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M2 Psych > 10/12 Antidepressants - Walworth > Flashcards

10/12 Antidepressants - Walworth Flashcards

1
Q

monoamine neurotransmission

action of reserpine

relationship between reserpine and depression →

monoamine hypothesis

A

neurotransmitters (norepi, DA, serotonin) are synthesized from a.a. precursors in specific neurons, packaged into vesicles, released in response to stimuli

  • bind to postsyn cell receptors
  • can also be re-uptaken by presyn cell transporter

reserpine binds to vesicles and inhibits VMAT (vesicular monoamine transporter) → prevents nerve endings from storing/concentrating monoamines in vesicles

  • combined with monoamine degradation by MAO in the cytoplasm…little to no active nt released by presyn

depletion of nt by reserpine can lead to depression

→→→ hypothesis for pathegenesis of depression!

Monoamine Hypothesis: depressed mood results from decreased monoamine neurotransmission

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2
Q

monoamine neurotransmitters related to depression

A

serotonin and central adrenergic neurotransmission modulate mood

→ depression represents decr availability of either 5-HT (serotonin) or NE or both

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3
Q

synthesis and catabolism of serotonin, norepi

A

serotonergic neurons:

  • pick up L-tryptophan → 5HTP → 5HT → released/reuptaken
    • 5HT can be degraded in cytoplasm by MAO

noradrenergic neurons:

  • pick up tyrosine → DOPA → DA → NE → released/reuptaken
    • NE can be degraded in cytoplasm by MAO
    • NE can be degraded in synapse by COMT
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4
Q

sites of action of major classes of antidepressants

A

1. block breakdown of nts

  • MAOIs (cytoplasm)

2. block reuptake of nts

  • SSRIs (membrane transporter)
  • SNRIs (membrane transporter)
  • TCAs (membrane transporter)

3. antagonize receptors for serotonin on postsynaptic cells

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5
Q

limitations to monoamine hypothesis of depression

possible explanation

A

TIME LAG/delay in clinical effect

  1. clinically useful antidepressants act rapidly at pharmacologic sites of action…

but clinical effects require 3 or more weeks of tx

  1. reserpine rapidly depletes nt…

but several weeks of tx are required to induce depression

possible role of presynaptic autoreceptors

autoreceptors bind nt released by a cell or neighboring cells

  • NOT reuptake transporter!
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6
Q

autoreceptor autoregulatory mechanisms

pretreatment

acute treatment

long-term treatment

A

pre-treatment

  • autoreceptors bind to nt (serotonin or NE) released by presynaptic cell
  • ligand-bound autoreceptors exert inhibitory effect on synthesis and release of nt

→→→ low level of signaling at postsyn cell

acute treatment

  • acute treatment blocks reuptake transporter proteins (TCA or SSRI) → increased binding to presyn autoreceptors → increased inhibitory effect on synthesis and release of nt

→→→ low level of signaling at postsyn cell continues

long-term treatment

  • long term tx with reuptake inhibitor → continuous exposure of autoreceptors to nt → downregulation of autoreceptors!!!
    • disinhibition of synthesis and release of nt

→→→ more nt made/released → therapeutic level of signaling achieved

model to explain why the time lag for txeffect might exist

  • may or may not hold up under scrutiny
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7
Q

sites of action of major classes of antidepressants

A

reuptake inhibition

  • noradrenergic neurons: NET targeted by
    • TCAs
    • SNRIs
  • serotonergic neurons: SERT targeted by
    • SSRIs
    • TCAs
    • SNRIs

inhibition of degradation

  • degradation of NE/5HT by MAO targeted by
    • MAOIs
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8
Q

SSRIs

drugs

clinical uses

A

selective serotonin reuptake inhibitors

  • bc relatively selective for 5HT transporter, side effects are limited to effect on 5HT-mediated responses

fluoxetine (Prozac)

paroxetine (Paxil)

sertraline (Zoloft)

citalopram

escitalopram (Lexapro)

fluvoxamine

SSRI clinical uses

  • major depression
  • anxiety disorder
  • OCD
  • PTS
  • PMDD
  • bulimia
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9
Q

SSRI adverse effects

A

resulting from elevation of serotonin in various tissues

  • nausea
  • headache
  • anxiety
  • agitation
  • insomnia
  • sexual dysfx
  • extrapyramidal effects (early on)
  • seizures with gross overdose
  • serotonin syndrome with MAOI
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10
Q

SNRI

drugs

clinical uses

A

serotonin and norepi reuptake inhibitor

  • inhibit both NE reuptake transporter (NET) and 5HT reuptake transporter (SERT)

venlafaxine (Effexor)

duloxetine (Cymbalta)

clinical uses

  • major depression
  • chronic pain
  • fibromyalgia
  • menopausal sx
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11
Q

SNRI adverse effects

A

lots of overlap with SSRI side effects (bc still blocking SERT)

  • nausea
  • headache
  • anxiety
  • agitation
  • insomnia
  • sexual dysfx
  • extrapyramidal effects (early on)
  • seizures with gross overdose
  • serotonin syndrome with MAOI

also effects from blocking NET

  • anticholinergic
  • sedation
  • hypertension (venlafaxine)
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12
Q

TCAs

drugs

clinical uses

A

tricyclic antidepressant

  • inhibit reuptake transporters for both NE and 5HT (like SNRIs)
  • also interact with variety of other receptors → broad range of side effects

imipramine (more selective for SERT)

amitriptyline

clomipramine (more selective for NET)

desipramine

nortriptyline

clinical uses

  • major depression
  • chronic pain
  • OCD (clomipramine)
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13
Q

TCA adverse effects

A

lots of overlap with SSRI side effects (bc still blocking SERT)

  • nausea
  • headache
  • anxiety
  • agitation
  • insomnia
  • sexual dysfx
  • extrapyramidal effects (early on)
  • seizures with gross overdose
  • serotonin syndrome with MAOI

also other effects

  • alpha-block (orthostatic hypotension)
  • muscarinic block
  • sedation
  • weight gain
  • arrhythmias and seizures with OD
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14
Q

MAOIs

drugs

clinical uses

A

monoamine oxidase inhibitors

  • inhibit MAO

phenelzine → combines irrev with MAO (long lasting inhibition)

tranylcypromine → does not bind irrev, but has prolonged effect

clinical uses:

  • major depression unresponsive to other drugs
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15
Q

MAOI adverse effects

A
  • hypertensive rxn in response to indirectly acting sympathomimetics
  • hypterthermia
  • CNS stimulation (agitation, convulsions)
  • HTN crisis with tyramine-containing food
  • serotonin syndrome with SSRI
  • orthostatic HTN
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16
Q

5HT2 antagonists

drugs

clinical uses

A

serotonin receptor (2) antagonists

  • anti-anxiety, anti-psychotic, anti-depressive effects

nefazodone → black box warning due to hepatotox

trazodone → prodrug, converted to 5HT2A antagonist

clinical uses

  • major depression
  • hypnosis (trazodone)
17
Q

5HT2 antagonist adverse effects

A
  • sedation
  • alpha-block (orthostatic hypotension)
18
Q

heterocyclic agents

drugs

clinical uses

A

bupropion → mech unclear

  • enhances both NE and DA neurotransmission

mirtazapine → blocks presyn alpha2 receptors (typically inhibit release of nt…action of mirtazapine disinhibits this release)

  • antagonist at 5HT2A/2C and 5HT3 receptors
  • antagonist of presyn alpha2 autoreceptor → enhances release of NE and 5HT

clinical uses

  • major depression
  • smoking cessation (bupropion)
  • sedation (mirtazapine)
19
Q

heterocyclics adverse effects

A

bupropion

  • lowers seizure threshold

mirtazapine

  • sedation
20
Q

summary table highlighting differences of antidepressants

A

SSRIs block 5HT reuptake, not a whole lot of other action

SNRIs block 5HT and NE reuptake, not a whole lot of other action

TCAs block 5HT and NE reuptake, also block other receptors (ACh M, alpha adrenergic, histamine)

others…

  • trazodone: antagonist at 5HT2 receptors
  • bupropion: mech unclear
  • mirtazapine: antagonist at 5HT2 receptors but also blockade of H1 receptors (sedative props)
21
Q

PK features of antidepressant drugs

general features

special notes for SSRI, SNRI

A

in general, most

  • rapid oral absorption
  • peak pl concentration in 2-3hr
  • half-life approx 0.5-1 day
  • tightly bound to plasma proteins
  • metabolized by liver
  • eliminated by kidney

SSRIs

  • norfluoxetine (metabolite of fluoxetine) has loooong halflife (7-9days)
    • imp to know if transitioning to diff drug! bc it prob wont all be cleared at time of transition

SNRIs

  • venlafaxine extensively metabolized via CYP2D6
    • keep an eye out for inducers
22
Q

major drug interactions with antidepressants

A

PK interactions

  • paroxetine and fluoxetine are inhibitors of CYP2D6
    • many drugs are 2D6 substrates (TCAs, haloperidol/risperidone, codeine/oxycodone, betablockers)
  • fluvoxamine and others are inhibitors of CYP3A4

PD interactions

  • sedative effect drugs are ADDITIVE with other sedatives (esp alc and benzodiazepines)
  • MAOIs sensitize pt to indirect sympathomimetics (tyramine) and to sympathomimetics (ephedrine)
  • SSRI/SNRI + MAOI → serotonin syndrome
23
Q

serotonin syndrome

A

most frequently from drug interactions from drugs acting on diff mechs to increase serotonin signaling

  • SSRI + MAOI
  • SSRI + drug with MAOI activity (ex. linezolid)
  • SSRI + serotonergic drug (ex. dextromethorphan, sumatriptan, tramadol, St. John’s word)
  • SNRI + MAOI

AMS, fever, tachycardia, HTN, agitation, tremor, myoclonus, hyperreflexia, ataxia, incoordination, diaphoresis, shivering, GI sx

24
Q

overdoses of antidepressants

A

TCAs : extremely dangerous (no refill, small quant rx)

MAOIs : intoxication is rare, req supportive tx

SSRIs : OD fatalities rare, intoxication req supportive tx

bupropion : seizures

mirtazapine : disorientation, tachycardia

OD with newer agents often involves other drugs, incl alcohol

25
Q

lithium

A

indicated for bipolar affective disorder

  • efficacy as monotherapy for manic phase

Li mechanism: unclear

  • enters cells via Na channels
  • substitutes for Na in generating APs, Na exchange across membranes

PK

  • completely absorbed in 6-8hr
  • distributed in total body water → slow entry to intracellular compartments, no protein binding
  • excreted entirely in urine
  • pl halflife 20hr
  • target pl conc approx 0.6-1.4 mEq/L
    • TOX seen at 2 mEq/L

drug interactions

  • diuretics decr renal clearance by 25%
  • some NSAIDs decrease clearance by incr Li reabs in proximal tubules
26
Q

Li toxicity and adverse effects

A

tremor common at therapeutic dose

  • controlled with propranolol or atenolol

reversibly decreases thyroid rx

reversible polydipsia, polyuria

inhibits K entry to myocytes

  • abnormal repol
  • extracellular hyperK
  • intracellular hypoK
27
Q

Li contraindications

A
  • severe deydration or Na depletion
  • signficant CVD
  • signficant renal impairment
  • during lactation
28
Q

overal drug list

A

M2 Psych (24 decks)

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