Week 10 Reverse

Question 1

4-6 weeks for symptom relief and up to 12 weeks for full effects.

Answer 1

SSRI: Onset of Action

Question 2

Fluoxetine has the longest half-life (~50 hours, with active metabolite ~10 days), reducing withdrawal risk; paroxetine and sertraline have shorter half-lives and higher risk for discontinuation syndrome.

Answer 2

SSRI: Half-lives & Implications

Question 3

Symptoms include flu-like symptoms, insomnia, imbalance, sensory disturbances, and hyperarousal; more likely with short half-life SSRIs like paroxetine; tapering recommended.

Answer 3

SSRI: Discontinuation Syndrome

Question 4

Include dizziness, anterograde amnesia, complex sleep behaviors (e.g., sleepwalking), next-day sedation (especially with ER formulations), and rebound insomnia.

Answer 4

Hypnotics: Adverse Effects

Question 5

Use short-term; choose agent based on half-life and sleep complaint (falling asleep vs. staying asleep); consider safety, especially in elderly.

Answer 5

Hypnotics: Management Considerations

Question 6

Rapid onset with IR formulations; ER and patch forms provide extended symptom control over the day.

Answer 6

Methylphenidate: Onset of Action

Question 7

Inhibits reuptake of dopamine and norepinephrine; increases synaptic concentrations of both neurotransmitters.

Answer 7

Methylphenidate: MOA

Question 8

Used for depression, chronic pain (e.g., neuropathy), migraine prophylaxis, and insomnia at low doses.

Answer 8

TCAs: Clinical Indications

Question 9

Anticholinergic (dry mouth, constipation), sedation, weight gain, orthostatic hypotension, cardiotoxicity (QT prolongation), and sexual dysfunction.

Answer 9

TCA: Adverse Effects

Question 10

GI upset, sexual dysfunction, insomnia, anxiety, headache, weight changes, and QT prolongation (especially with citalopram).

Answer 10

SSRI: Adverse Effects

Question 11

Similar to SSRIs with additional risks of elevated BP and HR at higher doses (notably venlafaxine); GI distress and sexual dysfunction common.

Answer 11

SNRI: Adverse Effects

Question 12

Dopamine/norepinephrine reuptake inhibitor; lowers seizure threshold; minimal sexual dysfunction; contraindicated in eating disorders.

Answer 12

Atypical Antidepressants: Bupropion

Question 13

Increases NE and 5-HT via α2 antagonism; causes sedation, weight gain, increased appetite; fewer sexual side effects.

Answer 13

Atypical Antidepressants: Mirtazapine

Question 14

MAOIs contraindicated with serotonergic drugs due to serotonin syndrome risk; TCAs avoided in suicidal patients due to overdose lethality.

Answer 14

Antidepressants: Contraindications

Question 15

FGAs (e.g., haloperidol): D2 blockade, higher EPS risk. SGAs (e.g., risperidone, olanzapine): D2 + 5HT2A blockade, lower EPS but higher metabolic risk.

Answer 15

1st vs. 2nd Gen Antipsychotics

Question 16

FGAs block D2 receptors. SGAs block D2 and 5-HT2A receptors. Some SGAs also act on other receptors (α, histamine, muscarinic).

Answer 16

Antipsychotics: MOA

Question 17

EPS (more common in FGAs), metabolic syndrome (SGAs), QT prolongation, sedation, orthostasis, prolactin elevation, and anticholinergic effects.

Answer 17

Antipsychotics: Adverse Effects

Question 18

Fluoxetine and paroxetine inhibit CYP2D6; fluvoxamine inhibits CYP1A2 and CYP2C19; drug interactions can impact efficacy and toxicity.

Answer 18

CYP450 & Antidepressants

Question 19

Combining serotonergic agents increases serotonin syndrome risk; combining CNS depressants (e.g., BZDs + opioids) increases sedation and respiratory depression.

Answer 19

Multidrug Regimen Risks

Question 20

First-line: SSRIs, SNRIs. Second-line: atypical antidepressants (e.g., bupropion, mirtazapine), TCAs, and MAOIs (last-line due to safety).

Answer 20

Depression: First- vs. Second-Line Agents

Question 21

SSRIs/SNRIs: depression, anxiety; TCAs: depression, pain; bupropion: depression, smoking cessation; trazodone/mirtazapine: depression + insomnia.

Answer 21

Antidepressant Class Indications

Question 22

Enhance GABA-A activity by increasing Cl- channel opening frequency; result in CNS depression, anxiolysis, sedation, anticonvulsant effects.

Answer 22

Benzodiazepines: MOA

Question 23

Acute anxiety, panic disorder, alcohol withdrawal, seizure emergencies, muscle relaxation, pre-op sedation, short-term insomnia.

Answer 23

Benzodiazepines: Indications

Question 24

Abrupt discontinuation can lead to SSRI discontinuation syndrome: flu-like symptoms, insomnia, imbalance, sensory disturbances, and hyperarousal. Tapering is essential to minimize symptoms.

Answer 24

SSRI Withdrawal: General Considerations

Question 25

Fluoxetine has a long half-life and active metabolite (norfluoxetine), making withdrawal symptoms less likely. Paroxetine and sertraline have shorter half-lives, increasing the risk of withdrawal symptoms.

Answer 25

SSRI Withdrawal: Fluoxetine vs. Others

Question 26

Venlafaxine is associated with significant withdrawal symptoms due to short half-life and rapid offset. Taper slowly to avoid flu-like symptoms, irritability, and agitation.

Answer 26

SNRI Withdrawal: Venlafaxine

Question 27

A 14-day washout is required when switching from or to an MAOI to avoid serotonin syndrome. Fluoxetine requires a longer washout (at least 5–6 weeks) due to its long half-life.

Answer 27

MAOI Washout Periods

Question 28

Switching between antidepressants often requires tapering and a washout period, especially with MAOIs. Cross-tapering or direct switches may be possible with closely related agents under supervision.

Answer 28

Antidepressant Switching: General Guidelines