File - JMH Psychiatry Residency
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Antidepressants
PRITE Review
Samir Sabbag
PGY-3 Psychiatry
August 24, 2009
Overview
Goal in Depresion
Achieve complete remission
With Treatment
News – if remission: lower relapse rate
Bad News – remitters have frequent relapses
Good
Suicide rates higher at ages 18-24
All effective Antidepressants boost
DA,
5HT and NE
Monoamine(MA) Hypothesis of
Depression
MA Boost Therapeutic Action
5HT
NE
DA
5HT
NE
DA
NE
DA
5HT
NE
DA
NE
DA
5HT
5HT
NE
DA
5HT
Selective Serotonin
Reuptake Inhibitors
(SSRIs)
Available SSRIs
Fluoxetine (Prozac)
Paroxetine (Paxil)
Sertraline (Zoloft)
Citalopram (Celexa)
Escitalopram (Lexapro)
Fluvoxamine ( Luvox)
Mechanism of action
All SSRIs inhibit
reuptake of 5HT
by presynaptic
neurons
SSRI Therapeutic Indications
Depression
OCD (give higher doses)
Panic Disorder
PTSD (help with intrusive and avoidant sx)
GAD
Premenstrual Dysphoric disorder
Social Anxiety disorder
Eating disorders (Fluoxetine)
SSRI ½ lives and metabolites
Fluoxetine
Active Metabolite: 7-9 days
Sertraline
: longest ½ life
4-6 days!
: 26h
Active Metabolite: 3-5 days
No active metabolites
Citalopram
: 35h
Escitalopram : 27-32h
Paroxetine
: 21h (most likely to cause withdrawal reaction)
Fluvoxamine : 15h
SSRIs
Plasma Protein binding
Highly bound
Fluoxetine, Sertraline and Paroxetine
Least bound
Escitalopram
CYP 450
Fluvoxamine: marked
1A2, 2C and 3A
Fluoxetine
2D6
effect on CYP
and Paroxetine
Least likely to cause problems
Citalopram, Sertraline and Escitalopram
SSRIs - General Side Effects
Restlessness, psychomotor retardation, mild
parkinsonism and dystonic movements (5HT-2A in
basal ganglia)
Myoclonus, sleep disturbance and nocturnal
awakening (2A in brainstem)
Sexual dysfunction, apathy and decreased libido (2A
and 2C in spinal cord)
N/V (5HT-3 in hypothalamus and brainstem)
Increased bowel motility, GI cramps and diarrhea
(5HT3 and 4 in GI tract)
GI Sx Most common SE leading to discontinuation
SSRIs - General Side Effects
Suicide
increased
thoughts/actions in children, adolescents
and young adults <25
Closely monitor first few weeks when starting SSRI
Pregnancy
Hematologic
Small increase in anencephaly, craniosynostosis and
omphalocele (as per population registries)
Prolonged bleeding time - functional impairment of platelet
aggregation
Endocrine
Can decrease glucose concentrations acutely
SSRIs - General Side Effects
Most common SE associated with long term
treatment:
Dysfunction – continues as long as the
drug is taken
Sexual
Sleep disturbances
Extremely
vivid dreams or nightmares
Bruxism, restless legs, nocturnal myoclonus
Yawning
associated with fatigue – effect of SSRI on
hypthalamus
Not
Citalopram and Escitalopram
Most selective inhibitors of serotonin reuptake
Citalopram may have some sedative effects (H1)
Citalopram
Escitalopram
Fluoxetine
5HT2C receptor block
NE
and DA release
Increased energy
Activation/anxiety
Antibulimic/anorexic
effects
Boosts antidepressant
action of Olanzapine in
Bipolar Depression
NE reuptake blockade
Fluoxetine
Of the SSRIs, most likely to cause
headaches
Can cause anxiety, specially during 1st
weeks of use on the long run decrease
anxiety
SSRI most likely to cause insomnia
Sertraline
Atypical Depression
Overeating and oversleeping
Extreme sensitivity with
interpersonal loss or rejection
Severe psychomotor retardation
Mood reactivity
Sigma 1 action anxiolytic
weak DA and NE reuptake inhibition
Improves
energy, motivation and concentration
Helps with atypical depression
Fist line in Panic d/o (also Paroxetine)
Paroxetine
Anticholinergic (M1)
calming/sedating
Good
for anxiety sx
weak NE reuptake inhibition
antidepressant
effects
Nitric Oxide Synthetase (NOS)
and 2D6
Sexual
dysfunction
Paroxetine
Withdrawal reaction with sudden d/c
Anticholinergic
rebound
Substrate and inhibitor for 2D6
Rapid decline in plasma when d/c
First line in Panic disorder (also Zoloft)
Anticholinergic activity
Dry mouth, constipation, sedation
Paroxetine
Fetal abnormalities
Cardiac
malformation (R Ventricular outflow
obstruction)
Pulmonary hypertension
Seen with doses >25mg in 1st trimester
More frequent and pronounced weight
gain than other SSRIs
Fluvoxamine
Not normally used as antidepressant
Used for OCD, Panic d/o, PDD,
Aggression in autism
SSRI with the most DDI of all
Serotonin Syndrome
Constellation of sx composed, in order of
appearance, by
1.
2.
3.
4.
5.
6.
Diarrhea
Restlessness
Extreme agitation, hyperreflexia, autonomic
instability with fluctuation of vital signs
Myoclonus, seizure, hyperthermia, rigidity, shivering
Delirium, coma, status epilepticus,
cardiovascular collapse
Death
Serotonin Syndrome
SSRI + MAOI, MAOB Inhibitors, L-Tryptophan,
Lithium, SSRIs, SNRIs, TCAs, Buspirone,
Meperidine, Nefazodone, Trazodone, Linezolid
may
raise SSRI to toxic levels
Treatment
Remove
offending agent
Supportive care
nitroglycerine, methysergide, cooling
blankets, chlorpromazide, dantrolene,
benzodiazepines, anticonvulsants,
mechanical ventilation, paralyzing agents
Serotonin Syndrome
May resemble NMS
Serotonin
Syndrome more likely to have
Myoclonus
Hyperreflexia
GI symptoms
NMS
more likely to have
Muscular rigidity
SSRI Discontinuation Syndrome
Abrupt discontinuation of SSRI
Especially
Shorter ½ lives
Least
Fluvoxamine and Paroxetine
likely: Fluoxetine
Longer ½ life
Symptoms
Dizziness,
weakness, nausea, h/a, anxiety,
rebound depression, poor concentration,
upper respiratory sx, paresthesias.
Tricyclic and Tetracyclic
Antidepressants
(TCAs)
Tricyclics
Which of the following is a
secondary TCA?
Protriptyline
Clomipramine
Maprotiline
Amitriptyline
Doxepine
Available TCAs
Tertiary Amines
Secondary Amines
Clomipramine
Desipramine
Imipramine
Protriptyline
Trimipramine
Nortriptyline
Amitriptyline
Doxepin
Tetracyclics
Maprotyline
Amoxapine
Pharmacologic Actions
Significant metabolism - 1st pass effect
CYP450
2D6
(many meds may rise levels to toxic)
Half-lives from 10-70 hours
Longer
Nortriptyline, Maprotiline and Protriptyline
Pharmacologic Actions
TCA’s block reuptake pumps
NE and/or 5HT
Most 5HT selective Clomipramine
Most NE selective Desipramine
TCA Receptor Structure
Serotonin reuptake block
NE reuptake block
SIDE EFFECTS
SIDE EFFECTS
Histamine 1 receptor block
Weight gain
Doxepin
most antihistaminergic of the TCAs
SIDE EFFECTS
Muscarinic (M1) receptor block
Bethanecol
Tx
urinary retention
(M1) Anticholinergic SE
Can aggravate Narrow Angle Glaucoma
Avoid
TCAs in this condition – Amitriptyline
Can cause Anticholinergic Delirium
Especially
if TCA used with dopamine
receptor antagonist or anticholinergics
Treatment: IM or IV physostigmine
Least Anticholinergic
Amoxapine, Nortriptyline
Desipramine, Maprotiline
SIDE EFFECTS
Alpha-1 adrenergic receptor block
Most common cause of TCA d/c
Orthostatic Hypotension
Overdose with TCAs
TCAs – block voltage-sensitive Na
channels
– coma, seizures
Heart – arrhythmia, death
Brain
OD –monitored with EKG
Most frequent cause of death: arrhythmia
EKG changes: PR, QRS, QTc prolongation
Very common cause for discontinuation:
Tachycardia
Uses in Depression
Melancholic Features
Depressed mood
Severe anhedonia
Early morning awakening
Weight loss
Profound guilt
Very effective
More likely to induce mania than
bupropion or SSRIs
Better response
Melancholic
features, prior major depressive
episodes, family hx
In the US
Clomipramine
only approved for OCD
Other Uses
Panic disorder
Imipramine
– FDA approved
OCD
Only
– most studied drug
GAD
Doxepin
Clomipramine – use first SSRIs
Pain and Migraine prophylaxis
Amitriptyline
TCAs have
caused SUDDEN
DEATH in children
and adolescents!
– used most often
Childhood enuresis
Imipramine
Special Considerations
Amoxapine
May cause Parkinsonian sx
Avoid in Parkinson’s Disease
Blood levels of 4 TCAs can be monitored
Nortriptyline, Desipramine, Clomipramine and Imipramine
Nortriptyline: THERAPEUTIC WINDOW
TCAs have low risk for inducing seizures
Except for Maprotiline
May cause seizures when dose increased
too fast or kept at hight doses
Clomipramine and Amoxapine
May lower seizure threshold
DO NOT give
TCAs during
ECT! serious
cardiac effects
Special Considerations
Nortriptyline
least
Desipramine and Protriptyline
most
likely to cause orthostatic hypotention
activating of the TCAs
Relative contraindication for TCA use
Bundle
branch block
Cardiac disease or age >40
Do
EKG prior to TCA use
Drug Interactions
CYP 1A2, 2D6 and 3A4 dirty drugs
Birth control pills and nicotine decrease TCA levels
Fluoxetine, Fluvoxamine and Paroxetine increase TCA
levels x4!! (CYP 2D6)
If used together use lower dose of TCA
Antipsychotics and Methylphenidate increase TCA levels
Monoamine Oxidase
Inhibitors (MAOIs)
Therapeutic Indications
Depression
Atypical
Depression
Panic Disorder
Bulimia
PTSD
Migraine
ADD
Available MAOIs
Irreversible
Phenelzine
Tranylcypromine
Reversible/Selective
MAO-A (RIMA)
Moclobemide
Isocarboxazid
(not in the US)
Selective MAO-B
Selegiline
(transdermal patch)
Pharmacokinetics
MAOIs inhibit MAO A and B
Stops MAO from destroying
NE, 5HT and DA
Increasing these neurotransmitters
Irreversible
MAO
enzyme synthesized again in 2 weeks
Need for dietary restrictions
Washout period needed when starting a new antidep.
Reversible
MAO
enz synthesized again in 24-48h
Flexible dietary restrictions
Irreversible MAOIs
MAOI
MAOI
Two things to know about MAOIs:
Serotonin Syndrome
fentanyl
SSRIs
SNRIs
clomipramine
meperidine
(Demerol)
Hypertensive Crisis
Mainly
NE
Tyramine
(Sublimaze)
Lithium/Carbamazepine
Tryptophan
Other opioids
(methadone, tramadol)
Hypertensive Crisis
Tyramine in diet + MAO-A inhibition in gut
NORMALY,
in someone
not taking
MAOIs…
NE
NE
MAO-A destroys
NE
Alpha-1
receptors
Hypertensive Crisis
Tyramine containing
products
Aged Cheese
Tap beers
Smoked fish
Fava beans
NE
MAO-A
NE
Alpha-1
receptors
MAO-A
Hypertensive Crisis
Irreversible
MAOI
+
NE
NE
Alpha-1
receptors
Interesting facts
Selegiline
Inhibits
MAO-B
no destruction of MAO-A in the gut
not involved with intestinal tyramine reaction
no dietary restrictions
HTN crisis
Can
also be caused by DDI
pseudoephedrine
Side Effects
Most frequent side effect
Orthostatic
Hypotension
Other SE
Insomnia
Dizziness
Weight
Paresthesias
gain
Edema
Sexual
Switch
to mania
dysfunction
Contraindicated in pregnancy and nursing
Bupropion
(Wellbutrin)
Pharmacokinetics
NE and DA reuptake inhibitor
3 formulations available
DRI
immediate
release (TID)
sustained release (BID)
extended release (QD)
Bupropion
3 active metabolites
hydroxybupropion
threohydroxybupropion
erythrohydroxybupropion
NRI
Therapeutic Indications
Depression
Seasonal Affective Disorder (SAD)
DA reward pathways
ADHD
the only FDA approved antidepressant
fist line treatment: phototherapy
Smoking cessation
comparable efficacy to SSRIs
second line agent
appropiate for comorbid ADHD and depression
Hypoactive sexual desire
self or additive to other antidepressants (SSRIs)
The Good, the Bad and the Ugly
The GOOD
No
sexual dysfunction
Safe in pregnancy (class B)
No anticholinergic effects
No weight gain
No drowsiness
No orthostatic hypotension/cardiovascular
Side Effects
The BAD
Insomnia
but increases REM sleep
Anxiety
Not good for panic d/o or anxiety
GI
distress (especially nausea)
Restlessness/Agitation
Hypertension
Psychotic symptoms
Side Effects
The UGLY
Seizures
Incidence is 0.05% with 300mg or less
Risk increases with doses >400mg per day
May
0.1%!!
cause death with OD
Uncontrollable seizures
Sinus bradycardia
Cardiac arrest
Selective SerotoninNorepinephrine Reuptake
Inhibitors
(SNRIs)
SNRIs
Venlafaxine (Effexor)
Depression
GAD
Social
anxiety disorder
Desvenlafaxine Succinate (DVS)(Pristiq)
Duloxetine (Cymbalta)
Depression
GAD
Diabetic
Neuropathic Pain
Pharmacokinetics
Selective NE and 5HT reuptake inhibitors
TCAs
do too, but not selective (SE!)
Potent inhibitor of NE and 5HT
Weak inhibitor of DA reuptake
At lower doses – act like SSRIs
At higher doses – inhibit NE and 5HT
No activity in
Cholinergic
(M1)
Histaminergic (H1)
Adrenergic (alpha1)
Pharmacokinetics
Half lives
– 3.5 hours
ODV – 9 hours
Duloxetine – 12 hours
Venlafaxine
Discontinuation
Syndrome!
P450
Venlafaxine – 2D6
Active metabolite O-desmethylvenlafaxine (ODV)
Duloxetine
– 2D6 and 1A2
Side Effects
Venlafaxine
Most
common: nausea, sedation, dry mouth,
dizziness, anxiety, nervousness, insomnia, weigh
loss, constipation
Sexual dysfunction
HTN at higher doses
Midryasis – monitor patients with acute narrow-angle
glaucoma
Platelet aggregation (serotonin-related impairment)
In pts with liver disease – decreased clearance
Side Effects
Duloxetine
Most common
Nausea
SE leading to discontinuation
Liver toxicity
Avoid in
Hepatic
insufficiency
ESRD
Uncontrolled
No HTN
narrow-angle glaucoma
Mirtazapine
(Remeron)
Pharmacokinetics
Does NOT work by inhibiting
reuptake of NE and 5HT!
Mechanism of Action
Antagonist
Mirtazapine
of central presynaptic alpha-2 adrenergic
receptors
Increased release of NE and 5HT from neurons
Blocks postsynaptic 5HT-2 and 3 receptors
Decreases anxiety, stimulates appetite, relieves insomnia,
decreased nausea and diarrhea
Strong antagonist of histamine H1 receptors
sedation at low dose – weaker at higher doses
Therapeutic Indications
Depression
melancholic
features
elderly
Augmentation with SSRIs or Venlafaxine
counteract nausea, agitation and insomnia
NO CYP 450 effects!
Cancer patients
GI
side effects of chemotherapy
sedation and stimulation of appetite
Side Effects
Weight gain and stimulation of appetite
Somnolence
in more than 50% of persons
avoid alcohol and sedating OTC
potentiates sedative effects
medications
↑ cholesterol, triglycerides and ALT
Dizziness
In some orthostatic hypotension
Agranulocytosis
Low incidence of sexual SE
Nefazodone and Trazodone
Nefazodone
Shortest ½ life of all antidepressants
2-3
hours!
Active metabolites
hydroxynefazodone
(principal)
mCPP (meta-chlorophenylpiperazine)
5HT effects – migraine, anxiety and weight loss
Nefazodone
Orthostatic hypotension,
dry mouth, sedation
No sexual
dysfunction
No anticholinergic SE
Increases REM
sleep
Cytochrome
P450 3A4
elevation of
Antianxiety,
antidepressant and
somnolence
Alprazolam
Triazolam
Haldol
Digoxin
Therapeutic Indications
Depression
Panic disorder
Premenstrual dysphoric disorder
GAD
Chronic pain
PTSD
Chronic fatigue syndrome
Nefazodone
When switching from SSRI to Nefazodone
Won’t
protect from withdrawal symptoms
High risk for hepatotoxicity
Trazodone
Active metabolite
mCPP
(metachlorophenylpiperazine)
Migraine, anxiety, weight loss
Strong anti H1 effect
Use
in insomnia
↓ REM sleep
↑ total sleep time
↓ number and duration of nighttime
awakenings
Trazodone
More risk of orthostatic hypotension than
Nefazodone (alpha 1)
½ life
5-9
hours
Can cause priapism