96 Section 2/ Drugs Acting on CNSPHENOTHIAZINESPHARMACOLOGICAL ACTIONS
a. Action on CNS: Effects differ in nor-
mal and psychotic individuals.
- Sedation: They produce sedation
which does not progress to anaesthesia.
They decrease the agitation, anxiety and
aggressiveness in psychotic patient without
affecting wakefulness. - Antipsychotic effect: In schizophrenic
patients, they improve thought disorders,
blunted affect, withdrawal and self centered
behaviour. They also improve the halluci-
nations and delusions.
They produce neuroleptic syndrome
which consists of motor retardation and
emotional quietening.
In animal studies, they reduce the spon-
taneous motor activity and produce cata-
lepsy (state of rigidity and immobility).
- Action on CTZ: Chlorpromazine de-
presses the chemoreceptor trigger zone
(CTZ) and acts as a powerful antiemetic
agent. - Effect on hypothalamus: They produce
hypothermia by acting on temperature
regulating centre. They also produce
central sympathoplegia resulting in
miosis and failure in ejaculation.
They produce parkinsonism like reac-
tion by increasing the spontaneous firing of
dopaminergic neurons of basal ganglia.
b. Effect on CVS: Chlorpromazine may
produce orthostatic hypotension prob-
ably due to inhibition of centrally me-
diated pressor reflexes. It also causes
prolongation of QT interval in ECG.c. Effect on endocrine system: They can
produce amenorrhoea and galactor-
rhoea due to increase in serum prolac-
tin level in females. It also blocks the
release of growth hormone, ADH and
gonadotrophin secretion.
d. Local anaesthetic: Chlorpromazine has
a potent local anaesthetic action.
e. ANS: They have varying degree of a
adrenergic blocking activity. They also
have weak anti-cholinergic, H 1 -
antihistaminic and anti 5-HT actions as
well.
They also cause blockade of postsynap-
tic monoaminergic (including 5-HT, norad-
renaline and dopamine) transmission in the
brain resulting in decrease in central sym-
pathetic activity.Pharmacokinetics
Phenothiazines are well absorbed after
oral and parenteral administration. They are
distributed in all the body tissues and
metabolised in liver by hydroxylation and
glucuronide conjugation and demethylation.
The metabolites are excreted in urine and bile
for long period of time even after discontinu-
ing the drug.Adverse Reactions
CNS side effects include lethargy,
drowsiness, increase in REM sleep, restless-
ness, excitement and impaired psychomo-
tor functions.
The other side effects include epileptic
seizures, disturbances in body temperature
regulation. ANS side effects include tachy-
cardia, difficulty in micturition, inhibition
of ejaculation, postural hypotension,
blurring of vision (with thioridazine), con-
stipation, nasal stuffiness etc.