Anti depressant Drugs - Isfahan University of Medical Sciences
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Transcript Anti depressant Drugs - Isfahan University of Medical Sciences
Anti depressant Drugs
Rezaei M. MD
Psychiatrist
Tricyclics
Tertiary amines:
Imipiramine
Amitriptyline
Clomipramine
Trimipiramine
Doxepin
Secondary amines
Desipiramine
Nortriptyline
protriptyline
Tetracyclics
Amoxapine
Maprotiline
Minaserin
Pharmacological actions
Absorbed from oral administration
Peak plasma concentration 2-8 hrs
Half life vary from 10 to 70 hrs ( nortriptyline,
maprotiline and protriptyline may have longer half lives )
5-7 days are needed to reach steady state plasma
concentration
Metabolized in liver by cytochrome p-450 enzyme
Drug interaction with quinidine, cimetidine , fluxetine,
serteraline, paroxetine , phenothiazine, carbamazepine
Genetic variability between persons are responsible for
up to 40-fold differences in plasma concentrations of
TCA`s
Mechanism of action:
Block the reuptake of NEP and serotonin
Competitive antagonists at the muscarinic acetylcholine,
histamine H1, @1 and @2-adrenergic receptors.(
Amoxapine, nortriptyline, desipramine, maprotiline have the
least anticholinergic activity.
Doxepine has the most antihistaminergic activity,
clomipramine is the most sertonin-selective of the TCAs)
Adverse effects
Psychiatric effects
A major adverse effect is the possibility of inducing a manic episode
in patients +/- history of BMD I disorder
Anticholinergic effects
Patient may develop a tolerance for these effects with continued
treatment.
Amitriptyline
Imipramine
Doxepin
Trimipramine
Dry mouth, constipation, blurred vision , urinary retention,
Treatment
Beware of narrow angle glaucoma
Severe reactions may induce CNS anticholinergic syndrome with
confusion and delirium
Sedation
Amitriptyline
Trimipramine
Doxepin
The least sedative effects are in desipiramine and
protriptyline
Autonomic effects
Orthostatic HOTN ,Partly because of @1-adrenergic
blockade
Nortriptyline least likely cause the problem
Fludrocortisone may be helpful
Other effects include sweating , palpitation, HTN
Cardiac effects
In the usual therapeutics doses: tachycardia, flattened T
wave, prolonged QT interval, and depr essed ST segment
Because the drug prolong conduction time, their use in
patients with preexisting conduction defects is
contraindicated.
The drug should be discontinued several days before
elective surgery because of occurrence of
hypertensive episodes during surgery in patients
receiving TCAs.
Neurlogical effects
Desipramine and protriptyline are associated with
psychomotor stimulation:
Myoclonic jerks and tremors of tongue and upper extremities
Speech block
Paresthesia
Peroneal palsy
Ataxia
Amoxapine is unique in causing
Parkinsonian symptoms
Akathisia
Dyskinesia
rarely; neuroleptic malignant syndrome
Maprotiline may cause seizures if
Dose increase too quickly
Dose keep at high level for too long
Overall TCAs have relatively low risk for inducing
seizures, except in patients who are at risk for seizures.
Allergic and hematological effects
Rash in 4-5 % in maprotiline
Jaundice is rare
Agranulocytosis, leukopenia and leukocytosis are rare.
However , a patient with fever or sore throat during
the first few months of TCA treatment, should have a
CBC immediately.
Other adverse effects :
Weight gain
Impotence
Gynecomastia
Amenorrhea
Nausea
Hepatitis
Vomiting
SIADH
SSRI
Major differences between them is different
pharmacokinetics profiles
Fluoxetine has the longest half life of 2-3 days, others of
about 2o hrs.
All well absorbed orally and metabolized in the liver
Paroxetine and fluoxetine are metabolized by CYP 2D6,
be careful in coadministration of drugs with the same
enzyme metabolizer
Fluvoxamine inhibits the CYP 3A4, so interfere with
terfenadine and astemizole.
If taken with food, it reduce nausea and diarrhea.
Therapeutic indications of SSRI
Depression ; they are first line in the general population
( mild and moderate Dep. ), the elderly, the medically ill
and those who are pregnant.
Serteraline may be more effective for treatment of
severe depression with melancholia
Over 50% of persons who respond poorly to one SSRI
will respond favorably to another.
Augmentation strategies
In depressed persons with partial response :
Bupropion
Lithium
Levothyroxine
Sympathomimetics
Pindolol
Clonazepam
Suicide
Markedly reduce the risk of suicide
Depression during pregnancy
No documented adverse reaction
SSRI may produce a self limited neonatal withdrawal
syndrome that consist of jitterness and mild tachypnea, it
begins several hrs after birth and may persist for days to a
few weeks. It is rare and does not interfere with feeding.
Postpartum depression(+/- psychotic feature)
Depression in the Elderly and Medically ill
Precise diagnostic evaluation to rule out dementia and
delirium.
They are less well tolerated by persons with preexisting GI
symptoms.
Chronic depression
They have to continue taking SSRI`s for at least 1 year.
Depression in children
Children of depressed adults are at increased risk of
depression.
Adverse effects in children includes GI symptoms, insomnia,
motor restlessness, social disinhibition, and hypomania or
mania; so SSRI use with small doses.
OCD
Fluvoxamine and Serteraline are approved for treatment of
pediatric OCD
Effective dose for OCD is higher than those required for
depression.
Panic Disorders
SSRI`s are far superior to benzodiazepines for treatment of
panic disorder with depression.
Are effective for childhood panic symptoms
Social Phobia
Posttraumatic Stress Disorder
SSRI`s are more effective than TCAD and MAO`s inhibitor
Marked improvement of both intrusive and avoidant
symptoms.
Specific phobias, GAD, separation anxiety
Bulimia Nervosa and other Eating Disorder
Fluoxetine
Obesity ; fluoxetine in combination with behavioral
program
Premenstural Dysphoric Disorder
Fluoxetine and Serteraline
Adverse Reactions of SSRI`s
Sexual dysfunction: inhibited orgasm and decreased libido.
Gastrointestinal : nausea, diarrhea, vomiting, dyspepsia,
anorexia.
Weight Gain
Headaches; 18-20 %
Anxiety
Insomnia and Sedation
Vivid dreams and Nightmares
Seizures
Extrapyramidal Symptoms
Galactorrhea
Hypoglycemia , rarely hyponatremia and SIADH
Serotonin Syndrome
Concurrent administration of an SSRI with MAOI, l-
tryptophan, or lithium can rise plasma serotonin
concentration
Diarrhea
Restlessness
Agitation , hyperreflexia, autonomic instability, rapid
fluctuations of vital signs
Myoclonus , seizures, hyperthermia, rigidity,
Delirium , coma, cardiovascular collapse and death.
SSRI`s Withdrawal
Dizziness
Weakness
Nausea
Headaches
Rebound depression
Anxiety
Insomnia
Poor concentration
Upper respiratory symptoms
Paresthesia
Migranelike symptoms
BUPROPION
More effective against symptoms of depression than
those of anxiety.
Half life 12 hrs.
Blockade of dopamine reuptake
Therapeutic indications:
Depression
Bipolar Disorders
ADHD
Cocaine Detoxification
Smoking cesation
BUPROPION
Adverse reaction
Headache
Insomnia
Upper respiratory symptoms
Nausea
Restlessness
Agitation
Irritability
Weight loss 25%
Dry mouth
constipation
Trazodone
Half life is 6-11 hrs
Specific inhibitor of serotonin reuptake
Depressive Disorder
Insomnia
Venlafaxine
May have faster onset of action than other antidepressant
Most effective drugs for treatment of severe depression with
melancholic features & GAD
Half life 3.5 hrs( SR-form 9 hrs )
Inhibitor of serotonin & norepinephrine reuptake and weak
inhibitor of dopamine reuptake
Therapeutic indications
Depression
GAD
OCD
Panic
Agarophobia , social phobia, ADHD
Adverse reactions:
Nausea
Somnolence
Dry mouth
Dizziness
Constipation
Asthenia
Anxiety
Anorexia
Blurred vision
Abnormal ejaculation and orgasm
Errectile disturbance and impotence
Duloxetine
Inhibitor of serotonin and norepinephrine
MAIO Drugs
Used less frequently than others
Increase biogenic amine neurotransmitter level
There are two type of MAO : A & B
MAOA metabolize NEP, SER, EPI
MAOB metabolize DOP, TYR
Therapeutic indications:
Depression, Atypical depression
Panic
Agarophobia
PTSD
Eating Disorder
Social phobia
Pain Disorder