Chemical structure of the tricyclic antidepressant
amitriptyline.
Tricyclic antidepressants (abbreviation TCA) are a class of antidepressant drugs first used in the 1950s. They are named after the drugs' molecular structure, which contains three rings of atoms (compare
tetracyclic antidepressant).
Example compounds
The first tricyclic antidepressant discovered was imipramine, which was discovered
accidentally in a search for a new antipsychotic in the late 1950s.
Antidepressant drugs in the tricyclic drug group (along with their actions as listed in MeSH) include:
| Name |
Brand |
Adrenergic uptake inhibitor |
Serotonin uptake inhibitors |
Dopamine antagonist |
Histamine antagonist |
| amitriptyline (& butriptyline) |
Elavil, Endep, Tryptanol, Trepiline |
yes |
|
|
|
| amoxapine |
Asendin, Asendis, Defanyl, Demolox, Moxadil |
yes |
yes |
metabolite |
|
| clomipramine |
Anafranil |
|
yes |
|
|
| desipramine |
Norpramin, Pertofrane |
yes |
|
|
|
| dothiepin hydrochloride |
Prothiaden, Thaden |
yes |
|
|
|
| doxepin |
Adapin, Sinequan |
yes |
|
|
yes |
| imipramine (& dibenzepin) |
Tofranil |
yes |
|
|
|
| iprindole |
- |
yes |
|
|
|
| lofepramine |
Gamanil |
yes |
|
|
|
| nortriptyline |
Pamelor |
yes |
|
|
|
| opipramol |
Opipramol-neuraxpharm, Insidon |
yes |
|
|
|
| protriptyline |
Vivactil |
yes |
|
|
|
| trimipramine |
Surmontil |
yes |
|
|
|
Note: Other sources suggest that most of the tricyclics combine adrenergic and serotonergic effects to some degree.
This is often reported as selectivity ratios. Some of the above, in order from most selective for nor-epinephrine to most
selective for serotonin: lofepramine, nortriptyline, amitriptyline, imipramine, clomipramine[1].
Amine classification
Tricyclics are sometimes classified as tertiary amines and secondary amines. In general, the
tertiary amines boost serotonin as well as nor-epinephrine (adrenergic) and produce more sedation, anticholinergic effects, and
orthostatic hypertension.[2] The secondary amines act
primarily on nor-epinephrine and tend to have a lower side-effect profile[3].
Tertiary amines include: amitriptyline, imipramine, trimipramine, doxepin, clomipramine, and lofepramine.
Secondary amines include: nortriptyline, desipramine, protriptyline, and amoxapine.
Mechanism of action
The exact mechanism of action is not well understood, however it is generally
thought that tricyclic antidepressants work by inhibiting the re-uptake of the neurotransmitters norepinephrine, dopamine, or serotonin by nerve cells.
Tricyclics may also possess an affinity for muscarinic and histamine H1 receptors to varying degrees. Although the
pharmacologic effect occurs immediately, often the patient's symptoms do not respond for 2
to 4 weeks.[4] Although norepinephrine and
dopamine are generally considered stimulatory neurotransmitters, tricyclic antidepressants also
increase the effects H1 histamine, and thus most have sedative effects.[5]
Chemistry of re-uptake inhibitors
The chemical action of re-uptake inhibitors in general was unknown for a long time. In August 2007, two research groups
independently reported that the tricyclic molecule docks to the transporter protein in a cavity adjacent to where the
neurotransmitter substrate binds, locking the substrate in place and thereby
obstructing re-uptake transport.[6]
Clinical use
Tricyclic antidepressants are used in numerous applications; mainly indicated for the treatment of clinical depression, neuropathic pain,
nocturnal enuresis, and ADHD, but they have also been used successfully for headache (including migraine headache), anxiety, insomnia, smoking
cessation, bulimia nervosa, irritable
bowel syndrome, narcolepsy, pathological crying or
laughing, persistent hiccups, interstitial
cystitis, and ciguatera poisoning, and as an adjunct in schizophrenia.[4]
Depression
For many years they were the first choice for pharmacological treatment of depression. Although still considered effective,
they have been increasingly replaced by SSRIs and other newer
drugs. Newer antidepressants are thought to have fewer side effects and are also
thought to be less effective if used in a suicide attempt, as the treatment and lethal doses
(see therapeutic index) are farther apart than with the tricyclic antidepressants.
Tricyclic antidepressants are sometimes still used to treat refractory depression
that has failed to respond to standard SSRI therapy.[7] They are not considered addictive and are preferable to the MAOIs. Side effects usually occur before depression is effectively suppressed; for this
reason and via other mechanisms they can be dangerous, as volition may be
increased, giving the patient greater ability to attempt suicide.[8]
ADHD
Tricyclic antidepressants have been shown to be effective in treating attention-deficit hyperactivity disorder.[9] ADHD is thought to be caused by dopamine and norepinephrine shortages in the brain's prefrontal cortex.
Tricyclic antidepressants block the reuptake of these neurotransmitters, thus acting as dopamine and norepinephrine
agonists.[10] They are commonly used in patients for whom psychostimulants (the primary
medication for ADHD) are ineffective or contraindicted. TCAs are more effective in treating the behavioral aspects of ADHD than
the cognitive deficits; they help limit hyperactivity and impulsivity but have little effect on attention.[11]
Analgesia
Tricyclics are also known as effective analgesics for different types of pain, especially
neuropathic or neuralgic pain (like back pain in radiculitis).[12][13] A precise mechanism for their analgesic action is unknown, but it is thought that they
modulate opioid systems in the CNS via an
indirect serotonergic route.[14] Typically pain modification requires lower dosages than for treating depression
(e.g. Amitriptyline at 10 to 30 mg rather than 75 to 150 mg). They are also effective in migraine prophylaxis, but not in relief of an acute migraine attack. This is also believed to be related to
serotonergic effects. There is, however, little evidence for an analgesic effect in acute pain.[4]
Nocturnal enuresis
Tricyclics with greater anti-muscarinic action (i.e., amitriptyline, imipramine and nortriptyline) may prove useful in helping to treat nocturnal enuresis
(bedwetting) in children over the age of 7 years. The drug needs to be gradually withdrawn and the total treatment period is
advised to be no greater than 3 months at a time. It is thought that the anticholinergic effects of tricyclics may inhibit
urination, and/or the CNS stimulant effect may lead to easier arousal when the stimulus of a full bladder occurs.[15] However, one robust review of
tricyclics for the treatment of enuresis found the benefits of tricyclics were relatively small and transient and due to
potentially serious adverse effects suggested more research into other methods (bedwetting
alarms, behavioural methods, desmopressin) which may be better suited for treatment
of this condition.[16]
Side effects
Many side effects are related to tricyclics antimuscarinic actions. The
antimuscarinic side effects are relatively common and include:
- Dry mouth (salivary secretion is affected)
- Dry nose
- Blurred vision (accommodation in the eye is affected)
- Decreased gastro-intestinal motility and secretion. This may lead to constipation
- Urinary retention or difficulty with urination
- Hyperthermia
Tolerance to these adverse effects often develops if treatment is continued, side effects may also be less troublesome if
treatment is initiated with low dose and then gradually increased, although this may delay the clinical effect.
Other side effects may include drowsiness, anxiety, restlessness, cognitive and
memory difficulties, confusion, dizziness,
akathisia, hypersensitivity reactions, increased
appetite with weight gain, sweating, decrease in sexual ability and desire, muscle twitches,
weakness, nausea and vomiting, hypotension, tachycardia, and rarely, irregular heart rhythms.[4] Rhabdomyolysis or
muscle breakdown has been rarely reported with this class of drugs. [1]
Interactions
TCAs are highly metabolized by the cytochrome P450 hepatic enzymes. Drugs that
inhibit cytochrome P450 (for example cimetidine,
methylphenidate, antipsychotics, and calcium
channel blockers) may produce decreases in the tricyclic's metabolism leading to increases in tricyclic blood
concentrations and accompanying toxicity. Drugs which prolong the QT interval including
antiarrythmics such as quinidine, the antihistamines astemizole and terfenadine, and some antipsychotics may increase the chance of ventricular dysrhythmias. TCAs may enhance the response to
alcohol and the effects of barbiturates and other CNS depressants. Side effects may also be enhanced by other drugs which have
antimuscarinic properties.[4]
Overdose
Tricyclic antidepressant overdose is a significant cause of fatal drug poisoning. The severe morbidity and mortality associated
with these drugs is well documented and due to their cardiovascular and
neurological toxicity. Additionally, they are a serious problem in the pediatric population
due to their inherent toxicity[17] and the availability of these in the home when prescribed for bed wetting and
depression.
Symptoms
The central nervous system and heart are the
two main systems that are affected. Initial or mild symptoms include drowsiness, a dry mouth,
nausea, and vomiting. More severe complications, include
hypotension, cardiac rhythm disturbances, hallucinations, and seizures. Electrocardiogram (ECG) abnormalities are frequent and a wide variety of cardiac dysrhythmias can occur, the most common being sinus tachycardia and intraventricular
conduction delay (QRS prolongation).[18] Seizures and cardiac dysrhythmias are the most important life threatening
complications.
Toxicity
Tricyclics have a narrow therapeutic index, i.e. the therapeutic dose is close to the toxic dose. In the medical literature the lowest reported toxic dose is 6.7 mg per kg
body weight, ingestions of 10 to 20 mg per kilogram of body weight are a risk for moderate to severe poisoning, although doses
ranging from 1.5 to 5 mg/kg may even present a risk. Most poison control centers
refer any case of TCA poisoning (especially in children) to a hospital for monitoring.[19] Factors that increase the risk of toxicity include
advancing age, cardiac status, and concomitant use of other drugs.[20] Serum drug levels are not useful in tricyclic
overdose.[21]
Toxic mechanism
Most of the toxic effects of TCAs are caused by four major pharmacological effects. TCAs have anticholinergic effects, cause excessive blockade of norepinephrine reuptake at the postganglionic synapse, direct alpha
adrenergic blockade, and importantly they block sodium membrane channels with slowing of membrane depolarization, thus having
quinidine like effects on the myocardium.[22]
Treatment
Initial treatment of an acute overdose includes gastric decontamination of the patient. This is achieved by administering
activated charcoal which adsorbs the drug in the
gastrointestinal tract either orally or via a nasogastric tube. Other decontamination methods such as stomach
pumps, ipecac induced emesis, or whole
bowel irrigation are not recommended in TCA poisoning.[23][24]
Symptomatic patients are usually monitored in an intensive care unit for a minimum of 12 hours, with close attention paid to
maintenance of the airways, along with monitoring of blood pressure, arterial pH, and continuous ECG monitoring.[22] Supportive therapy is
given if necessary, including respiratory assistance, maintenance of body temperature, and administration of sodium bicarbonate as an antidote. Sodium bicarbonate is given
intravenously and it has been shown to be an effective treatment for resolving the
metabolic acidosis and cardiovascular complications of TCA poisoning. If sodium
bicarbonate therapy fails to improve cardiac symptoms, conventional antidysrhythmic drugs such as phenytoin and magnesium can be used to reverse any cardiac abnormalities.
However, no benefit has been shown from lidocaine or other class 1a and 1c antiarrhythmic
drugs; it appears they worsen the sodium channel blockade, slow conduction velocity, and depress contractility and should be
avoided in TCA poisoning.[25] Hypotension is initially treated with fluids along with bicarbonate to
reverse metabolic acidosis (if present), if the patient remains hypotensive despite
fluids then further measures such as the administration of epinephrine, norepinephrine, or dopamine can be used to increase blood
pressure.[25] Another potentially severe symptom is seizures; often seizures resolve
without treatment but administration of a benzodiazepine or other anticonvulsive may be
required for persistent muscular overactivity. There is no role for physostigmine in the
treatment of tricyclic toxicity as it may increase cardiac toxicity and cause seizures.[22]
Tricyclic antidepressants are highly protein bound and have a large volume of
distribution; therefore removal of these compounds from the blood with hemodialysis,
hemoperfusion or other techniques are unlikely to be of any significant benefit.[24]
Epidemiology
Studies in the 1990s in Australia and the United
Kingdom showed that between 8 and 12% of drug overdoses were following TCA ingestion. TCAs may be involved in up to 33% of
all fatal poisonings, second only to analgesics.[26][27]
Development history
Tricyclic antidepressants were developed amid the "explosive birth" of psychopharmacology in the early 1950s. The story begins
with the synthesis of Chlorpromazine in December 1950 by Rhône-Poulenc's chief chemist, Paul Charpentier, from synthetic
antihistamines developed by Rhône-Poulenc in the 1940s.[28] Its psychiatric effects were first noticed at a hospital in Paris in 1952. The
first widely-used psychiatric drug, by 1955 it was already generating significant revenue as an antipsychotic.[29] Research chemists
quickly began to explore other derivatives of chlorpromazine.
The first TCA reported for the treatment of depression was imipramine, an imino-dibenzyl
analogue of chlorpromazine code-named G22355. It was not originally targeted for the treatment of depression. The drug's tendency
to induce manic effects was "later described as 'in some patients, quite disastrous'". The paradoxical observation of a sedative
inducing mania lead to testing with depressed patients. The first trial of imipramine took place in 1955 and the first report of
antidepressant effects was published by Swiss psychiatrist Ronald Kuhn in 1957.[30] Some testing of Geigy’s imipramine, then known as Tofranil,
took place at the Münsterlingen Hospital near Konstanz.[31] Geigy later became Ceiba-Geigy and eventually Novartis.
Many patents were filed in the 1950s and 1960s concerning variations on these three-ring structures with applications to
psychiatric conditions.
- Phenothiazine derivatives are described in U.S. patent 2,591,679 issued 1952-04-08 to John W. Cusic. The compounds described contain a sulphur group on the central carbon ring, and
a nitrogen atom in the cental ring to which the side chain attaches, in the manner of chlorpromazine. Most of the illustrated
side chains contain an amine group.
Merck introduced the second member of the TCA family, amitriptyline (Elavil), in
1961.[32]
These patents cover the structures of the compounds and their mode of chemical synthesis. Understanding of their mode of
action as re-uptake inhibitors and development of the serotonin theory of depression came in the years to follow.
References
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- ^ (2005) in McEvoy GK: AHFS drug information. American Society of Health-System Pharmacists. ISBN
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See also
External links
|
Psychoanaleptics: antidepressants (N06A) |
| MAOIs |
Harmaline • Iproniazid • Isocarboxazid • Nialamide • Pargyline • Phenelzine •
Selegiline • Toloxatone • Tranylcypromine • Rasagiline
RIMAs: Brofaromine • Beta-carbolines • Moclobemide |
| RIs |
| S RI |
SS RI (Alaproclate, Citalopram, Dapoxetine,
Escitalopram, Etoperidone, Fluoxetine, Fluvoxamine, Paroxetine,
Sertraline, Zimelidine) • TCAs/Tetras (Clomipramine, Nefazodone, Trazodone) |
| N RI / A RI |
Atomoxetine • Maprotiline • Reboxetine • Viloxazine • TCAs/Tetras (Amitriptyline, Amoxapine, Butriptyline, Desipramine/Lofepramine, Dibenzepin, Dothiepin, Doxepin, Imipramine, Iprindole,
Melitracen, Nortriptyline, Opipramol, Protriptyline, Trimipramine, Maprotiline) |
| D RI |
Vanoxerine • Phenmetrazine • TCAs (Amineptine) |
| SN RI |
Desvenlafaxine • Duloxetine • Milnacipran • Nefazodone • Venlafaxine |
| ND RI |
Bupropion |
| SND RI |
Brasofensine • Tesofensine • Nomifensine |
|
| SSREs |
Tianeptine |
| AAs |
Tetras (Mianserin, Mirtazapine) |
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