DEPRESSIVEILLNESSES ANDANTIDEPRESSANTS 119Imipramineandamitriptyline(tertiary amines) have more
powerful anticholinergic and cardiac toxic effects than second-
ary amines (e.g. nortriptyline).
Mechanism of action
The tricyclics block uptake-1 of monoamines into cerebral (and
other) neurones. Thus, the concentration of amines in the
synaptic cleft rises. As discussed above, they may also induce a
slow adaptive decrease in pre- and/or postsynaptic amine
receptor sensitivity.
Adverse effects
Autonomic (anticholinergic)/cardiovascularDry mouth,
constipation (rarely paralytic ileus, gastroparesis),
tachycardia, paralysis of accommodation, aggravation of
narrow-angle glaucoma, retention of urine, dry skin due
to loss of sweating, and (due to α-blockade) postural
hypotension. Rarely, sudden death due to a cardiac
dysrhythmia. In overdose, a range of tachydysrhythmias
and intracardiac blocks may be produced.
Central nervous systemFine tremor and sedation, but also
(paradoxically) sometimes insomnia, decreased rapid eye
movement (REM) sleep, twitching, convulsions, dysarthria,
paraesthesia, ataxia. Increased appetite and weight gain,
particularly with the sedative tricyclics, are common. On
withdrawal of the drug, there may be gastro-intestinal
symptoms such as nausea and vomiting, headache,
giddiness, shivering and insomnia. Sometimes anxiety,
agitation and restlessness follow sudden withdrawal.Allergic and idiosyncratic reactionsThese include bone marrow
suppression and jaundice (both rare).HyponatraemiaHyponatraemia is an adverse effect due to
inappropriate ADH secretion, and is more common in the
elderly.Contraindications
These include the following:- epilepsy;
- recent myocardial infarction, heart block;
- mania;
- porphyria.
RELATED NON-TRICYCLIC ANTIDEPRESSANT DRUGS
This is a mixed group which includes 1-, 2- and 4-ring struc-
tured drugs with broadly similar properties. Characteristics of
specific drugs are summarized below.Maprotiline– sedative, with less antimuscarinic effects, but
rashes are more common and fits are a significant risk.
Mianserin– blocks central α 2 -adrenoceptors. It is sedative,
with much fewer anticholinergic effects, but can cause
postural hypotension and blood dyscrasias, particularly in
the elderly. Full blood count must be monitored.Assess risk factors for
treatment resistanceAssess symptom severityPartial response to
first-line treatmentAdvance dose
as toleratedSymptoms persist after
6–8 weeksEnsure safe maximum
tolerated doseTrial of an alternative
medicationNonresponders:
mild-to-moderate
symptoms, low riskAll patients:
moderate-to-severe
symptoms, or high riskNo response to
first-line treatmentPersistent symptoms AUGMENTATION* Persistent symptomsTrial of an alternative
medicationPartial responders:
mild symptoms, low riskFigure 20.2:General algorithm for
the second phase of treatment of
depression. Augmentation*
involves the use of a combination
of medications to enhance the
efficacy of an antidepressant.
(Redrawn with permission from
Aronson SC and Ayres VE,
‘Depression: A Treatment
Algorithm for the Family
Physician’,Hospital Physician
Vol 36 No 7, 2000. Copyright
2000 Turner White
Communications, Inc.)