–60%; half-life 20–40 hours;

Sedative: PO 30–50 mg BID-TID;

Hypnotic PO/IM 65–200 mg/h, IV: 65–200 mg

Question 66

SEDATIVE-HYPNOTIC: BARBITURATES and Other

Provide 2 Examples of other Barbiturates

Answer 66

1. Chloral hydrate Class IV

2. Paraldehyde Class IV

Question 67

Chloral hydrate Class IV

Describe

Answer 67

• -No hangover* and less respiratory depression;
• give with meals or fluids to prevent gastric irritation

Question 68

Paraldehyde Class IV

Describe:

Answer 68

Exhaled via the lungs; strong odor and disagreeable taste; seldom used; has been used to control delirium tremens (DTS) in alcoholics; can be used for drug poisoning