Exam 5 Flashcards

Question 1

Q

Donepezil brand and class

Answer

A

Aricept

Acetylcholinesterase inhibitor

Question 2

Q

Memantine brand and class

Answer

A

Namenda

NMDA receptor antagonist

Question 3

Q

Alzheimer’s disease characteristics

Answer

A

Insidious onset
Neurocognitive deficits prominent
60-80% of cases

Question 4

Q

Alzheimer’s disease treatment options

Answer

A

Acetylcholinesterase inhibitors

NMDA receptor antagonist

Question 5

Q

Vascular dementia characteristics

Answer

A

Deficits occur in correlation with cerebrovascular accident.
Attention deficits prominent.

Question 6

Q

Vascular dementia treatment options

Answer

A

Modifying risk factors

Less evidence for cognitive enhancers

Question 7

Q

Dementia with Lewy bodies characteristics

Answer

A

Insidious onset
Core features (motor features and hallucinations)
Suggestive features (sleep behaviors, sensitivity to antipsychotics)

Question 8

Q

Dementia with Lewy bodies treatment options

Answer

A

AChEIs, NMDA antagonist

Dopamine agonists or antagonists, based on sx

Question 9

Q

Dementia with Lewy bodies treatment options

Answer

A

AChEIs, NMDA antagonist

Dopamine agonists or antagonists, based on sx

Question 10

Q

Frontotemporal dementia characteristics

Answer

A

Younger age of onset

Umbrella diagnosis for significant behavioral, social, or language symptoms

Question 11

Q

Frontotemporal dementia treatment options

Answer

A

Antidepressants

Antipsychotics

Question 12

Q

Potential reversible causes of dementia

Answer

A

Drugs
Eyes/ears
Metabolic disorders
Emotional
Nutritional/Electrolytes
Tumors/ trauma/ thyroid
Infection
Alcohol

Question 13

Q

Drugs that may cause cognitive dysfunction

Answer

A

TCAs
Diphenhydramine
Muscle relaxants
Benzodiazepines 
Eszoplicone, zaleplon, zolpidem
Barbiturates
Promethazine

Question 14

Q

Alternative options to TCAs that do not cause cognitive dysfunction

Answer

A

SSRIs (avoid paroxetine)
SNRIs
Bupropion

Question 15

Q

Alternative options to diphenhydramine that do not cause cognitive impairment

Answer

A

Cetirizine, fexofenadine, loratadine

Question 16

Q

Alternative options to muscle relaxants that do not cause cognitive impairment

Answer

A

APAP, NSAIDs, heat, ice

Question 17

Q

Alternative options to benzodiazepines (for anxiety) that do not cause cognitive impairment

Answer

A

Buspirone, SSRI (avoid paroxetine), SNRI

Question 18

Q

Alternative options to eszopiclone, zaleplon, zolpidem that do not cause cognitive impairment

Answer

A

Low dose trazodone, low dose doxepin, ramelteon, melatonin

Question 19

Q

Alternative options to barbiturates that do not cause cognitive impairment

Answer

A

Low dose trazodone, low dose doxepin, ramelteon

Use lowest effective dose

Question 20

Q

Alternative options to promethazine that do not cause cognitive impairment

Answer

A

Dolasetron, granisetron, ondansetron

Question 21

Q

Alzheimer’s disease

Answer

A

60-80% of dementia
Cognitive defects which impact social or occupational functioning
Diagnosis of exclusion
Memory loss is predominant
Patient often unaware of symptoms

Question 22

Q

What is the difference between a healthy brain and a brain with Alzheimer’s?

Answer

A

A brain with Alzheimer’s has plaques and a diseased and tangled neuron

Question 23

Q

Neurotransmitters involved in Alzheimer’s disease

Answer

A

Multiple neuronal pathways are destroyed, mass neurotransmitter deficits
Loss of choline acetyltransferase and acetylcholinesterase.
In moderate to severe AD- excessive glutamate which enhances cellular death

Question 24

Q

Genetic risk factors of Alzheimer’s disease

Answer

A

Family history- 1st degree relative increases risk
Apolipoprotein E (APOE)*4 Gene
-Everyone inherits *2, *3, or *4 from each parent. *4 increases late-onset AD risk
Early onset AD- presenilin 1 and 2 (PSEN1), Amyloid precursor protein (APP)

Routine testing not recommended at this time

Question 25

Q

Risk factors of Alzheimer’s disease

Answer

A

Dyslipidemia
Obesity
Diabetes
HTN
Smoking
Depression
Trisomy 21
TBI

Question 26

Q

AD timeline

Answer

A

Early brain changes
Subtle decline in thinking
Memory changes, confusion
Loss of activities in daily living (ADLs)
Loss of communication and social recognition

Question 27

Q

Screening of AD

Answer

A

US preventive Services Task Force: insufficient evidence to recommend for or against routing screening for dementia
Cognitive assessments- MINI-COG, Mini-mental state exam

Question 28

Q

Mini-Cog

Answer

A

AD scale
Score of 3, 4, or 5 indicated low likelihood of dementia
Components: 
1.) Repeat 3 unrelated words directly. 
2.) Draw a clock face showing 11:10
3.) Recall previous 3 unrelated words

Question 29

Q

Mini-Mental State Exam (MMSE)

Answer

A

AD scale
Score 0-30, lower numbers indicate greater impairment
>27 considered normal
Score 9-0= severe
Score 23-18= Mild

Tests orientation to time, place, registration repeat, serial 7s or spell “world backwards, registration recall, Gnosia (recognition), repetition, complex commands

Question 30

Q

Montreal Cognitive Assessment (MoCA)

Answer

A

AD scale
Score 0-30, lower numbers indicate greater impairment
>26 is considered normal cognition

Question 31

Q

Saint Louis University Mental Status Examination (SLUMS)

Answer

A

AD scale
Score 0-30, lower numbers indicate greater impairment
>27 is considered normal cognition

Question 32

Q

Slowing and managing progression of AD

Answer

A

Medications- pharmacological management
Avoiding cognitive dysfunction promoters.
Disease states- BP, lipid, glucose management
Education- pt and family support, expectations, legal/financial planning

Question 33

Q

AD treatment strategy

Answer

A

Start low and go slow
Success= decline in MMSE of <2points/year
-If decline is >3 points after 1 year, use alternative treatment
Consider washout period of 1 week if alternating agents

Question 34

Q

Nonpharm management for AD

Answer

A

Patient-centered focus
Create a low stress environment
Simple activities and exercise
Therapy animals
Avoid challenging beliefs/memories ("arguing" may be distressing

Question 35

Q

Complementary alternative options for AD

Answer

A

Prevagen (Apoaquorin)
Vitamin E
Ginkgo biloba
Caprylic acid
Huperzine A
Omega-3 fatty acids (linked to reduction in cognitive decline)
Axona (medical food that forms ketone bodies to reduce glucose use in brain)

Question 36

Q

Prevagen

Answer

A

Proposed mechanism is to protect neuronal cells from calcium-mediated toxicity by promoting calcium homeostasis.
High rate of publication bias
10mg in 90 days appears safe, may improve cognitive function in older adults without dementia
ADR- HA, dizziness, nausea

Question 37

Q

Vitamin E

Answer

A

Proposed mechanism: protects against oxidative stress and free radicals
No-low efficacy
ADR: bleeding risk, nausea, diarrhea, fatigue
Doses >400 IU/day associated with increased risk of prostate cancer, HF, mortality, hemorrhagic stroke

Question 38

Q

Ginkgo Biloba

Answer

A

Proposed mechanism: improve brain blood flow and mitochondrial function
Does not improve cognitive decline or AD
Publication bias likely
ADRs: bleeding risk, dizziness, diarrhea

Question 39

Q

Pharmacotherapy for cognitive symptoms of AD

Answer

A

Amyloid-beta antibody (Aducanumab )
Acetylcholinesterase inhibitors (Donepezil, Rivastigmine, Galantamine)
NMDA receptor antagonist- memantine
Combo- memantine/donepezil

Question 40

Q

Aducanumab-avwa

Answer

A

Approved in 2021 ONLY for patients with mild cognitive impairment or mild dementia
Very controversial- studies demonstrate reduction in amyloid buildup, however effectiveness unclear

Question 41

Q

Aducanumab dose and monitoring

Answer

A

IV infusion every 4 weeks
Monitoring: recent MRI prior to tx
F/U MRI prior to 7th and 12th infusion
Reason: microhemorrhages and/or focal superficial siderosis
Monitor ARIA (amyloid related imaging abnormalities)
-Edema, microhemorrhage, superficial siderosis

Question 42

Q

Aducanumab ADR

Answer

A

HA, fall, angioedema, urticaria

Question 43

Q

How are AChEIs thought to decrease symptom progression of AD?

Answer

A

AD is associated with neuronal death, resulting in reduced promotion of ACh. AChEIs are thought to slow the breakdown of ACh to compensate for the loss.

Question 44

Q

How is Namenda XR believed to delay symptom progression of AD?

Answer

A

AD causes sustained activation of NMDA receptors which may lead to excessive calcium influx, neuronal dysfunction, and cell death.
Namenda XR is believed to block sustained activation of NMDA receptors caused by abnormal glutamatergic activity.

Question 45

Q

Which FDA approved AD therapy is used for mild to moderate disease?

Answer

A

Adacanumab
Donepezil
Galantamine
Rivastigmine

Question 46

Q

Which FDA approved AD therapy is approved for moderate to severe disease?

Answer

A

Donepezil
Rivastigmine
Memantine
Memantine/Donepezil

Question 47

Q

Donepezil MOA and indication

Answer

A

Acetylcholinesterase inhibitor

Indicated for mild to severe AD

Question 48

Q

Donepezil dosing/admin

Answer

A

Take at bedtime without regard to food.
Aricept 23mg tab- do not crush or chew
ODT- dissolve on tongue and follow with water
May increase from 5mg to 10mg after 1 month

Question 49

Q

Donepezil interactions

Answer

A

Monitor for clinical response or ADR change in strong CYP3A4 inducers/ inhibitors

Question 50

Q

Rivastigmine MOA and indication

Answer

A

Acetylcholinesterase inhibitor

Indicated in mild to moderate AD (oral), mild to severe AD (patch) and Parkinsons dementia

Question 51

Q

Rivastigmine dosing/admin

Answer

A

Take WF
<6mg PO= 4.6 mg patch
6-12 mg PO= 9.5mg patch
Adjust every 2-4 weeks, retitrate if 3+ day interruption
Nicotine increases clearance by 23%

Question 52

Q

Galantamine MOA and indication

Answer

A

Acetylcholinesterase inhibitor

Indicated for mild to moderate AD

Question 53

Q

Galantamine dosing/admin

Answer

A

Take WF
Oral solution: mix with 3-4 oz of any nonalcoholic beverage and drink immediately
Titrate monthly and retitrate if 3+ day interruption
Avoid if CrCl <9mL/min
If CrCl 9-59= max dose 16mg/d

Question 54

Q

Galantamine DDI

Answer

A

Monitor for toxicity in 2D6/ 3A4 inhibitors

Question 55

Q

AchEI ADRs: GI

Answer

A

NVD, anorexia, weight LOSS

Peptic ulcer disease/GI bleed

Question 56

Q

AchEI monitoring

Answer

A

Monitor for GI complaints, weight loss, bleeding, NSAID use

Monitor for dizziness, falls, HR, BP

Question 57

Q

AchEI ADRs: CNS/CV

Answer

A

Dizziness, syncope, bradycardia, atrial arrhythmias, MI, seizures, SA and AV block, QT prolongation
Abnormal dreams, sleep disturbances
Routing HR checks at baseline, monthly during titration, and then Q 6 months

Question 58

Q

Memantine MOA and indication

Answer

A

NMDA receptor antagonist

Indicated for moderate to severe AD (NOT mild)

Question 59

Q

Memantine dosing/admin

Answer

A

Take without regard to food
Oral solution- slowly squirt into corner of mouth, do NOT mix with any other liquid, ER cap may be sprinkled on applesauce
Titrate weekly
If CrCl <29 mL/min, IR up to 5 mg BID, ER up to 14mg/day

Question 60

Q

Memantine interactions

Answer

A

Urine alkalinizers decrease clearance of memantine if urinary pH 8 or more

Question 61

Q

Memantine ADR

Answer

A

CNS- HA, confusion, dizziness, hallucinations

GI- diarrhea, constipation

Question 62

Q

Memantine monitoring

Answer

A

Monitor dizziness or falls, hallucinations

Monitor bowel movements

Question 63

Q

Memantine/Donepezil MOA and indication

Answer

A

Combo of NMDA receptor antagonist and AchEI

Indicated for moderate to severe AD in patients stabilized on memantine and donepezil

Question 64

Q

Memantine/Donepezil dosing/admin

Answer

A

Take at bedtime w/o regard to food
May be sprinkled on applesauce
If CrCl <29, use memantine ER 14mg formulation

Answer 65

A

Baseline cognitive status, physical status, functional performance, behavior
Monitor 2 and 3 months after therapy initiation (if 3 months on max tolerated AChEI ineffective, consider switch)
Monitor at least q 6 months thereafter
Treatment duration unclear

Answer 66

A

Noncognitive symptoms- depression, psychosis
Treatment of psychotic or behavioral symptoms should include environmental interventions and meds only if necessary
Asses underlying causes- meds, medical illness, environment, abuse, unmet needs

Answer 67

A

Experienced by up to 90% of pts

More common in later stages of disease

Answer 68

A

Delusions, hallucinations, depression, anxiety, euphoria, sexually inappropriate behavior, aggression, apathy, irritability, disinhibition, wandering, sleep disturbances

Answer 69

A

Patient with need, unmet or unnoticed by caregiver, acting out behavior
Environmental stressor, diminished stress-tolerance, behavior

Answer 70

A

Ensure the patient and staff/caregiver are safe
Compare behaviors to baseline
Investigate reversible causes- delirium, ADR, other
Evaluate for precipitating factors

Answer 71

A

Ensure the patient and staff/caregiver are safe
Compare behaviors to baseline
Investigate reversible causes- delirium, ADR, other
Evaluate for precipitating factors

Answer 72

A

First line
Psychosocial approach- activities of interest, social interactions, comfort
CBT- milder disease and comorbid depression

Answer 73

A

Haloperidol, aripiprazole, risperidone all have most evidence
Olanzapine, Quetiapine alternatives
Shortest duration, lowest effective dose, monitor closely

Answer 74

A

risk of death

Answer 75

A

Risk of movement disorders-pseudoparkinsonism, tardive dyskinesia, dystonia, akathisia, risperidone, haloperidol, quetiapine, olanzapine
Risk of QTc prolongation and CV events- IV haloperidol
Risk of hypotension and syncope

Answer 76

A

Always try nonpharm first
Reserve for cases where behavioral disturbances put pt or caregiver at risk.
Re-evaluate need regularly
Rarely use for >12 weeks

Answer 77

A

DA theory- hyperactive mesolimbic DA and hypoactive mesocortical DA systems. DA releasing agents can cause psychosis

Glutamate theory-NMDA receptor hypofunction. Ketamine and PCP block NMDA receptors and produce psychosis

Serotonin theory: 5-HT2A receptor hyperactivity in cortex. LSD is a 5HT2A agonist and produces psychosis

Answer 78

A

Phenothiazines- chlorpromazine, fluphenazine
Thioxanthenes- thiothixene
Butyrophenones-haloperidol, benperidol

Answer 79

A

2nd gen

Clozapine, olanzapine, risperidone, quetiapine, ziprasidone, aripiprazole

Answer 80

A

1st gen (typical) antipsychotics referred to as neuroleptics. They decreased nerve function, major tranquilizer.
MOA- blockage of D2 dopamine receptors. Drugs antagonize the behavioral and biochemical effects of DA.

Answer 81

A

Produced by 1st gen antipsychotics
Suppression of spontaneous movements, reduction in initiative and interest, reduced emotion
Patients still are easily aroused and have intellectual faculties

Answer 82

A

> 60% D2 receptors needed for clinical improvement

Differences in potency but not in efficacy

Answer 83

A

Acute: DA receptor blockade results in blockade of DA mediated effects, receptor blockade results in compensatory increase in DA neuronal firing.

Chronic effects: DA receptor super-sensitivity, depolarization inactivation. Reduction in active DA neurons.

Answer 84

A

Function: normal in patients. control of movement
Drug effect: D2 receptor blockade results in extrapyramidal symptoms (parkinsonism) and tardive dyskinesia
EPS is acute, tardive dyskinesia is chronic
Terminates in basal ganglia

Answer 85

A

Function: hyperactivity related to psychosis and positive symptoms, reward pathway
Drug effect: D2 receptor blockade and depolarization (inactivation) blockade would reduce positive symptoms. But also may cause secondary negative symptoms (apathy, lack of motivation). Blocks reward pathway.
Terminates in nucleus accumbens

Answer 86

A

Function: hypofunction may be related to impaired cognition
Drug effect: DA receptor blockade may worsen negative symptoms
Terminates in frontal cortex

Answer 87

A

Function: normal in pts. DA inhibits prolactin secretion
Drug effect: D2 receptor blockade would elevate serum prolactin levels. Breast enlargement, fertility issues, milk production
Terminates in hypothalamus

Answer 88

A

Many are related to DA receptor blockade
EPS: parkinsonism, dystonias, akathisia (due to DA blockade in basal ganglia)
Tardive dyskinesia- late occurring oral-facial movements. May be due to DA receptor supersensitivity.
Increased prolactin levels
Neuroleptic malignant syndrome

Answer 89

A

Selective inhibitor of the pre-synaptic human VMAT2.
FDA approved for tx of tardive dyskinesia
Impaired VMAT2 leads to reduced DA storage, increased intraneuronal DA metabolism. Resulting in depletion of intraneuronal DA and less release and less receptor activation

Answer 90

A

alpha1
D2
H1
M1
5-HT2C

Answer 91

A

Dizziness, orthostatic hypotension, reflex tachycardia

Answer 92

A

Extrapyramidal side effects, increased prolactin levels

Answer 93

A

Sedation, weight gain

Answer 94

A

Blurred vision, constipation, dry mouth

Answer 95

A

Weight gain

Answer 96

A

Atypical has low EPS, including tardive dyskinesia. Able to maintain efficacy while decreasing EPS compared to 1st gen.
Mechanistic diff in 5-HT2A receptor antagonism (5-HT2/D2 antagonists, D2/5-HT1A partial agonists)
Clozapine is uniquely effective in treatment resistant schizophrenics

Answer 97

A

Pines, dones, and a rone, two pips and a rip

Answer 98

A

5-HT2A/D2 antagonists (pines, dones, and a rone)

DA2/5-HT1A partial agonists (two pips and a rip)

Answer 99

A

Agents have a higher affinity for 5-HT2A vs D2 receptors
pines, dones, and a rone
clozapine, olanzapine, quetiapine, asenapine, ziprasidione, lurasidone, risperidone, iloperidone, palidperidone, lumateperone

Answer 100

A

Two pips and a rip

Aripiprazole, Brexipiprazole, Cariprazine

Answer 101

A

Short term- activated neurons

Long-term= inactivated neurons- depolarization inactivation

Answer 102

A

Short term- receptor blockade- motor AE

Long term- receptor super-sensitivity, tardive dyskinesia

Answer 103

A

dizziness, orthostatic hypotension, reflex tachycardia

Answer 104

A

EPS, increased prolactin levels

Answer 105

A

Sedation, weight gain

Answer 106

A

Blurred vision, constipation, dry mouth

Answer 107

A

weight gain

Answer 108

A

5-HT1A agonism achieves the same outcome as 5-HT2A antagonism, it opposes effects of D2 receptor blockade in striatum and cortex.
Increases nigrostriatal DA release (diminishing EPS)
Increases mesocortical DA release, improving negative symptoms

Answer 109

A

DA system stabilizer- in the case of too much DA, acts as an antagonist. In the case of too little DA, acts as an agonist.
Unique MOA- activation of presynaptic DA receptors. D2 antagonist in hyperdopaminergic states and D2 agonist in hypodopaminergic states.
5-HT1A partial agonist, possible 5-HT2B antagonist

Answer 110

A

Weak D2 antagonist; stronger 5-HT2 antagonist
D2/5-HT1A partial agonists
Little/No DA receptor super sensitivity with chronic admin
Selective depolarization inactivation of mesolimbic DA neurons.
Fast dissociation from D2 receptors.
Increase DA, ACh, and NE release in cortex

Answer 111

A

Low EPS
Low tardive dyskinesia
Less hyperprolactinemia (except risperidone)
Doesnt worsen (may improve) negative symptoms

Answer 112

A

Recent studies show that concomitant treatment with the opioid antagonist samidorphan lessens weight gain with olanzapine

Answer 113

A

5-HT2A inverse agonist
No D2 blockade
Approved for tx of hallucinations/ delusions in psychosis in PD, in trials for schizophrenia

Answer 114

A

Psychiatric disorder with persistent psychosis, impaired social functioning, and impaired occupational functioning.

Answer 115

A

Prodrome- period before diagnosis with social isolation, lack of energy, worry, inattentiveness
Age- late teens to early 30s for diagnosis
Sex- about equal, but male onset is earlier

Answer 116

A

Significantly higher mortality rates than general population- CV disease, cancer, accidents, suicides
Higher rates of smoking
Chronic disease requiring life long therapy
Course of relapse and remission varies between patients

Answer 117

A

Largely unknown
Fetal insults during pregnancy (infection, fetal distress, etc.)
Infections and autoimmune inflammatory processes
Cannabis use in youth/adolescence
Higher in urban areas/ low socioeconomic process (may be due to social drift)
Genetic correlation

Answer 118

A

2 or more symptoms, each present for a significant amount of time during a 1 month period. One of the symptoms must be delusions, hallucinations, or disorganized speech
Social/occupational dysfunction
Duration- continuous signs >6 months, with at least 1 month being positive symptoms

Answer 119

A

Hallucinations, hostility, excitability, delusions, suspiciousness/persecution, conceptual disorganization, grandiosity

Answer 120

A

Schizoaffective/mood disorder

Answer 121

A

Delusions
Hallucinations
Disorganized thinking
Motor behaviors

Answer 122

A

Catatonia- alterations in environmental reactivity

Abnormal motor movements

Answer 123

A

Inferred from speech communication

Difficulty communicating due to lack of ability for the listener to understand the individual’s thought expression

Answer 124

A

Fixed, false beliefs
Persecutory, grandiose, somatic
Remain despite contrary evidence

Answer 125

A

Perceptive experience (any of the senses)
Exist despite a lack of external stimulus

Answer 126

A

Avolition
Affective flattening
Anhedonia
Asociality
Alogia

Answer 127

A

Enlarged ventricles
Reductions in total brain volume
Loss of gray matter in frontal cortex/temporal lobes

Answer 128

A

Glutamate- NMDA receptor dysfunction increasing limbic DA release, neurotoxicity
GABA- alterations in the prefrontal cortex affecting cognition
5-HT- transporter density increase, 5-HT2a antagonism increases DA release in prefrontal cortex.
Acetylcholine receptors-
nicotinic and muscarinic

Answer 129

A

Any antipshychotic could be considered 1st line except clozapine and lumateperone
Adequate trial- 2-6 weeks
After failure- switch to one of the above
Third line: clozapine, trial 12+ weeks
Beyond: augmenting clozapine, multiple agents, ECT

Answer 130

A

CBTp
Physcoeducation
Employment support, family support, and assertive community treatment
ECT
rTMS

Answer 131

A

DA D2 receptor blockade- leads to therapeutic effects and EPS
Muscarinic- M1 receptor blockade
Histaminic- H1 receptor blockade
Alpha- alpha 1 receptor blockade
Agents differ in potency and receptor affinity

Answer 132

A

Chlorpromazine
Fluphenazine
Haloperidol
Loxapine
Perphenazine
Trifluoperazine
Thioridazine
Thiothixene

Answer 133

A

Similar to 1st generation antipsychotics
Increase D2 receptor dissociation
Additional serotonin 5HT2a antagonism
Exception: aripiprazole, brexpiprazole, and cariprazine are partial agonists at D2 receptors.

Answer 134

A

Aripiprazole, brexpiprazole and cariprazine

Answer 135

A

Risperidone

Answer 136

A

Dopaminergic
Histaminic
Adrenergic
Muscarinic
Serotonergic

Receptors for schizophrenia

Answer 137

A

Therapeutic effects
EPS
Hyperprolactinemia

Answer 138

A

sedation, weight gain

Answer 139

A

Postural hypotension and reflex tachycardia

Answer 140

A

Antihcolinergic- dry mouth, constipation, urinary retention, blurred vision, decreased cognition

Answer 141

A

Reduced EPS, weight gain, modulation of dopamine release

Answer 142

A

Haloperidol
Fluphenazine
Thiothixene
Trifluoperazine

Increase prolactin, lost of EPS (DA effects)
Lower sedation AE

Answer 143

A

Perphenazine
Loxapine
Chlorpromazine
Thioridazine

Dry mouth, hypotension, sedation

Answer 144

A

Chlorpromazine, fluphenazine, haloperidol, thiothixene

Answer 145

A

Loxapine
FDA indicated for ACUTE treatment of agitation in schizophrenia/bipolar disorders in adults
BBW and REMS program- potential to cause respiratory distress. Do not use in any underlying respiratory illness.
ONLY use in facilities that can intubate/ventilate patients.

Answer 146

A

Lurasidone, Ziprasidone, lumateperone

Answer 147

A

Non compliance common- results in relapse, healthcare costs, morbidity
LAI may be effective in relapse prevention, prevention of illness worsening
Data suggests early use of LAI-APs benefit hospitalization and all-cause discontinuation

Answer 148

A

SL tablet, transdermal

Answer 149

A

Aripiprazole

Iloperidone

Answer 150

A

Haloperidol and fluphenazine
Esterified in sesame oil, can’t use in sesame oil allergy.
Absorption slower than elimination.
Haloperidol- loading dose, 20mg x PO dose optional, then 10-15mg PO
Fluphenazine- 12.5mg IM to 10mg PO

Answer 151

A

Risperidone
Paliperidone
Olanzapine
Aripiprazole

Answer 152

A

Reconstituted polymer

No oral overlap

Answer 153

A

Invega sustenna- 117mg Q 4 weeks
then
Invega Trinza- Q 3 months, start after 4 months on Sustenna
OR
Invega Halfyera- Q 6 months, start after 4 months on Sustenna or 1 cycle of Trinza
Sustenna, Trinza reduced dose in CCl 50-80mL/min, do not use in <50mL/min
Halfyera use not recommended for CrCl <90mL/min

Answer 154

A

Maintena- 14 day PO overlap
Aristada- 21 day PO overlap
Initio- initial injection, no oral overlap

Answer 155

A

Must be monitored for 3 hours following each administration for post injection delirium sedation syndrome (PIDSS)
REMS program

Answer 156

A

New antipsychotic agent- additional D2 presynaptic partial agonist activity
Administer WF
Low metabolic risk
ADR: Most common somnolence, xerostemia, nausea, dizziness
Place in therapy unclear

Answer 157

A

Indicated for schizophrenia and Bipolar I disorder, manic or mixed, and maintenance
Samidorphan is an opioid antagonist- added to help with weight management, no comparative data to metformin

Answer 158

A

Elderly patients, dementia related psychosis

Answer 159

A

Seizure disorder
Neuroleptic Malignant Syndrome
Movement disorders
Bloody dyscrasias (neutropenia)
Inability to adjust to extreme heat
CV disease
Hyperprolactinemia 
Dysphagia

Answer 160

A

Seizure disorder
Neuroleptic Malignant Syndrome
Movement disorders
Bloody dyscrasias (neutropenia)
Inability to adjust to extreme heat
CV disease
Hyperprolactinemia 
Dysphagia

Answer 161

A

Seizures
Neuroleptic malignant syndrome
Metabolic abnormalities that can increase CV risk
Hyperprolactinemia
Blood dyscrasias 
Orthostasis and syncope
Dysphagia
Inability to adjust to extreme heat

Answer 162

A

Brexpiprazole, aripiprazole, olanzapine/fluoxetine, quetiapine, lurasidone

Answer 163

A

More commonly seen with typical antipsychotics
DA effects > ACh effects
Acute dystonia, pseudoparkinsonism, akathisia, tardive dyskinesia

Answer 164

A

Occurs within 1-3 days
Spastic muscle contraction, usually head + neck
Increased in males, younger, higher doses, higher potency

Manage with IM anticholinergic- diphenhydramine, benztropine

Answer 165

A

Occurs within 1-3 months of initiation
Symptoms resemble PD- gait disturbances, cogwheel rigidity, bradykinesia
Increased in female, elderly, high doses, high potency

Manage by decreasing dose, anticholinergic agents
-Benzotropine, diphenhydramine, trihexyphenidyl

Answer 166

A

Occurs within the first 3 months, sooner in fast titration
Symptoms include subjective restlessness, jitteriness, fidgeting, pacing
Increased in high dose, high potency, fast titration, concomitant stimulant use
Manage by decreasing dose, change agent, pharmacologically
propranolol, lorazepam

Answer 167

A

Typicals > atypicals
Symptoms include repetitive involuntary movements generally involving the mouth and face
May be irreversible
Increased in females, elderly, DM, affective disorders, early EPS development, alcohol use
Manage by minimum effective dose, atypical medications
-Valbenazine, Deutetrabenazine

Answer 168

A

Rare but life threatening
Symptoms- fever, lead-pipe rigidity, mental status changes, autonomic dysfunction
Manage with supportive care, d/c antipsychotic- bromocriptine, dantrolene

Fever
Arms
Leukocytosis
Tremors
Elevated CPK
Rigidity

Answer 169

A

Caution in pre-existing abnormalities, other QTc prolonging agents, patients with QTc near 500
Baseline ECG may be appropriate
Least: aripiprazole
Most: ziprasidone, thioridazine 
BBW: thioridazine

Answer 170

A

Hyperprolactinemia from hypothalamic DA blockade
Galactorrhea, gynecomastia, amenorrhea, sexual dysfunction
More common with typical antipsychotics, does not happen with partial agonsits

Answer 171

A

Much more common with atypicals (SGAs)
Central obesity
High BP
High triglycerides
Low HDL cholesterol
Insulin resistance
Consider metformin with antipsychotic induced weight gain and insulin resistance

Answer 172

A

Thioridazone- pigmentary retinopathy (max dose 800mg/day)
Low potency agents- skin discoloration with sun exposure
All agents- transient elevations in LFTs

Answer 173

A

Clozapine
Olanzapine
Quetiapine

Answer 174

A

Increase prolactin levels
Risperidone
iloperidone
paliperidone

Answer 175

A

Asenapine- SL, transdermal
Lorazidone- WF
Ziprasidone= WF

Answer 176

A

Cariprazine
Aripiprazole
Brexipiprazole

Answer 177

A

Mortality and psychosis
Seizures- dose dependent, consider seizure prophylaxis (valproate)
Orthostasis, syncope, bradycardia, cardiac arrest- avoid combo with benzos, risk greatest during titration period
Myocarditis and cardiomyopathy- baseline ECG recommended, eosinophilia may be early indicator
Agranulocytosis- strict CBC monitorins, REMS

Answer 178

A

For agranulocytosis

Want ANC >1500

Answer 179

A

Paliperidone

Answer 180

A

Increased risk of hypotension
Avoid IM olanzapine with benzodiazepines
Separate by 1 hour at least

Answer 181

A

Pregnancy- main concern is movement disorders and withdrawal 
Clozapine and lurasidone may have least risk
Lactation- avoid
Partial agonists (CAB) reduce prolactin levels

Answer 182

A

More susceptible to metabolic changes (weight gain)
Schizophrenia rare in pediatrics
Risperidone and aripiprazole can be used in autism

Answer 183

A

Used for BPSD, anxiety, agitation, hypnosis, depression augmentatation
Rare: parkinsons disease psychosis

Answer 184

A

MOA: inverse agonist of 5-HT2A
Indicated ONLY for PD related psychosis
Being studied for schizophrenia

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