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Class antipsychotics
1. Dr. RAGHU PRASADA M S
MBBS,MD
ASSISTANT PROFESSOR
DEPT. OF PHARMACOLOGY
SSIMS & RC.
1
2. The most important types of psychosis are:
Schizophrenia
Affective disorders (e.g. depression, mania)
Organic psychoses (mental disturbances caused by
head injury, alcoholism, or other kinds of organic
disease).
3. PET studies
Post-mortem studies
Drugs increasing central dopamine activity- L-dopa,
amphetamines
Excessive dopaminergic activity plays a role in the
disorder.
The enhancement of function of 5-HT2
Pharmacologically, they are characterized as dopamine
receptor antagonists, though many of them also act on
other targets, particularly 5-HT receptors, which may
contribute to their clinical efficacy.
4. LSD- 5HT2 agonist –
Visual hallucinations
5-HT has a modulatory effect on dopaminergic
neurones
Glutamate hypothesis
Phencyclidine, ketamine
Glutamate-NMDA antagonists –can produce psychotic
symptoms
5. The nigrostriatal pathway (coordination of voluntary
movement
Mesolimbic- mesocortical ( behavior )
Tuberoinfundibular- pituitary system (endocrine)
The medulla oblongata (vomit)
Medullary - periventricular pathway ( eating
behavior)
6. Positive Symptoms-mesolimbic.
Hallucinations, delusions, paranoia, ideas of
reference.
Negative Symptoms-mesocortical
Apathy, social withdrawal, anhedonia, emotional
blunting, cognitive deficits, extreme inattentiveness
or lack of motivation to interact with the
environment.
These symptoms are progressive and non-responsive
to medication.
7. DOPAMINE RECEPTORS
There are at least 5 subtypes of receptors:
D1 and D5: mostly involved in postsynaptic
inhibition.
D2, D3, and D4: involved in both pre-and
postsynaptic inhibition.
D2: the predominant subtype in the brain:
regulates mood, emotional stability in the limbic
system and movement control in the basal ganglia.
8.
9. Presynaptic Effects
Blockade of D2 receptors
Compensatory Effects
Firing rate and
activity of
nigrostriatal and
mesolimbic DA
neurons.
DA synthesis, DA
metabolism, DA
release.
Postsynaptic Effects
Depolarization Blockade
Inactivation of nigrostriatal
and mesolimbic DA
neurons.
Receptor Supersensitivity
Prolonged use-feedback
inhibition of dopamine
releasedecreased
dopamine turnover
12. Pharmacologic effects and mechanism:
CNS: A. Neuroleptic Effect-Antipsychotic drugs probably
owe their therapeutic effects mainly to blockade of D2-
receptors (lies in midbrain-cortex and midbrain-limbic
system ) Mesolimbic,mesocortical D2
More effective for treating positive symptom
B. Antiemetic Effect--- inhibit chemoreceptor trigger zone or
directly depress the medullary vomiting center.
C. Temperature-regulating Effect--- produce hypothermia
13. Pharmacologic effects:
(2) Autonomic Nervous System: block α-adrenergic
and M-Cholinergic receptors and result in
hypotension, dry mouth, constipation and blurred
vision.
(3) Endocrine system: increase the release of
prolactin and decrease corticotropin release and
secretion of pituitary growth hormone.
17. Unique receptor affinity
Clozapine: D4 = 1>5-HT2 = M>D2 = D1 = 2;H1, low
incidence of EPS, low sedation, no gynacomastia
Quetiapine: 5-HT2 = D2 = 1 = 2; H1
drowsiness and
postural hypotension
Risperidone: 5-HT2 >>1 >H1 >D2 >2>>D1
Aripiprazole-partial agonist at D2 and 5-HT1A
5HT2A agonist- called as DA:5HT stabiliser in CNS
Has long t1/2 of 3 days
18. Sertindole –long plasma T1/2
Asenapine –sub lingually
Effective negetive > positive symptoms
Effective in patients refractory to typical neuroleptics
Less liability to cause EPS low affinity for D1 and
D2 receptors
Antagonists at 1, m, H1, D2
19.
20. Most antipsychotics are readily but incompletely
absorbed.
Significant first-pass metabolism.
Bioavailability is 25-65%.
Most are highly lipid soluble.
Most are highly protein bound (92-98%).
High volumes of distribution (>7 L/Kg).
Slow elimination.
Duration of action longer than expected, metabolites
are present and relapse occurs, weeks after
discontinuation of drug.
21. Treatment of psychotic disorders: schizophrenia,
Schizo affective disorders -mania, paranoid states,
alcoholic hallucinosis.
Drug induced psychosis
Anesthesia in hypothermia and artificial hibernation
(used with pethidine and promethazine).
Nausea ,Vomiting-CPZ
Tourettes syndrome
Huntingtons disease
Preanaesthetic medication
Intractable hiccups -CPZ
22.
23. Behavioural Effects (pseudodepression, akinesia,
confusion)
Neurological Effects (Parkinsonism, Akathisia,
Dystonia, Tardive Dyskinesia)-
Tardive dyskinesia comprises mainly involuntary
movements of face and tongue, but also of trunk
and limbs, appearing after months or years of
antipsychotic treatment. It may be associated
with proliferation of dopamine receptors
(possibly presynaptic) in corpus striatum.
24. c) Autonomic Effects (orthostatic hypotension,
impaired ejaculation)
d) Metabolic and Endocrine Effects (weight
gain, hyperprolactinemia, loss of libedo,
impotence)
e) Toxic or allergic effects (agranulocytosis,
choleostatic jaundice- clozapine)
