Drugs Acting On Central Nervous System PDF

Summary

This document provides an overview of drugs that affect the central nervous system, categorizing them as opiod (narcotic) analgesics and non-opiod analgesics. It details mechanisms of action, therapeutic uses, and examples of each type of drug. It is suitable for medical professionals or advanced undergraduate/postgraduate students in the field of pharmacology or related disciplines.

Full Transcript

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‫ﻛﻠﯾﺔ اﻟطب اﻟﺑﯾطري‬

‫ﺟﺎﻣﻌﺔ واﺳط‬
‫ ﺳرﺣﺎن اﻟزﯾﺎدي‬.‫د‬

[DRUGS ACTING ON CNS]
The central nervous system (CNS) is the part of the nervous system consisting of the
brain and spinal cord. The central nervous system is so named because it integrates
information it receives from, and coordinates and influences the activity of, all parts of
the bodies of bilaterally symmetric animals
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Drugs Acting On Central Nervous System

I. Narcotic Analgesics

Analgesics are drugs that relieve pain due to multiple causes.

Analgesics are classified into 2 main groups:

Opioid (Narcotic) Analgesics Non-opioid Analgesics
(analgesics- antipyretics)
· Are the most powerful analgesics Are mild analgesics and effective in certain
that can relieve any type of pain types of pain as headache, toothache …
except itching.
· Act mainly at the level of the cortex. · Act on the level of the thalamus and
hypothalamus.

· Can produce addiction. · No addiction.
Used to lower the elevated body
temperature.
·Example: Morphine and codeine. Example: NSAIDs e.g. salicylates, and paracetamol

NARCOTIC ANALGESICS

They are derived from opium alkaloids. Many alkaloids are isolated from

opium, but few of them are used clinically.

OPIUM ALKALOIDS

I. Morphine

Dose: 8­15mg by injection (subcutaneously or IM) as morphine hydrochlorideor
morphine sulfate.

Pharmacological Actions of Morphine:

(I) On C.N.S:

A. Centers Depressed by Morphine:

1. Cortical pain center:
2. Respiratory center:
3. Cough center:
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4. Inhibition of the polysynaptic spinal reflexes.
5. Inhibition of the vasomotor center in large doses.
B. Centers stimulated by Morphine:
1. Vomiting center: Emetic chemoreceptor trigger zone (CTZ) in the medullais stimulated
by morphine leading to nausea and vomiting.
2. Occulomotor center:
Morphine causes severe miosis
3. Stimulation of monosynaptic spinal reflexes (stretch reflex).
4. Release of antidiuretic hormone (ADH) form the posterior pituitary.
5. Stimulation of cardiovagal center: leading to slow and full pulse.

Opioid Receptors:
Several types of opioid receptors have been identified at various sites in the
nervous system and other tissues.
Mu (μ) receptors are responsible for:
(1) Supraspinal analgesia
(2) Euphoria, sedation.
(3) Respiratory depression,
(4) Physical dependence.
(5) Constipation.
(6) Miosis.
Kappa (κ) receptors are responsible for:
(1) Spinal analgesia.
(2) Miosis and sedation.
Delta ()receptors:
Supraspinal analgesia
Tolerance: (failure of responsiveness to the usual dose of the drug)
Tolerance develops to the analgesic and respiratory depressant actions oforphine after
10­14 days.

Therapeutic Uses of Morphine:

(1) As a powerful analgesic in the treatment of severe pain
(2) Pre­anaesthetic medication: 10­15 mg subcutaneously or IM one hourbefore the
general anaesthesia.
(3) to alleviate dyspnoea.
(4) Certain cases of severe cough e.g. cancer of the bronchial tree.
(5) Certain cases of severe diarrhea (loperamide) given orally after removingthe
poison causing the diarrhea from the intestine by a purgative.
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II. Codeine (Methyl Morphine)
1. It is less potent.
2. It produces constipation.
3. Nausea and vomiting are less.
4. Less addiction.
Uses:
1. As cough depressant (for dry cough).
2. As analgesic with aspirin and paracetamol.

SYNTHETIC MORPHINE DERIVATIVES

1. Heroin (Diacetyl Morphine) (semisynthetic)
2. Pethidine
3. Fentanyl
4. Methadone
5. Loperamide (Imodium) and diphenoxylate: are nonanalgesicopioids, used for
antimotility effect on the gut.

OPIOID ANTAGONISTS

1. Nalorphine : It has antagonist action on Mu receptors, with a partial agonist
action on deltaand Kappa receptors so it is considered as a partial antagonist.
2. Naloxone: It is a pure narcotic antagonist at all opioid receptor sites with no
morphine likeproperties i.e. it is a pure antagonist.
3. Naltrexone: has a longer duration of action than naloxone and a single oral

Therapeutic Uses:

1. Treatment of acute morphine poisoning (it stimulates respiration, improvesmiosis,
vomiting and G.I spasm).

2. Diagnosis of opium addiction (precipitate withdrawal symptoms).

Sedative–Hypnotic Drugs
The major therapeutic use of sedative­hypnotic drugs is to cause sedation (with
concomitant relief of anxiety) or to encourage sleep.
Examples of Sedative-Hypnotic drugs:
1­ Benzodiazepines
2­ Buspirone
3­ Zolpidem
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4­ Barbiturates
5­ Chloral hydrate, paraldehyde
6­ Ethyl alcohol (Ethanol)

I. BENZODIAZEPINES
Benzodiazepines (BZs) are the most widely used anxiolytic drugs.

Mechanism of Action:
Gamma­aminobutyric acid (GABA) is the major inhibitory neurotransmitter in the CNS.
BZs potentiate GABA­ergic inhibition at all levels of the CNS. BZs bind to specific, high
affinity BZ receptors present in various parts of the CNS. These receptors are separate but
adjacent to the receptor for GABA. The binding of BZ enhances the affinity of the
GABA receptors for GABA neurotransmitter, resulting in a more frequent opening of
adjacent chloride channels. The increased influx of Cl­ into the neuron results in
enhanced hyperpolarization and inhibition of neuronal firing.

Pharmacological Actions:
1. Reduction of anxiety: At low doses, BZs are anxiolytic.

2. Sedation and induction of sleep: At higher doses, all BZs which are used to treat
anxiety can produce hypnosis.

3. Muscle relaxation: BZs relax the spasticity of skeletal muscles, probablyby increasing
presynaptic inhibition in the spinal cord. Diazepam inparticular, has a very pronounced
depressant activity on skeletal muscles.

4. Anticonvulsant effect.

Classification of Benzodiazepines

 Short-acting; triazolam (3­8 hours).
 Intermediate-acting; alprazolam (10­20 hours).
 Long-acting; diazepam (1­3 days).

2. ZOLPIDEM
Mechanism of action:Zolpidem is a hypnotic that binds selectively to a subset of the
BZs receptorfamily and facilitates GABA­mediated neuronal inhibition.

3. BARBITURATES

Non­selective CNS depressants, which produce effects ranging from sedationand
reduction of anxiety to hypnosis and unconsciousness. Barbiturates werein the past the
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mainstay of treatment used to sedate or to induce and maintainsleep.Today, they have
been largely replaced by BZs.

Classification:

1. Ultra-short acting: Thiopental Na is highly lipid soluble; it is an IV anesthetic
that acts within seconds with duration of action of 20 minutes. (pre­anesthetic
medication).
2. Short-acting: Pentobarbital and secobarbital act for 3­8 hours. (anesthesia)
3. Long-acting: Phenobarbital (more than 24 hours). Antiepileptic

Mechanism of Action:

Barbiturates facilitate the actions of GABA at multiple sites in the CNS butthey do not
bind to the same site of BZs on the GABA­receptor/chloride channel. They cause
activation of GABAA receptors. This increases theduration of opening of the Cl­ channel
associated with the receptor, and theneuronal membrane is therefore hyperpolarized and
less likely to fire.

Therapeutic Uses:

1. Anaesthesia: Thiopental Na is used intravenously to induce anaesthesia.

2. As sedative-hypnotic agents: Barbiturates have been replaced by BZs.However,
pentobarbital may still be used as sleeping pills.

3. Anticonvulsants: Emergency treatment of convulsions in statusepilepticus by
thiopental as the last approach. Phenobarbital is used in longtermmanagement of tonic­
clonic seizures.

4. α2-Adrenoceptor agonists

E X A M P L E S: Xylazine, detomidine and medetomidine

Clinical applications

1. Sedative­hypnotics
2. muscle­relaxant
3. analgesic properties.
4. Chemicalrestraint
5. premedication in small and large animals.
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Mechanism of action

The sedative, analgesic and muscle­relaxant propertiesof the α2­agonists are mediated at
central α2­receptors. The primary mechanism involves a decreasein noradrenaline
(norepinephrine) release and therebyinhibition of impulse transmission. Sedation has
beenattributed to depression of neurons in brain stem.

SOME OLDER AND LESS COMMONLY USED SEDATIVE–HYPNOTICS

Chloral hydrate is an effective sedative and hypnotic that induces sleep in about 30
minutes and lasts about 6 hours. Chloral hydrate is metabolized into two major
metabolites; trichloroethanol (active and relatively nontoxic) and the other is
trichloroacetic acid, which is toxic and tends to accumulate in the body.

Paraldehyde produces hypnosis in about 15 minutes and its effect lasts for 4­8 hours..
Paraldehyde was used in patients with hepatic or renal failure as it is mainly eliminated
through the lung.

TRANQUILIZER
Classes of tranquilizers

1. Phenothiazines
E X A M P L E S: Acepromazine, chlorpromazine, promethazine, promazine,
prochlorperazine.
Mechanism of action
The sedative and antiemetic actions of phenothiazinesare due to antagonism of dopamine,
primarily at D2receptors.

2. Butyrophenones
E X A M P L E S: Fluanisone, droperidol and azaperone.

Mechanism of action
As for the phenothiazines, the sedative and antiemeticeffects of the butyrophenones are
primarily mediated byantagonism of dopamine. α­Adrenergic antagonismaccounts for the
cardiovascular effects of these agents.
3. Benzodiazepines
E X A M P L E S: Diazepam, midazolam and zolazepam
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CENTRAL NERVOUS SYSTEM STIMULANTS

Stimulation of CNS can be produced in men and animals by a large number of natural
and syntheticsubstances. As a group, the CNS stimulants have few clinical uses, but some
are important as drugsof abuse.

Drugs which cause CNS stimulation fall into three broad categories:

1. Convulsants and respiratory stimulants.
2. Psychomotor stimulants.
3. Psychotomimetic drugs (hallucinogens).
Stimulation of CNS can be produced in men and animals by a large number of natural
and syntheticsubstances.

1- CONVULSANTS and RESPIRATORY STIMULANTS

They are also called analeptics and act mainly on brain stem and spinal cord.They mainly
stimulate the respiratory and vasomotor centers in the brain stembut have little effect on
the mental function.

Examples of analeptics:

1­ Nikethamide
2­ Doxapram
3­ Strychnine:
Mechanism of Action:

Strychnine blocks the receptors for glycine which is the main inhibitorytransmitter acting
on motor neurons this will lead to increased reflex excitabilityof the spinal cord.Any
sensory stimulus, will initiate asymmetrical, uncoordinated tonicconvulsions of all limbs
that affect the most powerful muscles acting at a givenjoint. The back is arched, the neck
is thrown backwards and the face shows abitter smile. Death occurs due to involvement
of the respiratory muscles,respiration ceases and medullary paralysis occurs due to the
hypoxia.

Treatment of Strychnine Poisoning:

1. Transfer the patient to quiet dark room under the supervision of well­trainedstaff. Any
external stimulus must be avoided.
2. Thiopental i.v. in small repeated doses to stop convulsions. Mephensin (acentral
muscle relaxant) may be used.
3. Gastric lavage with 0.5% potassium permanganate or 2% tannic acidsolution to
remove the alkaloid from the stomach.
4. Artificial respiration and O2 inhalation.
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2. PSYCHOMOTOR STIMULANTS
These drugs have marked effect on the mental function and behavior; theyproduce
excitement, euphoria, reduced fatigue, and increased motor activity.Some are drugs of
abuse.
Examples: methylxanthines, amphetamines, and cocaine.

Methylxanthines

These include theophylline found in tea, theobromine found in cocoa, andcaffeine.
Caffeine, the most widely consumed stimulant in the world, is found in highest
concentrations in coffee but is also present in tea, cola drinks,chocolate candy and cocoa.

Mechanism of Action:

Methylxanthines act by several mechanisms including:

1. Translocation of extracellular calcium.

2. Inhibition of phosphodiesterase leading to increases in cyclic adenosinemonophosphate
(cAMP) and cyclic guanosine monophosphate (cGMP).

Therapeutic Uses:

1­ Caffeine: In combination with salicylates to relief simple headache and incombination
with ergotamine to relief migraine. To stimulate the depressedCNS in case of alcohol
ingestion.

2­ Theophylline: In cases of bronchial asthma, biliary colics, congestive heartfailure and
cardiac edema.
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Anti-Epileptic Drugs

Anti-epileptic drugs

Epilepsy is a recurrent, sudden, transient, excessive discharge of cerebral neurons without
anyimmediate provoking cause resulting in abnormal movements and/or sensory
perceptions (seizure).

1. Carbamazepine

Carbamazepine is structurally related to the tricyclic anti­depressants.

Mechanism of action

1. Use­dependent blockade of Na+ channels, which reduces cellexcitability, is the main
mechanism of action.
2. Suppresses repetitive neuronal firing.
3. Reduces propagation of abnormal impulses in brain.
4. Attenuates action and release of glutamate (excitatory neurotransmitter).
2. Phenytoin (diphenylhydantoin)

Mechanism of action

1. Use­dependent blockade of Na+ channels, which reduces cellexcitability, is the
main mechanism of action
2. Blockade of L­type Ca2+ channels
3. Potentiation of GABA action at GABAA receptors.

3.Lamotrigine

Mechanism of action

1. Use­dependent inhibition of neuronal Na+ channels (like carbamazepineand
phenytoin)
2. It interferes with synthesis of glutamate and aspartate.
3. Reduces glutamate release, possibly through inhibition of voltagesensitiveCa+2
channels.
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4.Sodium valproate

Mechanism of action
1. Use­dependent blockade of Na+ channels.
2. Potentiation of GABA by enhanced synthesis and release as well asreduced
degradation.
3. Attenuation of the excitatory action of glutamate.
4. Inhibition of T­type Ca2+ channels

5.Phenobarbital and Primidone

6. Benzodiazepines
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General anesthetics
General anaesthesia is a state of:
1. loss of sensation,
2. controllable reversible loss of consciousness and,
3. skeletal muscle relaxation.
Four stages of anaesthesia are known:
· Stage I (analgesia): loss of sensation but patient is still alert and speaking.

· Stage II (Excitement): CNS excitation+ ­ BP (irregular) + ­ respiratory rate + release
of subconscious emotions.

· Stage III (surgical anaesthesia): regular respiration + relaxed skeletal muscles +
progressive decrease in eye reflexes till eye movement stops and pupil is fixed

· Stage IV (Medullary paralysis): fatal depression of RC and VMC.

Classification of general anesthetic agents:

1. Inhaled volatile agents: They are hydrocarbons. They are suitable for
maintaining the anesthetic state as long as the surgical procedure is going on. In
the past, anaesthesia was induced and maintained by inhalation of a volatile agent
alone. If this method is used, the patient passes through the previously mentioned
stages (I­III) during induction and recovery of which the excitation stage (stage II)
is undesirable. Nowadays, this is overcome by using a bolus of intravenous
anesthetic for induction (see below), followed by an inhalation anesthetic for
maintenance. In children, this is less problematic and anaesthesia is often both
induced and maintained with an inhalational anaestheticagent.

2. IV anesthetic drugs: General intravenous anaesthesia can be used for short
surgical procedures. For longer procedures, an IV anesthetic agent is used for
rapid induction followed by an inhalational agent.

Pre-anaesthetic medications.

These are drugs used to facilitate smooth induction of anaesthesia and help to lower the
dose and side effects of anesthetic drugs. According to circumstances, pre­medication
may involve any combination of the following drugs (i.e. balanced general anaesthesia):

1. Benzodiazepines or barbiturates to induce sedation and to relieve anxiety.
2. H1 blockers (anti­allergic) and H2 blockers (to reduce gastric acidity).
3. Anti­emetic e.g. metoclopramide.
4. Opioid analgesics e.g. morphine or pethidine
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5. An anticholinergic e.g. scopolamine for prevention of bradycardia and to decrease
airway secretions.
Mechanism of action of general anaesthetic agents
1. It is suggested that incorporation of theanaesthetic into cell membrane
phospholipids alters cell membrane fluidity.
2. Anaesthetic agents may also enhance action of GABAA and glycinereceptors
and inhibit central actions of acetylcholine, serotonin, andglutamate.

Note; Resumption of consciousness (reversal of anaesthesia) occurs when the intravenous
anesthetic is redistributed out of CNS or metabolized, or when an inhalational anesthetic
is redistributed out of CNS or exhaled. Residual neuromuscular blockade may need
reversal with neostigmine

Intravenous anaesthetics
Examples:
1. Thiopental
2. Ketamine
3. Propofol

Inhalational anesthetics
Inhaled anesthetics are given with oxygen to avoid hypoxia during anaesthesia.
Following induction with an intravenous anesthetic, an inhalational agent can be used to
maintain anaesthesia.

Example

Halothane (Fluothane): an old but still used inhalational agent for mask induction in
children, because it is the least irritant volatile agent.
Enflurane: old and not recommended because of its powerful cardiac and respiratory
depressant actions.
Isofluranehas largely replaced halothane and enflurane because it offers the most rapid
induction and recovery and has little post­anesthetic organ toxicity
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Local anesthetics
Definition:
A local anesthetic is an agent that interrupts pain impulses in a specific region of the body
without loss of patient consciousness.

Chemical structure of local anesthetics

Mechanism of action
Local anesthetics block nerve conduction:
1. By interacting directly with specific receptors on neuronal Na+ channels, inhibiting
Na+ ion influx.
2. By impairing propagation of the action potential in the axons. Factors affecting onset,
intensity, and duration of neural blockade

1. Lipid solubility: a lipophilic local anesthetic is more potent because it is easier to
cross nerve membranes. This property is determined by the aromatic portion of the
molecule.
2. Protein binding: local anesthetics with a higher degree of protein binding have a
prolonged duration of action.
3. The pKa: The pKa is the pH at which 50% of the local anesthetic is in the ionized
form and 50% is in the unionized form. All local anesthetics are weak bases with pKa =
8­9.

 Local anesthetics with pKa close to physiologic pH are associated with agreater
fraction of the molecules existing in the unionized form = morepenetration across
nerve membranes = faster onset. (Small gap betweenpH and pKa)
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 Local infection (acidosis) increases the ionized drug fraction which meansless drug
will be available to penetrate across membranes and bind tointracellular local
anesthetic receptors on Na+ channels = slower onset.(Increased gap between pH and
pKa)

4. Dose: Increasing dose of the anaesthetric will increase the duration of the block.

Techniques of administration
1. Surface administration: High concentrations (up to 10%) of drug in an oily vehicle
can slowly penetrate the skin or mucous membranes to give a small localised area of
anaesthesia.
2. Infiltration anaesthesia: A local injection of local anesthetic solution, sometimes with
a vasoconstrictor, produces a local field of anaesthesia. The anesthetic effect produced is
more efficient than surface anaesthesia. This technique is extensively used in dentistry.
3. Peripheral nerve block anaesthesia: Injection of solution around a nerve trunk.
4. Epidural anaesthesia: Injection or slow infusion via a cannula adjacent to, but outside
the duramater. This technique is used extensively in obstetrics.
5. Spinal anaesthesia: Injection into lumbar subarachnoid space, usually between the
third and fourth lumbar vertebrae. Spinal and epidural anaesthesia can be used together,
often using an opioid (fentanyl) alone or in combination with a local anesthetic.
6. Intravenous regional anaesthesia (Bier block): Local anaesthetic injected into a vein
of a limb after application of a tourniquet. The resultant anaesthesia is produced by direct
diffusion of the local anesthetic from the vessels into the nearby nerves. It is used for
manipulation of fractures or surgery on wrist, hand and fingers.