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Презентация на тему Neuroleptics, lithium, tranquilazers, sedatives

Neuroleptics (Antipsychotic Drugs)
Lecture № 5   Neuroleptics, Lithium,  Tranquilazers, Sedatives.ZAPORIZHZHIA STATE MEDICAL Neuroleptics (Antipsychotic Drugs) MECHANISM OF ACTION:  		blockade of dopamine D2-receptors IN PERIPHERY : Pharmacological Effects:Antipsychotic Actions: 		⇓ Hallucination and AgitationAntiemetic EffectsExtrapyramidal Effects: 	D2-Rs blockade in Extrapyramidal Еffects: due to Blocking of D2 receptors in the Nigrostriatal Pathway: Clinical Uses of Neuroleptics 1. SCHIZOPHRENIA: Positive Symptoms of Schizophrenia : DELUSIONS, Aminazine (Chlorpromazine) - 					blocks CNS D2 receptors α-Recetor and GANGLIONIC BLOCKADE ? DROPERIDOL amp. 0.25%-10 ml – 				a BUTYROPHENONE derivative, more potent and to Lithium Salts Lithium Carbonate – Caps. 0.15 and 0.3 g; Tab. 0.3 CLINICAL USESBipolar Affective DisordersMajor Depression Schizoaffective Disorder Alcohol DependenceADVERSE EFFECTSPsychomotor retardation LethargyEpileptiform TRANQUILIZERS (ANXIOLYTIC DRUGS)   I. Benzodiazepines (BZDs):		Diazepam (Sibazon ) – amp. 0.5%-2 ml; BENZODIAZEPINES   according to their Duration of Action:1. Long-acting (24-48 hours):			Diazepam 			Phenasepam MECHANISM OF ACTION of BZDs:Bind to the α-subunit of the GABAA Rs		surrounding CLINICAL USES of BZDs1.ANXIETY and PANIC DISORDERS2. MUSCULAR DISORDERS: 	DIAZEPAM – 		⮟ Psychological and Physical Dependence -   if high doses are given BZD Antagonist: FLUMAZENIL –  a GABA receptor competitive antagonist that can DIAZEPAM (Sibazon) amp. 0.5%-2 ml; Tab. 0.005 g 	is a Tranquilizer, a Gidazepam Tab. 0.02 g; 0.05 g – 	DAY TRANQUILIZER – has ACTIVATING Busbirone - Tab. 10 mg - an non-BZD anxiolyticMECHANISM OF ACTION:⮟ Blocks 5-HT1A Sedative Drugs:1. BROMINE SALTS:	Sodium Bromide - NaBr	 Potassium Bromide - KBr2. VALERIAN’S BROMISM – chronic intoxication with BROM salts.Bromides eliminate slowly (T1/2=12 days), MANIFESTATION: Valerian’s and Motherwort’s Preparations - are widely used sedative drugs. VALERIAN’S Thank You for Attention!
Слайды презентации

Слайд 2 Neuroleptics (Antipsychotic Drugs)

Neuroleptics (Antipsychotic Drugs)

Слайд 3 MECHANISM OF ACTION: blockade of dopamine D2-receptors IN PERIPHERY

MECHANISM OF ACTION: 		blockade of dopamine D2-receptors IN PERIPHERY : BLOCK

: BLOCK : M - Cholinoreceptors α - Adrenoreceptors

H1- Histamine Receptors Serotonin (5-HT) Receptors DIRECT SPASMOLYTIC ACTION

Слайд 4 Pharmacological Effects:
Antipsychotic Actions:
⇓ Hallucination and Agitation
Antiemetic Effects
Extrapyramidal

Pharmacological Effects:Antipsychotic Actions: 		⇓ Hallucination and AgitationAntiemetic EffectsExtrapyramidal Effects: 	D2-Rs blockade

Effects:
D2-Rs blockade in the Nigrostriatal Pathways => =>

Parkinsonian Symptoms
Anti-muscarinic Effects:
Blurred Vision, Dry Mouth, Sedation, Confusion, Inhibition of GIT and Urinary Smooth Muscles

Слайд 7 Extrapyramidal Еffects:
due to Blocking of D2 receptors

Extrapyramidal Еffects: due to Blocking of D2 receptors in the Nigrostriatal

in the Nigrostriatal Pathway:
Parkinsonian Symptoms
Akathisia (Motor

Restlessness) - the inability to sit still
because of Uncontrollable Movement
Tardive Dyskinesia: Inappropriate Postures of the Neck, Trunk, and Limbs
Malignant Neuroleptic Syndrome:
Skeletal Muscle Rigidity, Hyperthermia, Stupor





Слайд 8 Clinical Uses of Neuroleptics
1. SCHIZOPHRENIA:
Positive Symptoms

Clinical Uses of Neuroleptics 1. SCHIZOPHRENIA: Positive Symptoms of Schizophrenia :

of Schizophrenia : DELUSIONS, HALLUCINATIONS and THOUGHT DISORDERS
Negative Symptoms

of Schizophrenia: withdrawal,
blunted emotions, reduced ability to relate to people

2. PREVENTION OF SEVERE NAUSEA and VOMITING: Drug-induced nausea
3. OTHER USES: treatment of DRUG ADDICTION, NEUROLEPTANESTHESIA, hypertensive crises

Слайд 9 Aminazine (Chlorpromazine) -
blocks CNS D2 receptors
α-Recetor

Aminazine (Chlorpromazine) - 					blocks CNS D2 receptors α-Recetor and GANGLIONIC BLOCKADE

and GANGLIONIC BLOCKADE
? HISTAMINE- and SEROTONIN -mediated

activity.
It has great:
Sedative,
Hypotensive,
Antiallergic,
Anticonvulsant activity
It may produce Galactorrhea (excessive production of milk – due to ?Prolactin release )
Clinical uses: Schizophrenia,
Acute Psychosis in Severely Agitated Patients

Слайд 10 DROPERIDOL amp. 0.25%-10 ml –
a BUTYROPHENONE derivative,

DROPERIDOL amp. 0.25%-10 ml – 				a BUTYROPHENONE derivative, more potent and

more potent and to have fewer autonomic effects than

other typical neuroleptics.
It blocks subcortical D2 and α-adrenergic receptors, and blocks CNS receptors at the CTZ.
It has no CholinoBlock action.
The drug produces marked sedation and has an antiemetic effect.
IM injection: Sedation begins in 3-10 min,
peaks at 30 min, and lasts for 2-4 hrs.
CLINICAL USE: a drug of choice at

NEUROLEPTANESTHESIA –the combination of neuroleptics with opioid analgesics, FENTANYL.
Anesthetic Premedication,
Maintenance of General Anesthesia.

Слайд 11 Lithium Salts Lithium Carbonate – Caps. 0.15 and 0.3

Lithium Salts Lithium Carbonate – Caps. 0.15 and 0.3 g; Tab.

g; Tab. 0.3 g Lithium Citrate – Syrup – 300

mg/5 ml (6% Syrup )

“Anti-Manic” drugs, also considered as “mood-stabilizing” agents because of their primary action of preventing
MOOD SWINGS in patients with
Bipolar Affective (Manic-Depressive) Disorder.
Antimanic Action: antipsychotic and antimanic effects -
by competing with other cations for exchange at
the Na+/ K+ ion pump, thus altering cation exchange
at the tissue level.
? Noradrenaline and Dopamine turnover


Слайд 12 CLINICAL USES
Bipolar Affective Disorders
Major Depression
Schizoaffective Disorder
Alcohol

CLINICAL USESBipolar Affective DisordersMajor Depression Schizoaffective Disorder Alcohol DependenceADVERSE EFFECTSPsychomotor retardation

Dependence


ADVERSE EFFECTS
Psychomotor retardation
Lethargy
Epileptiform seizures
Impaired Speech
Muscle Weakness
Arrhythmias
HYPOTENSION

Dry Mouth
Nausea,

Vomiting
Polyuria
Leukocytosis
Hypothyroidism

Слайд 13 TRANQUILIZERS (ANXIOLYTIC DRUGS)
   I. Benzodiazepines (BZDs):
Diazepam (Sibazon )

TRANQUILIZERS (ANXIOLYTIC DRUGS)   I. Benzodiazepines (BZDs):		Diazepam (Sibazon ) – amp. 0.5%-2

– amp. 0.5%-2 ml; Tab. 0.005 g
Chlordiazepoxide (Chlozepide) –

Tab. 0.005 g
Nozepam (Oxazepam, Tazepam) – Tab. 0.01 g
Lorazepam – Tab. 1 and 2 mg
Phenasepam – Tab 0.5 and 1 mg
Alprazolam (Xanax) – Tab. 0.25 and 0.5 mg
Mezapam (Rudotel) – Tab. 10 mg
Tofizopam (Grandaxin) – Tab. 50 mg
II.   Other Anxiolytics
Buspirone – Tab. 5 and 10 mg
Amyzyl – Tab. 1 and 2 mg
Hydroxyzine – amp. 5%-2 ml; Tab. 10 and 25 mg

Слайд 14 BENZODIAZEPINES according to their Duration of Action:
1. Long-acting

BENZODIAZEPINES  according to their Duration of Action:1. Long-acting (24-48 hours):			Diazepam 			Phenasepam

(24-48 hours):
Diazepam
Phenasepam
Chlordiazepoxide
2. Intermediate-acting (6-24 hours):
Alprazolam
Nozepam
Lorazepam
3.

Short-acting (< 6 hours):
Midazolam (Dormicum)
Gidazepam

Слайд 16 MECHANISM OF ACTION of BZDs:

Bind to the α-subunit

MECHANISM OF ACTION of BZDs:Bind to the α-subunit of the GABAA

of the GABAA Rs
surrounding the Cl ¯ channels
designated

as BZD Rs (omega-Receptors)
► ? Affinity of GABA Rs
► ? Frequency of Cl ¯ channel opening
► ? Cl ¯ Conductance => Hyperpolarization
=> Post-synaptic Potential away from
its Firing Threshold =>
►Inhibition of Action Potential Formation and
Further Neuronal Firing

Слайд 18 CLINICAL USES of BZDs
1.ANXIETY and PANIC DISORDERS
2. MUSCULAR

CLINICAL USES of BZDs1.ANXIETY and PANIC DISORDERS2. MUSCULAR DISORDERS: 	DIAZEPAM –

DISORDERS:
DIAZEPAM –
⮟ Skeletal Muscle SPASMS in Muscle

Strain
⮟ SPASTICITY from degenerative disorders,
such as Multiple Sclerosis
3. SEIZURES:
CLONAZEPAM – Epilepsy
DIAZEPAM – Grand Mal Epileptic Seizures
Status Epilepticus
CHLORDIAZEPOXIDE, DIAZEPAM,
NOZEPAM (OXAZEPAM) – Alcohol Withdrawal
4. SLEEP DISORDERS

Слайд 19 Psychological and Physical Dependence - if high

Psychological and Physical Dependence -  if high doses are given

doses are given over a prolonged period
ADVERSE EFFECTS of

BZDs:

DROWSINESS
CONFUSION
ATAXIA
COGNITIVE IMPAIRMENT:
? LONG-TERM RECALL
? ACQUISITION of NEW KNOWLEDGE
Early Morning Insomnia
Daytime anxiety with AMNESIA and CONFUSION


Слайд 20 BZD Antagonist:
FLUMAZENIL –
a GABA receptor

BZD Antagonist: FLUMAZENIL – a GABA receptor competitive antagonist that can

competitive antagonist that can rapidly reverse the effects of

BENZODIAZEPINES.
Blocks actions of BZDs
(and imidazopyridines) but does not antagonize the CNS effects of other sedative-hypnotic, ethanol, opioid, or
general anesthetics

Слайд 21
DIAZEPAM (Sibazon) amp. 0.5%-2 ml; Tab. 0.005 g

DIAZEPAM (Sibazon) amp. 0.5%-2 ml; Tab. 0.005 g 	is a Tranquilizer,


is a Tranquilizer, a LONG ACTING BENZODIAZEPINE
MECHANISM OF ACTION:

binds to BDZ receptors, which are separate from but adjacent to the GABA receptors, trigger an opening of a Cl- channel =>
=> ? in Cl- Conductance =>
=>HYPERPOLARIZATION that moves the postsynaptic potential away from its firing threshold and inhibits
the Formation of Action Potentials.
PHARMACOLOGIC EFFECTS: ? anxiety, sedative and hypnotic action, anticonvulsunt and myorelaxant action.
CLINICAL USES: neurotic and neurosis-like conditions with symptoms of anxiety and phobia, increased irritability; epilepsy and status epilepticus, alcohol withdrawal, muscle spasm, as adjunct to anesthesia and endoscopic procedures.

Слайд 22 Gidazepam Tab. 0.02 g; 0.05 g –
DAY

Gidazepam Tab. 0.02 g; 0.05 g – 	DAY TRANQUILIZER – has

TRANQUILIZER – has ACTIVATING EFFECT
a SHORT ACTING BZD

with anxiolytic, anticonvulsive and weakly expressed myorelaxant action.
It also stabilizes the functions of the Vegetative NS.
MECHANISM OF ACTION:
? the effect of the GABA in the ASCENDING RETICULAR ACTIVATING SYSTEM,=> increases inhibition and
blocks cortical and limbic arousal.
INDICATIONS:
Neurotic and Neurosis-like conditions with symptoms of anxiety and phobia, increased irritability; Acute alcohol withdrawal, Muscle spasm,
Convulsive disorders.

Слайд 23 Busbirone - Tab. 10 mg - an non-BZD

Busbirone - Tab. 10 mg - an non-BZD anxiolyticMECHANISM OF ACTION:⮟ Blocks

anxiolytic
MECHANISM OF ACTION:
⮟ Blocks 5-HT1A Serotonin receptors and
presynaptic Dopamine receptors

? Norepinephrine biotransformation

=> Indirect effect on BZD-GABA-CHLORINE receptor complex or GABA receptors
=> has no anticonvulsant or muscle relaxant activity and does not appear to cause physical dependence
The drug is 95% protein-bound;
onset of therapeutic effect may require 1 - 2 weeks.
INDICATIONS:
Anxiety disorders, major depression,
parkinsonian syndrome, premenstrual syndrome,
drug addiction.

Слайд 24 Sedative Drugs:
1. BROMINE SALTS:
Sodium Bromide - NaBr
Potassium

Sedative Drugs:1. BROMINE SALTS:	Sodium Bromide - NaBr	 Potassium Bromide - KBr2.

Bromide - KBr
2. VALERIAN’S PREPARATIONS:
(Valeriana officinalis)
Infusion, Tincture, Extract

from
Rhizome and Root of VALERIAN

3. MOTHERWORT’S PREPARATIONS:
(Leonurus cardiaca)
Tincture from Plant Grass
(Tinctura Leonuri)
Mechanism of Action:
⮟ Intensification of slowdown processes in the brain
Clinical Uses: Neurosis
Adverse Efects: Skin Rashes, Sedation,
Behavioral Changes.

Слайд 25 BROMISM – chronic intoxication with BROM salts.
Bromides eliminate

BROMISM – chronic intoxication with BROM salts.Bromides eliminate slowly (T1/2=12 days),

slowly (T1/2=12 days),
MANIFESTATION: total retardation, apathy,
memory disorders,

skin rashes
The IRRITATIVE ACTION of bromides induces
Mucous Inflammations along with
COUGH, RHINITIS, CONJUNCTIVITIS, DIARRHEA.

TREATMENT: the drug should be discontinued and its elimination must be accelerated.
Bromide excretion may be enhanced by using of :
Sodium Chloride, NaCl
abundant drinking, and diuretics (saluretics).

Слайд 26 Valerian’s and Motherwort’s Preparations -
are widely

Valerian’s and Motherwort’s Preparations - are widely used sedative drugs.

used sedative drugs.
VALERIAN’S preparations - Infusion, Tincture, Extract


are produced from Rhizome and Root of
VALERIANA OFFICINALIS which contain:
valerian acid, organic acids, alkaloids,
tannic substances
MOTHERWORT’S PREPARATIONS - Infusion and Tincture from plant Grass - contain:
ether oils, alkaloids, saponins, tannic substances.
SEDATIVE and WEAK TRANQUILIZING EFFECTS
do not cause myorelaxation, ataxia, psyhologic and physical dependence.
CLINICAL USES: Light Neurosis,
Somatic Diseases with Neurotic Syndrome
ADVERSE EFFECTS: Allergic Reactions.

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