Block 4 Lecture 2 -- ADHD

Question 1

What have been the most significant developments for ADHD drugs in the past 10 years?

Answer 1

drug formulation (LA, ER)

Question 2

How do males and females differ in ADHD presentation, referral, diagnosis?

Answer 2

males:

• • 6-10x more likely to be referred
• • more externalizing behaviors
• • 3x more likely to be diagnosed
• • more likely to have co-morbid neuropsychiatric issues

Question 3

What CNS “pathways” are involved in attention?

Answer 3

1) Alerting pathways
2) orienting pathways
3) working memory pathways
4) executive control pathways

Question 4

What regions are involved in CNS alerting pathways?

Answer 4

1) locus coeruleus
2) HT
3) PFc
4) parietal cx
5) reticular activating system in the brainstem

Question 5

What regions are involved in CNS orienting pathways?

Answer 5

1) parietal cx
2) visual cx
3) auditory cx

Question 6

What is the function of the locus coeruleus?

Answer 6

• • NE synthesis
• • ANS control center

involved in the CNS alerting pathways

Question 7

What regions are involved in the CNS executive control pathways?

Answer 7

1) PFc
2) limbic area
3) basal ganglia
4) cerebellum

Question 8

What regions are involved in the CNS working memory pathways?

Answer 8

1) PFc
2) cingulate cx
3) entorhinal cx
4) hippocampus
5) Amygdala

Question 9

What is the function of CNS orienting pathways?

Answer 9

1) tune spatiotemporal representation of relevant sensory stimuli
2) increase focus on a specific stimulus

Question 10

What is the function of CNS working memory pathways?

Answer 10

process and focus info about sensory stimuli or tasks

– over seconds to mins

Question 11

What is the function of the executive control CNS pathways?

Answer 11

integration and organization of information

Question 12

What genes are HYPOTHESIZED (not proven) to be mutated/involved in ADHD?

Answer 12

1) DAT
2) D4/D5 DAr
- - exon 3 7-repeat allele yields blunted response to DA
3) DBH

Question 13

What are the theories for ADHD pathology?

Answer 13

1) genetic

2) DA deficiency hypothesis

Question 14

What is the basis for the DA deficiency hypothesis?

Answer 14

1) stimulants work for 80% of pts
2) some imaging studies show DA/DAr deficits
3) animal studies support DA’s role in motor control, attention, and impulsivity

Question 15

What is the basis for the genetic theories of ADHD?

Answer 15

one of the most heritable neuropsychiatric conditions!

– 3-8x higher incidence if a parent has ADHD

Question 16

What are the weaknesses of the DA deficiency hypothesis?

Answer 16

1) literature doesn’t support one theory for ALL parts of ADHD
2) literature doesn’t support co-morbidities solely due to DA deficit

Question 17

What are risk factors for ADHD?

Answer 17

1) heredity
- - most significant!
2) labor/delivery complications
3) sub-optimal family environment
4) in utero tobacco smoke or lead exposure
5) developmental drug/alcohol exposure
- - NOT directly caused by bad parenting, tv, etc.

Question 18

What are co-morbidities of ADHD?

Answer 18

1) cigarette smoking
2) conduct disorder
3) bipolar disease
4) depression, anxiety, OCD
5) learning disabilities
6) tourettes
7) sleep disturbances
8) sensory dysfunction
9) pervasive disorders (Asbergers)

Question 19

What are the most common co-morbidities of ADHD?

Answer 19

1) learning disabilities! (40%)
2) conduct disorder (25%)
- - males much more than females
3) bipolar (10%)

tourettes (40-80% of tourettes pts have ADHD)

cigarette smoking is 2-3x the age-adjusted rate
– as symptoms increase, more likely to smoke

Question 20

What are the 3 presentations of ADHD?

Answer 20

1) primary inattention
2) primary hyperactivity/impulsivity
3) combined inattention and hyperactivity/impulsivity

Question 21

What are the possible diagnoses for a patient with symptoms?

Answer 21

• • mild, moderate, or severe
• • primary inattention, primary hyperactivity/impulsivity, or combined

– +/- autism spectrum disorder

presentation can vary across years

Question 22

How did DSM-IV differ from the current DSM-V?

Answer 22

1) presentations called “subtypes”
2) sxs had to appear before 6 yo
3) no mild/mod/severe
4) no ASD co-diagnosis
5) no differences for older patients

Question 23

What is the Vanderbilt ADHD diagnostic parent rating scale?

Answer 23

a tool that differentiates oppositional-defiant disorder, conduct disorder, and anxiety/depression from ADHD

Question 24

MoA of methylphenidate:

Answer 24

blocks DAT and NET

– DAT moreso than NET

Question 25

What kind of system is methylin ER? What are counseling points?

Answer 25

methylcellulose polymer / wax matrix;

• • 8 hour release
• • swallow whole
• • may still require BID admin

(same as ritalin SR)

Question 26

What kind of system is ritalin SR? What are counseling points?

Answer 26

intermediate-acting

methylcellulose polymer / wax matrix;

• • 8 hour release
• • swallow whole
• • may still require BID admin

(same as methylin ER)

Question 27

What kind of system is Metadate CD/ER? What are counseling points?

Answer 27

intermediate-acting

IR/ER bead mixture

• • CD is caps, ER is tabs
• • can open and sprinkle on food

Question 28

What kind of system is Ritalin LA? What are counseling points?

Answer 28

intermediate-acting

IR/ER beads formulated in SODAS

Question 29

What are the short-acting forms of MPH?

Answer 29

1) MPH – Ritalin, Methylin

2) Dex-MPH – Focalin

Question 30

What are the intermediate-acting forms of MPH?

Answer 30

1) Methylin ER, Ritalin SR
- - methylcellulose/wax polymer matrix
2) Metadate ER, Metadate CD
- - ir/er beads
3) Ritalin LA
- - sodas

Question 31

What are the long-acting forms of MPH?

Answer 31

1) Concerta
- - OROS
2) Focalin XR
- - sodas
3) Daytrana TD patch
4) quillivant XR
- - ER liquid MPH

Question 32

What is SODAS?

Answer 32

spheroidal oral drug absorption system

• • outer polymer dissolves, holes form
• • GI fluid enters
• • drug solubilizes and escapes

Question 33

What is OROS?

Answer 33

osmotic-release oral system

• • outer immediate release core
• • water enters thru semi-permeable membrane
• • osmotic pressure pushes layers of ensuing ER drug solution out of laser-drilled hole

Question 34

Describe ER liquid used in quillivant XR.

Answer 34

20% true soln; 80% ionic exchange resin suspension

Question 35

What kind of system is concerta? Counseling points?

Answer 35

OROS

• • 12 hour release
• • QD dosing

Question 36

What kind of system is Focalin XR?

Answer 36

SODAS

Question 37

What kind of system is Quillivant XR? Counseling Points?

Answer 37

ER liquid ion exchange resin

– QD dosing

Question 38

What is the MoA of amphetamines?

Answer 38

1) act on VMAT to reverse DAT
2) decrease MAO activity
- - DA affected moreso than NE

Question 39

What are the short-acting amphetamines?

Answer 39

1) Dextroamphetamine and amphetamine salts (Adderall)

2) Dextroamphetamine (Dexedrine, Dextrostat)

Question 40

What are the long-acting amphetamines?

Answer 40

1) Dexedrine spansule
2) Adderall XR
3) Lisdexamfetamine (Vyvanse)

Question 41

What kind of system is Dexedrine spansule?

Answer 41

IR/ER bead mixture

Question 42

What are the considerations for short-acting amphetamines?

Answer 42

1) best for initial treatment!
2) 2-3 x/day dosing :(
3) approved for kids 3+

Question 43

What are the considerations for long-acting amphetamines?

Answer 43

worse effects on:

• • evening appetite
• • sleep
• • growth stunting

Question 44

What are the considerations for Vyvanse (also a long-acting amphetamine)?

Answer 44

1) delayed onset in therapeutic action

2) less abuse and diversion potential

Question 45

Describe PK of lisdexamfetamine.

Answer 45

• • hydrolyzed to d-amphetamine during first pass
• — in intestines or liver
• — Lys is cleaved
• • rate-limited biotransformation

Question 46

Describe PK of MPH.

Answer 46

t1/2 = 3-4 hr

BID dosing

Question 47

How does dexmethylphenidate compare to methylphenidate?

Answer 47

lower dosage

Question 48

In what ages are short-acting MPH and amphetamines approved?

Answer 48

MPH: 6+
amphetamines: 3+

Question 49

You’re starting an ADHD patient on psychostimulant therapy. How do you do this?

Answer 49

1) titrate slow
- - want efficacy at lowest possible dose to avoid ADRs
2) don’t pick an SR form
- - difficult for titration
- - variable PK
- - variable time to max efficacy

Question 50

When are psychostimulants contraindicated?

Answer 50

1) bipolar disorder
2) schizophrenia
3) aggression
- - more DA worsens manic-depressive switching, and schizo and aggressiveness
4) h/o drug/EtOH abuse

Question 51

What are ADRs of psychostimulants?

Answer 51

1) black box: sudden death in children
2) diminished appetite, weight loss
3) delayed sleep onset / insomnia
4) late-day “wear off”
5) increased HR and BP
6) irritability, obsessiveness, social withdrawal

Question 52

How to manage appetite and sleep effects of psychostimulants?

Answer 52

appetite/weight loss
-- wears off over time
-- time meals to correlate with minimal med effect
insomnia
-- change dose/formulation
-- follow sleep hygiene

Question 53

What is the MoA of atomoxetine?

Answer 53

selective NET inhibitor

Question 54

What are ADRs of atomoxetine?

Answer 54

1) dry mouth
2) constipation
3) n/v
4) insomnia
5) sympathomimetic ADRs limit use

Question 55

When is atomoxetine used in ADHD?

Answer 55

1) substance abuse
2) stimulant failure or severe ADRs
3) need a 24h solution
- - ex: behavior problems in the am
- - ex: sleep disruption is a problem

Question 56

Why is atomoxetine not first line?

Answer 56

lower efficacy than stimulants

Question 57

What a2-adrenergic agonists are available for use in ADHD?

Answer 57

1) clonidine (IR/XR)

2) guanfacine (IR/XR)

Question 58

What is the MoA of clondine IR/XR?

Answer 58

probably POST-synaptic a2-adrenergic receptors in prefrontal cortex

Question 59

When are a2-adrenergic agonists used for ADHD?

Answer 59

NOT first line

1) best for hyperactive/aggressive patients
2) substance abuse
3) severe tics
4) seizure disorders
5) sleep disturbances
6) psychostimulant failure

Question 60

How is clonidine/guanfacine administered for ADHD?

Answer 60

1) ER formulations more useful, but still BID

2) can be adjunct to stimulants

Question 61

What are ADRs of clonidine/guanfacine

Answer 61

sedation (IR worst)
dry mouth
hypotension

Question 62

What antidepressants are used for ADHD treatment?

Answer 62

1) bupropion
2) duloxetine
3) venlafaxine
4) TCAs: imipramine and nortriptyline

NO SSRIs alone, not effective

Question 63

MoA of bupropion:

Answer 63

DAT/NET

– also lowers seizure threshold

Question 64

MoA of duloxetine:

Answer 64

SERT/NET

Question 65

MoA of Venlafaxine:

Answer 65

SERT/NET

Question 66

MoA of TCAs:

Answer 66

DAT/NET/SERT

Question 67

When are antidepressants used for ADHD?

Answer 67

maybe for ADHD + depression

– off-label

Question 68

What are the drug classes used for ADHD?

Answer 68

1) psychostimulants
2) selective NET inhibitors
3) a2-adrenergic agonists
4) antidepressants

Question 69

What are the effects of pharmacotherapy in ADHD?

How does it compare to counseling vs. the combination?

Answer 69

1) lessens sxs, sets stage for CBT benefits
2) continuous improvements
3) may slightly DELAY growth
4) no increase in substance abuse/diversion

– better than counseling; no obvious advantage with the combo

Question 70

What are the non-drug treatments of ADHD?

Answer 70

1) personal and family education
2) lifestyle changes
3) assistance in educational settings
4) improving interpersonal relationships
5) improving health habits
- - sleep, exercise, eating

Question 71

What are the DSM-V requirements for ADHD diagnosis in kids?

Answer 71

6 signs of inattention or hyperactivity for ≥ 6 mos

• • must appear before age 12
• • 2 settings
• • 2 independent evaluators

Question 72

What are the DSM-V requirements for ADHD diagnosis in adults?

Answer 72

5 signs of inattention or hyperactivity for ≥ 6 mos

• • child-onset, persistent, and current sxs
• • usually have significant sxs
• • 2 settings, 2 evaluators

Question 73

How does ADHD change with age?

Answer 73

decreased hyperactivity and impulsivity

persisting inattention

Question 74

What is DA’s supposed role in ADHD treatment?

Answer 74

decreasing inappropriate system “noise”

Question 75

What is NE’s supposed role in ADHD treatment?

Answer 75

increasing appropriate signaling

Question 76

What things lead to sudden onset disorders resembling ADHD?

Answer 76

1) head trauma
2) stroke
3) prefrontal cortex damage

Question 77

What is the thought for pathophysiology behind ADHD?

Answer 77

defects in one of the brain attention pathways

– specific neurochemical deficits are difficult to identify

Question 78

How is impulsivity studied?

Answer 78

delayed discounting

– presence of impulsive choice associated with gambling, risky behaviors, etc.

Question 79

What is the underlying pathophys of impulsivity?

Answer 79

damage to PFc DA system