Exam 4

Question 1

Behavior depends on

Answer 1

Perception, Genetics, Experience

Question 2

Biopsychosocial model

Answer 2

Biology, psychology, social, and environmental factors may ALL be important

Question 3

Interventions for mental illness

Answer 3

Non-pharm neuromodulation, pharmacological interventions, psychotherapy and illness education

Question 4

Neuroplasticity

Answer 4

Allows an individual to adapt to a rapidly changing environment through strengthening, weakening, pruning, or adding of synaptic connections and by promoting neurogenesis.

Question 5

Neuroplasticity in daily life

Answer 5

Long term potentiation (LTP)- strengthens neuronal connections.
Long term depression (LTD)- weakens neuronal connections.
Global processing- forms big picture understanding, context.
Local processing- perceives small details, faces

Question 6

Factors of change in neuroplasticity

Answer 6

Age

Illnesses

Question 7

Types of brain damage

Answer 7

Tumors/malignancies
Strokes
TBI
Infections/toxins
Congenital disease
Epilepsy
Neurodegenerative conditions- dementia, huntingtons, parkinsons
Mental illness

Question 8

Common neurotransmitters in mental illness

Answer 8

BDNF, Glutatmate, GABA, acetylcholine, DA, serotonin, NE

Question 9

BDNF

Answer 9

Promotes neurogenesis

Question 10

Glutamate

Answer 10

Neuronal development, synapse organizations, DA regulation

Question 11

GABA

Answer 11

Neuronal circuitry in prefrontal cortex, inhibition

Question 12

Acetycholine

Answer 12

Cortical plasticity, processing senses

Question 13

DA

Answer 13

Reward, positive symptoms

Question 14

Serotonin

Answer 14

Multiple functions,modulates BDNF

Question 15

NE

Answer 15

Arousal, sensory integration, memory

Question 16

Illness education

Answer 16

Stigma- taking the vagueness out of mental illness, making it medical.
Expectations- time needed for neurons to grow or change. May not feel better with one dose/session.
Balancing interventions- behavior/environment, meds, both have neuronal impact

Question 17

Psychotherapy examples

Answer 17

Cognitive behavioral therapy
Dialectical behavioral therapy
Exposure therapy
Eye movement desensitization and reprocessing

Question 18

Who is most likely to benefit from psychotherapy?

Answer 18

Depression, anxiety, PTSD, OCD
May be effective in bipolar, ADHD
Minimal benefit in schizophrenia

Question 19

Bright light therapy

Answer 19

Bright light intended to mimic sun exposure
Controlled exposure of intense, but safe light
-6,000-10,000 lumens for 30 min/day
UV filtered

Question 20

Bright light therapy risk vs benefit

Answer 20

Risk- choosing a good product, photosensitive agents, AE

Benefits- may help sleep disorders, safe, patient accepted.

Question 21

Who is most likely to benefit from bright light?

Answer 21

Depression= first line in SAD

Bipolar disorder if absence of mania, must be on an anti-manic

Question 22

Repetitive transcranial magnetic stimulation

Answer 22

Brain stimulation therapy
Electromagnetic coil is placed against the head in a specific location and short pulses pass through the skull and stimulate nerve cells. Treatments lasts 4-6 wks and is 5 days/week

Question 23

Risks vs benefit of rTMS

Answer 23

Risks- very expensive, contraindications similar to MRIs, timely, AE
Benefits- less AE than ECT, well accepted if the patient has time and money, noninvasive

Question 24

Who is likely to benefit from rTMS?

Answer 24

Depression= 2nd or 3rd line

Bipolar- 3rd line

Question 25

Electroconvulsive therapy (ECT)

Answer 25

A procedure given with neuromuscular blockers and generalized anesthesia (sedated then paralyzed then electrical current then seizure then recovery)
Can be done outpatient.

Question 26

Process of ECT

Answer 26

Psychiatric and medical examination- informed consent- 3 treatments/week for 2-4 weeks, f/u

Question 27

ECT risk vs benefit

Answer 27

Risk= AE

Benefit- high efficacy rate, faster than antidepressants. Safe in pregnancy, elderly, very low mortality rates

Question 28

Who is most likely to benefit from ECT?

Answer 28

Depression- 1st line in severe/psychosis
Bipolar- 2nd line in bipolar depression
Some evidence in schizophrenia

Question 29

Sedative

Answer 29

A drug that produces a calming state and reduction of anxiety

Question 30

Hypnotic

Answer 30

A drug that produces drowsiness, facilitates sleep

Question 31

Anxiolytic

Answer 31

A drug that reduces anxiety

Question 32

Barbiturates

Answer 32

Classified based on duration of action
Tolerance- greater to sedation than to anticonvulsant or lethal effects; thus narrow therapeutic index
Thiopenal, methohexital, pentobarbital, secobarbital, amobarbital, phenobarbital

Question 33

Which barbiturates are ultrashort acting (5-15 minutes)

Answer 33

Thiopental, methohexital, pentobarbital

Question 34

Which barbiturates are short acting (3-8 hours)?

Answer 34

Pentobarbital, secobarbital, amobarbital

Question 35

Which barbiturate is long acting (days)

Answer 35

Phenobarbital

Question 36

Benzodiazepines

Answer 36

Term refers to portion of chemical structure composed of benzene ring; halogens (F, Cl) increase lipid solubility.
Broad spectrum of activity- anxiolytics, sedatives, hypnotics, muscle relaxants, anti-convulsants

Question 37

Advantages of benzodiazepines

Answer 37

High margin of safety, little respiratory or CV depression

Question 38

Which therapeutic uses of benzodiazepines require a long 1/2 life?

Answer 38

Anticonvulsant, anxiolytic

Question 38

Which therapeutic uses of benzodiazepines require a long 1/2 life?

Answer 38

Anticonvulsant, anxiolytic

Question 39

Which therapeutic uses of benzodiazepines requires rapid entry into the brain?

Answer 39

Status epilepticus

Question 40

Which therapeutic use of benzodiazepines requires short elimination 1/2 life

Answer 40

Hypnotic

Question 41

Short acting benzodiazepines

Answer 41

Midazolam, triazolam

Question 42

Intermediate acting benzodiazepines

Answer 42

alprazolam, clonazepam, oxazepam, temazepam

Question 43

Long acting benzodiazepines

Answer 43

Chlordiazepoxide, diazepam, flurazepam

Question 44

GABA/Benzodiazepine receptor complex

Answer 44

All clinically important actions are mediated by the GABA-benzodiazepine receptor complex.
Ion channel that facilitates chloride entry into neuron leading to hyperpolarization and reduced neuronal firing.

Question 45

GABA-Benzo receptor ligands

Answer 45

GABA, Benzo,

Benzo antagonist- flumazenil

Question 46

What drug is used for Benzo OD

Answer 46

Flumazenil

Question 47

Benzo AE

Answer 47

CNS depression: sedation, psychomotor impairment, ataxia, abuse
Anterograde amnesia
Physical dependence/withdrawal
Interactions with alcohol and other sedatives.

Question 48

Buspirone

Answer 48

Non-benzo anxiolytic.
Agonist at 5-HT1A receptors. Does not exhibit cross tolerance with benzos
Anxioselective- has no other properties

Question 49

Buspirone advantages and disadvantages

Answer 49

Advantage- fewer and less severe CNS effects compared to benzos (no physical dependence)
Disadvantage- slower OOA, 1-2 weeks

Question 50

Benzo vs. buspirone

Relief of generalized anxiety

Answer 50

Both

Question 51

Benzo vs buspirone

Which has addiction liability

Answer 51

Benzo

Question 52

Benzo vs buspirone, which has rebound anxiety?

Answer 52

Benzo

Question 53

Benzo vs buspirone, which has physical dependence?

Answer 53

Benzo

Question 54

Benzo vs buspirone, which has delay in anxiolytic effect?

Answer 54

Buspirone

Question 55

Benzo vs buspirone, which potentiates alcohol sedation

Answer 55

Benzo

Question 56

Hypnotics: Novel benzodiazepine agonists

Answer 56

Zolpidem, Zaleplon, Eszoplicone

Non-benzo that act as agonists or positive allosteric modulators at the GABA/Benzo receptor complex

Question 57

Novel benzo agonists BBW

Answer 57

Risk of serious injuries in sleepwalking

Question 58

Novel benzo agonists (z drugs) properties

Answer 58

Strong sedative effects mask anxiolytic  action
Only weak anticonvulsant effect
Little evidence of physical dependence
Short 1/2 life
No rebound insomnia

Question 59

Novel benzo agonists (z drugs) MOA

Answer 59

Binds to alpha-1 subunit containing sites

Question 60

Hypnotics: melatonin receptor agonists

Answer 60

Ramelteon and Tasimelteon
Activates melatonin receptors
Rapid onset with minimal rebound insomnia

Question 61

Suvorexant

Answer 61

Orexin antagonist
Lacks abuse potential
Hypnotic but not sedating

Question 62

Drugs for bipolar disorder

Answer 62

Lithium

Carbamazepine, valproate, lamotrigine, quetiapine, cariprazine

Question 63

Etiology of depression

Answer 63

Biogenic amine hypothesis
-Disorders of mood result from dysfunction of brain monoamine neurotransmitters (serotonin and NE primarily)
Newer focus on neuroplasticity

Question 64

What type of diet promotes depression?

Answer 64

Tryptophan deficient diet

Question 65

Classification of antidepressants

Answer 65

Tricyclic antidepressants (TCAs)
Selective serotonin (5-HT) reuptake inhibitors (SSRIs)
Selective serotonin-NE reuptake inhibitors (SNRIs)
Monoamine oxidase inhibitors (MAOIs)
Heterocyclics
Ketamine

Question 66

TCA drugs

Answer 66

Amitriptyline, desipramine, imipramine

Question 67

TCA MOA

Answer 67

Inhibit the reuptake mechanisms (transporters) responsible for the termination of the synaptic actions of both NE and 5-HT in the brain. Results in potentiation of their neurotransmitter actions at postsynaptic receptors

Question 68

TCA effects

Answer 68

Acute- block the reuptake of NE and 5-HT.

Delayed- Weeks, therapeutic onset with all antidepressants (except ketamine)

Question 69

Tricyclic antidepressants AE

Answer 69

Muscarinic ACh blockade- dry mouth, urinary retention, constipation
a-adrenergic (NE) blockade- orthostatic hypotension
Histamine blockade- sedation, weight gain
Sodium channel blockade- cardiac toxicity

Question 70

Selective serotonin reuptake inhibitor agents

Answer 70

Fluoxetine, sertraline, paroxetine, fluvoxamine, citalopram, escitalopram

Question 71

SSRIs acute effects

Answer 71

Selectively block reuptake of 5-HT. Minimal inhibitory effect on NE transporter or blockade of ACh or NE receptors

Question 72

What is better tolerated, SSRIs or TCAs?

Answer 72

SSRIs

Question 73

Serotonin-norepinephrine reuptake inhibitors (SNRIs) MOA

Answer 73

SNRIs bind and inhibit transporters for both NE and 5-HT

Enhance the actions of both neurotransmitters

Question 74

SNRIs drugs

Answer 74

Desvenlafaxine, duloxetine, venlafaxine, levomilnacipramine

Question 75

How do SNRIs differ from TCAs?

Answer 75

In lacking significant blocking effects on peripheral receptors including H1, muscarinic, or a-adrenergic receptors

Question 76

Serotonin receptor antagonists/ SRI agents

Answer 76

Trazodone, nefazodone (not us)

Question 77

Serotonin receptor antagonists actions

Answer 77

5-HT2A/C receptor antagonist and 5-HT uptake inhibitor

Question 78

Vilazodone

Answer 78

Antidepressant

5-HT reuptake inhibitor/ 5-HT1a partial agonist`

Question 79

Vortioxetine

Answer 79

Antidepressant

5-HT stimulator/modulator

Question 80

Monoamine oxidase inhibitors drugs

Answer 80

Phenelzine and tranylcypromine
Non selective inhibitors of MAO A and B, inhibit NE and 5-HT
Selegiline- selective inhibitor of MAO-B at low doses

Question 81

MOA of MAOIs

Answer 81

Inhibit monoamine oxidases that metabolize NE and 50HT and dopamine
Increase vesicular stores of 5-HT and NE

Question 82

DDI and MAOIs

Answer 82

Foods containing tyramine with MAOIs can lead to htn crissi

Question 83

Which antidepressants have the worst sexual AE

Answer 83

SSRIs
Venlafaxine
Some- tricyclics, MAOIs

Question 84

Which antidepressants have the worse conduction AE

Answer 84

Tricyclics

Question 85

Which antidepressants have the worst seizure AE

Answer 85

Bupropion is worst
Tricyclics
Some- venlafaxine, SSRIs, trazadone

Question 86

Which antidepressants have the worst sedation?

Answer 86

Tricyclics, trazodone

Question 87

Which antidepressants have the worst anti-adrenergic (orthostatic hypotension) AE

Answer 87

Tricyclics

Trazodone

Question 88

Which antidepressants have the worst anticholinergic AE

Answer 88

Tricyclics

Question 89

Acute antidepressant drug action

Answer 89

Increased concentrations of transmitter in synapse, Predictive of antidepressant action.

Question 90

Chronic antidepressant drug action

Answer 90

Enhanced 5-HT and NE transmission

Down regulation of receptors

Question 91

Rapid acting antidepressant

Answer 91

Ketamine

-lack of sustained response

Question 92

Post-partum depression

Answer 92

Brexanolone

Question 93

Bipolar agents (mood stabilizers)

Answer 93

Prophylactic treatment

Lithium

Question 94

AE of lithium

Answer 94

Low therapeutic index
Polydipsia and polyuria
Renal toxicity
CNS AE is tremor

Question 95

Biopsychosocial model

Answer 95

Biology, psychology, social, and environmental factors may all be important in psych disorders

Question 96

Prevalence of MDD in US adults

Answer 96

Very common
Female
Native Americans
Low socioeconomic status
Stressors- medical, mental, socioeconomic
First-degree relative with depression (40-50% heritability)

Question 97

DSM-5 Diagnosis of MDD

Answer 97

Depressed mood and/or anhedonia (lack of pleasure) occurring almost every day for >2 weeks
AND
5+ additional symptoms that cause significant distress and/or impairment in social or occupational functioning

Question 98

Signs of depression (D-SIGECAPS)

Answer 98

Depressed mood
Sleep- insomnia or hypersomnia
Interest- diminished 
Guilt- feelings of worthlessness 
Energy- loss
Concentration- diminished
Appetite- significant weight loss or gain
Psychomotor agitation or retardation
Suicide

Question 99

Standardized rating scales for MDD

Answer 99

HAM-D
MADRS
PHQ-9
PHQ-2
QIDS

Question 100

MDD differential diagnosis

Answer 100

Rule out non-organic causes

• substance use (alcohol, benzodiazepines)
• Medications can cause “depression-like” symptoms
• Other medical conditions- hypothyroidism, anemia, heart disease

Question 101

Drug induced depression

Answer 101

Antihypertensives- Beta blockers, calcium channel blockers
CNS depressants- alcohol, benzodiazepines, opioids
Anti-infectives- fluoroquinolones, acyclovir
Misc. - Isotretinoin, oral contraceptives, corticosteroids

Question 102

Response and remission of depression

Answer 102

Untreated episodes usually last around 6 months
Periods of remission shorten with subsequent episodes
1/2 will fully respond
15% may never experience remission/recovery

Question 103

Depression recurrence

Answer 103

About 1/2 of patients will experience a single episode
Patients who have experienced 3 or more episodes exhibit a 90% recurrence.
Other risk factors-chronic medical conditions, other psychiatric comorbidities, childhood maltreatment

Question 104

Depression and suicidality

Answer 104

If untreated, lifetime risk of suicide is about 20%
Highest in older (>75 yo) white males, LGBTQ+, teenager/ adolescents
Other risk factors: IS PATH WARM

Question 105

IS PATH WARM suicide risks

Answer 105

ideation 
substance abuse
Purposelessness
anxiety
Trapped
Hopelessness
Withdrawal
Anger
Recklessness
Mood change

Question 106

Pathophysiology of depression

Answer 106

Monoamine deficiency
Receptor dysregulation
Chronic stress
Unknown

Question 107

Monoamine hypothesis of depression

Answer 107

Based on the MOA of the earliest antidepressants.
MAOIs and TCAs work to increase the levels of NE, Serotonin, and Dopamine
Hypothesis: Depressed patients are deficient in monoamine neurotransmitters
….but antidepressants increase neurotransmitters in the synapse on day 1 and antidepressants dont work for weeks.

Question 108

Neurotransmitter receptor hypothesis (AKA sensitivity hypothesis) of depression

Answer 108

Extension of monoamine hypothesis
Attempts to account for delayed antidepressant activity
Hypothesis: Depletion of monoamine neurotransmitters leads to neural hypersensitivity and receptor up-regulation.
…but there is no reproducible evidence of consistent monoamine deficiency in depressed patients

Question 109

Monoamine hypothesis of gene expression (stress model) of depression

Answer 109

Evidence that despite normal monoamine levels and their receptors, these systems do not respond normally in depressed patients.
Cortisol is released causing a reduction in brain-derived neurotrophic factor (BDNF)
Hypothesis: Serotonin enhances BDNF and neurogenesis in the hippocampus, reversing negative effects of cortisol. Glutamate modulation quickly releases BDNF in the brain.

Question 110

Summary of theories of depression

Answer 110

There appears to be a dysfunction in the frontal cortex and limbic structures
Manipulation of serotonin and NE systems can alter depressive symptoms

Question 111

MDD: Treatment algorithm

Answer 111

1st line- SSRI (except fluvoxamine), SNRI, NaSSA, NDRI, vortioxetine
Titrate for 1-4 weeks
No response- change agent, test for weeks 4-8
Partial response- augment, increase dose, change agent, psychotherapy
Full response- continue for 4-9 months or indefinite
3rd line- TCAs, MAOIs, misc, augmenting agents

Question 112

St. Johns Wort

Answer 112

Modest efficacy
TID
Induces multiple CYP enzymes
ADRs- N/V/D, photosensitivity, sexual dysfunction
Just put them on an SSRI instead

Question 113

A-adenosyl methionine (SAMe)

Answer 113

Low/modest efficacy in depression

ADRs include dizziness, dry mouth, constipation, insmonia

Question 114

L-methylfolate in depression

Answer 114

Prescribed medical food
Well tolerated, mixed efficacy
Adjunt in MTHFR polymorphism

Question 115

Omega 3 fatty acids in depression

Answer 115

Safe

Low efficacy

Question 116

Vitamin D in depression

Answer 116

Deficiency more common in depressed patients

Efficacy is mixed, does not prevent depression

Question 117

Classes of antidepressants

Answer 117

SSRIs
SNRIs
NDRIs
NaSSa
ASRIs/SPARI
TCAs
MAOIs
Misc.

Question 118

STAR*D trial

Answer 118

The largest, longest duration controlled trials ever conducted to study depression.
Studied patients in multiple settings and in multiple phases of treatment.
Level one- start with citalopram and then add additional agents or switch if necessary

Question 119

BBW for all drugs approved for MDD

Answer 119

Increased risk of suicidality

Question 120

Serotonin syndrome

Answer 120

Applies to any agents with serotonergic properties
Potentially life threatening
Management- remove offending agent, 5-HT2A antagonists (cyproheptadine)

Question 121

Serotonin syndrome triad

Answer 121

Mental status changes, autonomic instability, neuromuscular abnormalities

Question 122

Serotonin syndrome s/s

Answer 122

Mental status changes- agitation, pressured speech
Autonomic instability- tachycardia, diarrhea, shivering, diaphoresis, mydriasis
Neuromuscular abnormalities- Clonus, hyperreflexia tremor, seizure

Question 123

Anti-depressant withdrawal

Answer 123

Agents should be tapered over weeks if able (except fluoxetine, it self tapers)
Abrupt d/c can precipitate withdrawal syndrome
Flu-like symptoms
Insomnia
Nausea
Irritability
Sensory disturbance
HA
(FINISH)

Question 124

Serotonin selective reuptake inhibitors (SSRI) MOA

Answer 124

Inhibition of reuptake of serotonin in the presynaptic neuron of the CNS.

Question 125

When to use SSRIs

Answer 125

1st line agent for MDD

Low risk of toxicity in overdose

Question 126

SSRIs agents

Answer 126

Fluvoxamine
Fluoxetine
Paroxetine
Escitalopram
Citalopram
Sertraline

Question 127

Citalopram dosing

Answer 127

10-40mg QD

*max 20mg if >60 years old, significant hepatic impairment, and 2C19 PM

Question 128

Which SSRI has the longest T1/2?

Answer 128

Fluoxetine
4-6 days T1/2
Metabolite in 4-16 days

Question 129

SSRIs: sexual dysfunction

Answer 129

Very common, about 1/3 of patients
Decreased libido, delayed ejaculation, anorgasmia
Treatment strategies- wait before changing therapy as tolerance may develop, use sildenafil for erectile problems, add bupropion, mirtazapine, buspirone

Question 130

Which SSRI causes sexual dysfunction most commonly?

Answer 130

Paroxetine

Question 131

SSRIs AE

Answer 131

N/V/D
Insomnia
Fatigue/sedation
Weight gain
Diaphoresis
Seizures
SIADH (rare)
Anxiety/agitation in early treatment
Risk of bleeding- increased with other antiplatelet therapy added

Question 132

Which SSRI causes insomnia the most?

Answer 132

Fluoxetine

Question 133

Which SSRI causes N/V/D the most?

Answer 133

Sertraline

Question 134

Which SSRI causes fatigue the most

Answer 134

Paroxetine

Question 135

Which SSRI causes weight gain the most?

Answer 135

Paroxetine

Question 136

Paroxetine-specific SSRI AE

Answer 136

Anticholinergic effects (avoid in elderly)

Question 137

Citalopram-specific SSRI effect

Answer 137

QTc prolongation

Do not give more than >40mg/day or 20mg if >60 years old

Question 138

SSRIs DDI

Answer 138

All SSRIs:
MAOIs- hypertensive crisis, serotonin syndrome. Linezolid also has MAOI effects.
Triptans, sibutramine- serotonin syndrome
NSAIDs, antiplatelets, anticoagulants- bleeding risk

Fluoxetine, paroxetine- Potent CYP2D6 inhibition, may increase conc of tricyclic antidepressants, may interfere with tamoxifen treatment

Fluvoxamine- CYP1A2 potent inhibition

Question 139

Serotonin/NE Reuptake Inhibitors (SNRIa) MOA

Answer 139

Inhibit both serotonin and NE presynaptic reuptake
More specific to NE-5HT than TCAs (better safety and tolerability)
1st line

Question 140

SNRI agents

Answer 140

Levomilnacipran
Duloxetine
Venlafaxine
Desvenlafaxine

Question 141

SNRIs AE

Answer 141

All:
N, dizziness, insomnia, sedation, constipation, sexual dysfunction, urinary retention, risk of SIADH
Dose related increase in diastolic BP

Question 142

Which SNRIs do you have to caution with uncontrolled narrow angle glaucoma?

Answer 142

Duloxetine, Levomilnacipran

Question 143

Which SNRI has the most pronounce increase in diastolic BP?

Answer 143

Venlafaxine and desvenlafaxine

Question 144

Which SNRI has risk of tachycardia?

Answer 144

Levomilnacipran

Question 145

Which SNRI has risk of rare interstitial lung disease?

Answer 145

Venlafaxine, desvenlafaxine

Question 146

Duloxetine-specific SNRI AE

Answer 146

More anticholinergic AE, urinary retention

Increases risk of hepatotoxicity, esp with ETOH

Question 147

SNRIs DDI

Answer 147

All-

serotonin syndrome, bleeding risk

Question 148

Duloxetine DDI

Answer 148

Substrate of CYP 1A2, 2D6

Inhibitor of 2D6

Question 149

Venlafaxine DDI

Answer 149

Substrate of 3A4, 2D6

Question 150

Levomilnacipran DDI

Answer 150

Substrate of 3A4`

Question 151

Norepinephrine dopamine reuptake inhibitor (NDRI) agent

Answer 151

Bupropion

Question 152

Bupropion MOA and use

Answer 152

1st line, augmenting agent
MOA: Inhibits reuptake transporters of synaptic dopamine, NE
Has NO serotonin effects

Question 153

Bupropion AE

Answer 153

N, V, weight loss, tremor, insomnia, xerostomia, HTN

Low risk of sexual dysfunction

Question 154

Bupropion DDI

Answer 154

MAOIs- HTN crisis
Seizure threshold lowering agents, beta lactam abx, alcohol, antipsychotics
CYP2B6 substrate, 2D6 inhibitor

Question 155

Bupropion contraindications

Answer 155

Seizure disorder
High alcohol/benzo intake
Bulimia, anorexia

Question 156

Noradrenergic and specific serotonergic antidepressant (NASSA) agent

Answer 156

Mirtazapine

Question 157

Mirtazapine MOA and use

Answer 157

1st line with compelling reason

MOA: antagonizes presynaptic a-2 adrenergic receptors (increase NE, serotonin) , H1 receptor antagonist

Question 158

Mirtazapine ADR

Answer 158

sedation, increased triglycerides, dry mouth, sexual dysfunction, appetite stimulation

Question 159

Vortioxetine MOA

Answer 159

1st line agent

SSRI with 5-HT1A agonism, mixed antagonist/partial agonist

Question 160

Vortioxetine AE

Answer 160

Nausea, constipation, vomiting, sexual dysfunction

Question 161

Vortioxetine DDI

Answer 161

CYP2D6 primary substrate- dose adjustment

Wait 21 days before starting MAOI (long t1/2)

Question 162

Serotonin antagonist/reuptake inhibitor (SARI) agents

Answer 162

trazodone, vilazodone

Question 163

Trazodone use and MOA

Answer 163

3rd line/ augmenting (d/t sedation)

MOA: Antagonist at post-synaptic 5HT2, inhibits reuptake of serotonin

Question 164

Trazodone AE

Answer 164

Sedation, dizziness, orthostatic hypotension

Priapism

Question 165

Trazodone DDI

Answer 165

Similar to SSRIs

Trazodone is 3A4 substrate

Question 166

Vilazodone use and MOA

Answer 166

MOA- SSRI and 5-HT receptor PARIAL agonist (SPARI)
Newer, less data
3rd line

Question 167

Vilazodone ADR

Answer 167

GI: Diarrhea, N, V, xerostomia
Neurologic: dizziness, insomnia
CYP3A4 substrate

Question 168

Tricyclic antidepressants use and MOA

Answer 168

3rd line for MDD
MOA: Inhibits reuptake of NE and 5-HT
Antagonizes histamine, alpha-adrenergic and muscarinic receptors, cardiac sodium channels (AE)

Question 169

Why has use fallen out of favor with TCAs?

Answer 169

OD can occur with a 1 week supply

Poor tolerability

Question 170

TCA agents

Answer 170

Amitripyline
Imipramine
Doxepin
Clomipramine
Maprotiline
Protriptyline
Desipramine
Nortriptyline

Question 171

TCA AE

Answer 171

Sedation
Decreased seizure threshold
CV events- orthostatic hypotension/syncope, arrhythmias
Sexual dysfunction
Tremor
Photosensitivity
Heat intolerance
Risk of seizure

Question 172

Anticholinergic effects of TCAs

Answer 172

Cholinergic rebound

Drying effects: SLUD

Question 173

Anti-histaminic effects of TCAs

Answer 173

Weight gain

Sedation

Question 174

Alpha-1 adrenergic effects of TCAs

Answer 174

Orthostasis
Hypotension
Dizziness

Question 175

TCA DDI

Answer 175

CNS depressants
QT prolonging agents
alpha-adrenergic blockers (increases hypotension)
Serotonin syndrome
CYP interactions: 
2D6 substrates (except comipramine)
2C19 substrates (nortriptyline, doxepin)
1A2 substrate: clomipramine

Question 176

Monoamine oxidase inhibitors (MAOIs) moa and use

Answer 176

3rd+ line for MDD
MOA: Inhibition of MAOa and MAOb causing increased concentrations of NE, 5-HT, and dopamine in neuronal synapse
Infrequently used

Question 177

MAOI agents

Answer 177

Tranylcypromine
Isocarboxazid
Phenelzine
Selegiline

Question 178

MAOI AE

Answer 178

Hypotension, dizziness common
Anticholinergic AE
Sedation or insomnia
HA
Sexual dysfunction
Cautions in cardiac disease, hepatic impairment
Contraindicated with pheochromocytoma

Question 179

MAOIs food interactions

Answer 179

Hypertensive crisis:
Food interaction from MAO-a inhibition in GI- excess of tyramine
Symptoms: stiff neck, HA, n, v, diaphoresis, increased BP
Dietary tyramine- cheese, wine, beer, fermented foods, MSG, coffee, chocolate
ALL MAOIs except selegiline patch

Question 180

MAOIs DDI

Answer 180

Serotonin syndrome- 2 week washout when changing to/from MAOI (5 weeks for fluoxetine, 3 weeks for vortioxetine)
Increased BP= stimulants, sympathomimetics *epinephrine, albuterol, decongestants

Question 181

MAO regeneration

Answer 181

14 days

Question 182

Esketamine

Answer 182

Intranasal jetamine
Used for augmentation in severe depression that has failed 2 trials of antidepressants
REMS program- must be administered by registered clinician and monitored for 2 hours after

Question 183

Antipsychotics in depression

Answer 183

FDA approved agents for augmentation- aripiprazole, brexpiprazole, olanzapine, quetiapine XR

Question 184

Additional depression augmenting agents

Answer 184

Stimulants

Buspirone

Question 185

Pharmacogenomics in depression

Answer 185

Polymorphisms in 2D6, 2C9, and 2C19 may affect medication levels
Short S or long L in 5-HT transporters, alterations in expression of BDNF and tryptophan hydroxylase may alter antidepressant response

Question 186

Depression in pregnancy

Answer 186

SSRIs most common (AVOID paroxetine)
SNRI
TCAs less frequently used, but has more data
Augmenting agents- mirtazapine, bupropion, antipsychotics

Question 187

AE of brexanolone

Answer 187

Presyncope, drowsiness, sedation, dizziness, xerostemia
BBW: Impairment/loss of consciousness
REMS required

Question 188

Depression drugs effects on lactation

Answer 188

Risk of AE from breastfeeding low
Some cases of somnolence with citalopram
Bupropion may decrease milk supply
“pump and dump” not recommended

Question 189

Pediatrics and adolescents depression agents

Answer 189

Start LOW and SLOW
recommend f/u in 1 week
Within 6 weeks change therapy if not effective

Question 190

Depression in elderly

Answer 190

More physical symptoms- insomnia, pain
Less likely to respond to therapy
Low and slow
ECT is safe
SSRIs first line (avoid paroxetine, citalopram dose restriction)
Stimulants (methylphenidate) may help

Question 191

Which drugs are 1st line in depression?

Answer 191

SSRIs

Question 192

Is delirium reversible?

Answer 192

Yes

Question 193

Delirium

Answer 193

Disturbance of consciousness, attention, cognition, and perception.
Develops over a short period of time (hours to days)
Tends to fluctuate during the course of the day.

Question 194

DSM5 criteria for delirium

Answer 194

Alteration in attention and awareness
The alteration is abrupt and fluctuates throughout the day
There is also an alteration in cognition
Alterations are not better accounted for by any other disorder.
There is physical evidence that the alteration is caused by a medical condition, substance, or variety of causes

Question 195

Where is delirium found?

Answer 195

Hospital
Long term care
ER
Palliative care 
Hospice

Question 196

How common is delirium in patients > 65 years old

Answer 196

50% of patients

Question 197

Where is delirium most common?

Answer 197

ICU

Question 198

Consequences of delirium

Answer 198

More than doubles mortality rate
Increases LOS by 2-5 days
1 in 3 patients have some residual cognitive impairment
Common cause of new institutionalization (delirium and incontinence most common causes)

Question 199

Confusion assessment method (CAM)

Answer 199

Must have acute fluctuation course and inattention

And disorganized thinking or LOC

Question 200

Delirium S/S

Answer 200

Disturbed attention
Fragmented sleep
Memory impairment
Disoriented to time and place
Abrupt altered change in consciousness can be hyper or hypoactive

Question 201

Types of delirium

Answer 201

Hyperactive
Hypoactive
Mixed

Question 202

Symptoms of hyperactive delirium

Answer 202

Restlessness, agitation, hallucinations, delusions

Question 203

Which type of delirium is most common in the elderly?

Answer 203

Hypoactive or mixed.

Often unrecognized

Question 204

S/S of hypoactive delirium

Answer 204

Lethargy, sedation, slow response and movement

Question 205

Dementia vs delirium

Answer 205

Dementia- insidious onset, gradual deterioration
Awareness is often clear until advanced stages in dementia
Dementia pts do not have hallucinations or delusions until late stage
Dementia patients have reversed sleep cycles.

Question 206

Depression vs delirium

Answer 206

Depression- onset takes a while to develop.
Patients have low mood, does not fluctuate.
Depression is chronic
ADL- compromised in patients with depression

Question 207

Sundowning

Answer 207

Dysfunction of circadian rhythm
Behaviors that occur in the evening- confusion, agitation, pacing/wandering, increased verbal activity
Management- proper sleep hygiene. trazodone, melatonin

Question 208

Risk factors for delirium

Answer 208

H/O ETOH use
Age >70
Kidney or liver disease
Poly pharmacy (>6 meds)
Sensory impairment
Dementia, depression, underlying brain disease, previous delirium

Question 209

Pharmacology of drug induced delirium

Answer 209

Dopamine activation

Cholinergic inhibition

Question 210

What causes delirium?

Answer 210

Dementia and drugs
Electrolytes/Eyes, ears other senses
Lungs, liver, kidney, brain, heart
Infection
Retention
Injury
Unfamiliar environment
Metabolic
Sleep

Question 211

What electrolytes cause delirium

Answer 211

Hyponatremia

Hypercalcemia

Question 212

Anticholinergic drugs and delirium

Answer 212

TCAs (amitriptyline)
Antihistamines
Incontinence agents- tolterodine, oxybutynin
Antipsychotics- olanzapine

Promethazine
Digoxin
Skeletal muscle relaxants
Paroxetine
benztropine
Cefepime, quinolones, imipenem, linezolid

Question 213

Psychotropics

Answer 213

Lunesta, belsomra, sonata, ambien
Benzos
Antidepressants

Question 214

Other medication causes of delirium

Answer 214

Metoclopramide
Steroids
H2RAs
all antihypertensives and diuretics
Drug withdrwaawl
Antiarrhythmics
NSAIDs

Question 215

Opioids and delirium

Answer 215

Highest risk-codeine, tramadol

All others have risk

Question 216

Prevention of delirium

Answer 216

Ensure sensory aids
Encourage hydration, mobility, senses intact
Maintain sleep pattern
Avoid sedation, catheters, loud noices

Question 217

Management of delirium principles

Answer 217

Treat underlying cause
D/C any new medication added if no clear cause.
Non pharm management is critical.
Antipsychotics are DOC, but no drug is FDA approved for delirium

Question 218

Evaluation of delirium

Answer 218

BMP, ammonia and calcium
CBC
Urinalysis
B12
TSH
Tox screen
Vital signs
O2 saturation

Question 219

Non pharm delirium tx

Answer 219

Family involvement, sitter, normalize sleep-wake cycle, sensory evaluation, music, remove catheters, mobilize pt, avoid restraints, hydration and nutrition

Question 220

Medication tx of delirium hyperactive

Answer 220

Haloperidol, olanzapine, quetiapine
BBW- 7 days or less
Use only when delirium puts patients at risk to themselves or others

Question 221

Haloperidol for delirium

Answer 221

First line, especially if severe
Low doses Q 4 H
QTc prolongation
More effective in pts halllucinatinf

Question 222

Olanzapine for delirium

Answer 222

More sedating than haloperidol, but less likely to cause EPS

Question 223

Quetiapine in delirium

Answer 223

More appropriate for mild delirium
More sedating than haloperidol
Safest in parkinsons disease

Question 224

Acetylcholinesterase inhibitors in delirium

Answer 224

Consider with patients who have dementia

Question 225

Benzos in delirium

Answer 225

Only use for alcohol withdrawal or parkinsons related delirium

Question 226

Valproic acid in delirium

Answer 226

Appropriate for patients with underlying behavioral manifestations of dementia.
Not for acute delirium

Question 227

SAR of benzodiazepines

Answer 227

Aromatic ring
Electronegative electron withdrawing group (Cl, F, nitro)
Phenyl group- increases activity
Carbonyl or H-bond acceptor (could also be NH)
Hydroxyl group= shorter duration of action