Pharmacology of CNS Stimulants PDF Fall 2024

Summary

This document is lecture notes on the pharmacology of CNS stimulants, including various drugs, mechanisms of action, and adverse reactions. It's for a course called PHM 736 in the Fall of 2024.

Full Transcript

PHM 736
Fall 2024
Lunawati Bennett MS; PhD; PharmD; FACN

For I know the plan I have for you declared the Lord, plan to prosper you and
not to harm you to give you hope and future. Then you will call upon ME and
come and pray to ME, and I will listen to you. You will seek ME and find ME when
you search ME with all your heart. Jeremiah 29: 11-13
 ADD-attention deficit disorders  M1- muscarinic
 ADHD- attention deficit hyperactive  H1- histamine
disorders  5HT- serotonin
▪ MAOI- monoamine oxidase  NE- norepinephrine
inhibitors  DA- dopamine
▪ MAO- monoamine oxidase ▪ CV- cardiovascular
▪ MOA- mechanism of action ▪ OROS- oral osmotic controlled
▪ DDI- drug -drug interactions
delivery
▪ ADRs- adverse drug reactions
▪ GABA- gamma amino butyric acid
▪ OCD-obsessive compulsive disorder
▪ TCA- tricyclic anti depressant
▪ BBW- black box warning
Generic Name Trade Name Type
Bupropion HCL Wellbutrin ® Antidepressant, ADHD

Amitriptyline HCL Elavil ® TCA, antidepressant

Clonidine HCl Catapres®, Kapvay ®  2 agonist

Amphetamine+dextroamphetamine Adderall ® CII stimulant
Ritalin®, Methylin®,
Methylphenidate HCL Metadate®, Concerta ® CII stimulant

Lisdexamfetamine Vyvance ® CII stimulant

Atomoxetine HCl Straterra® non- CII stimulant

Modafinil Provigil ® C IV stimulant

You are responsible for underlined ADRs, drug names of each class, and brand names
At the end of this lecture and after studying the material, the student should be able to :

1. Identify sign/problems of ADHD and how psychostimulants can improve ADHD
problems
2. Compare and contrast psychostimulants and psychomimetics using known drugs
3. Identify MOA, ADRs, BBW (if any) and component of Adderall XR®, Concerta®,
Vyvance®, Ritalin LA®, and Dexedrine spansule ®
4. Identify ADRs, contraindication and management of overdose of psychostimulants
5. Identify MOA, ADRs, BBW, and DDI of atomoxetine
6. Identify MOA, ADR and use of alpha 2 agonists
7. Identify MOA , characteristics, ADR of modafinil and other drug for treatment of
narcolepsy
1. Psychostimulants: for moderate to severe ADHD
Methylphenidate, amphetamine, dextroamphetamine, lisdexamphetamine

2. Antidepressants : second line therapy
Imipramine, Desipramine, Nortriptyline, Bupropion

3. Anti hypertensives: to treat aggressive behavior
Clonidine, Guanfacine

4. Atomoxetine (Strattera®)- non psychostimulant
5. Modafinil (Provigil ®) – off label use. Also use for narcolepsy
6. Antipsychotics: for comorbid aggression, or resistant disorder
Aripripazole, haloperidol, Olanzapine, Risperidone

7. Lithium, Valproate, carbamazepine: for explosive behavior, aggression, impulsivity
  Improve Core Symptoms: inattention, impulsivity, hyperactivity

 Can also improve other symptoms: non-compliance, impulsive
aggression, social interactions, academic efficiency and accuracy, family
dynamics

What is the difference between psychomotor stimulants and psychomimetics ?

Psychomotor stimulant: ____________________________________________

Psychomimetic: ____________________________________________________
Psycho Stimulants t1/2 dosing____
 Adderall XR ® (amphetamine+dextro) 10 hr 10-30mg
 Desoxyn ® (methamphetamine) 4 -5 hr 10-25 mg
 Dexedrine Spansule ® (dextroampetamine SR) 7 hr 5-15 mg
 Dexedrine ® (dextroamphetamine) 5 hr 5-14mg
 Vyvanse ®(lisdexamfetamine) 10-12 hr 30-70 mg
 Metadate CD ® (methylphenidate ER) 8 hr 20-60 mg
 Concerta ®(methylphenidate ER) 9-10 hr 18-72mg
 Ritalin LA® (methylphenidate ER) 7-8 hr 10-60 mg
 Methylin ER ® (methylphenidate ER) 6 hr 20-30 mg
 Focalin ®(dexmethylphenidate) 4 hr 2.5-15 mg
 Focalin XR ® dexmethylphenidate) 8 hr 5-20mg
 Daytrana ® (Methylphenidate patch ) 12 hr 10-30 mg
 Quillivant XR ® (methylphenidate)-powder 5 hr 20-60 mg
 MOA: Promote release of NE, DA, 5-HT from nerve terminals
 catecholamine in the synaptic (inhibit reuptake), inhibit the action of MAO

Absorption: kidney, lungs & brain. High Vd

Metabolism: deamination (inactive), B-hydroxylation (active)
demethylation (methamphetamine become amphetamine)

Excretion: urine metabolites or unchanged. Reabsorption depends on pH of
the urine

Effects: Euphoria, ↑ confidence, ↑ alertness, ↑ mental/physical abilities,
improved self-esteem ( if withdrawal have opposite effects)
✓ The euphoria caused by amphetamine is 4-6 hr, which is 4-8 times longer than cocaine
 ADRs: insomnia, dizziness, headache, confusion,  seizure (if have history of
seizure), exacerbation of mixed/mania episodes in bipolar disorders
____________, ___________, ________, _________,_____, _____
bronchodilation, pulmonary edema, pulmonary hypertension,
↓ urine volume, new or worse behavior and thought problems

Monitor: height, weight, symptoms improvement, mood worsening, CV

Methamphetamines have stronger CNS action than amphetamine, but
amphetamines have more potent effect than methamphetamine on cardiac ADRs
such as : chest pain, BP, HR, MI may occur with overdose, tachycardia with PVC
(premature ventricular contractions)
MOA: Block NE and DA reuptake into presynaptic neurons,
NE and DA release from nerve terminals,
Inhibit the action of MAO

 Indications: ADD/ADHD, narcolepsy (excessive sleepiness)
 Unlabeled indication: depression in elderly and medically ill
 Use with caution in bipolar, DM, HTN,
 Should be taken 30-45 minutes before meal
 Don’t take with alcohol. Less irritability, anxiety or anorexia effect than
amphetamine
 ADRs: same as methamphetamine
 Monitor: height, weight
Golan et al, 2012
 Prodrug, Lisdexamfetamine =L-lysine-d-amphetamine that is converted to
d- ampehtamine.
▪ Drug become active when metabolized in the GI tract that break down L lysine→ releasing the
active drug, d-amphetamine

ADR: BP
BBW: serious cardiovascular sudden death, MI, stroke (in pts with preexisting cardiac problem)

Advantages: less abuse potential, less drug blood level fluctuations, longer onset of
effects, can’t be injected or snorted

DDI: monoamine oxidase inhibitor (MAOI), opioid, sympathomimetics
Need 14 days of wash out period after MAOI use
Contraindication of using stimulants
✓ agitated states (may aggravate symptoms),
✓ cardiovascular disease, glaucoma, moderate to severe hypertension, and hyperthyroidism
✓ concomitant use with MAOI or within less than 14 days of use ( can cause hypertensive crisis )

Treatment of overdose amphetamine, methylphenidate, cocaine
Hypertension: IV phentolamine or PO doxazosin
Tachycardia: IV β-blocker or verapamil
Hyperthermia: cooling blanket, dantrolene
Seizures: IV diazepam or phenytoin
Agitation: IV benzodiazepine (diazepam)
Hydration: with IV fluids to prevent renal damage
ADRS Management strategy

Wt loss,  appetite Give high calorie meals

Stomachache Give with meal,  dose

Insomnia Give dose earlier in the day, consider giving guanfacine, clonidine ,
melatonin at bed times
Rebound symptoms Use longer acting stimulant, atomoxetine, or anti-depressant

HTN, pulse fluctuation  dose, change medication

Hallucination d/c stimulant, reassess diagnosis, mood stabilizer or antipsychotic
maybe needed
Irritable Assess comorbid condition, mood stabilizer or antipsychotic maybe
needed

Dipiro et al, 2011
Tricyclic anti-depressants (TCA)
▪ Drugs: Imipramine, desipramine, nortriptyline
▪ MOA: inhibit 5 HT and NE reuptake, block M1, 1, H1 receptors
▪ Second line alternative for 10-20% of pts who are unresponsive to psychostimulants
▪ Maximal benefits are primarily observed in depressed or angry patients
▪ Potential for lethal overdose. Need for screening labs and EKG.
▪ ADRs: sedation, dizziness, constipation, heart block, weight gain

Bupropion (Wellbutrin ®)
MOA:  presynaptic release of NE and DA
Use: antidepressant, smoking cessation, ADHD
ADRs: anorexia, insomnia
MOA: selectively inhibit re-uptake of norepinephrine

 Does not exacerbate tics. Full effect may not be seen until 6-8 weeks

 ADRs: ↓ appetite, nausea, ↓weight, somnolence,__________, ____________, fatique, mood
changes, liver damage, ________________

 DDI: MAOI, alcohol, 2 agonist, CNS depressants, CP2D6 inhibitor
 Protein binding: 98%
 Metabolism: hepatic via CYP2D6 and CYP2C19 (no dose adjustment in renal but adjustment in hepatic )
Excretion : urine 80%, feces 17%
 t1/2: 5 hr, up to 24 hr in poor metabolizer of CYP2D6

17
BBW: risk of suicidal ideation of Atomoxetine (2 of 2)
MOA: stimulate 2 in brain. In presynapse: inhibit NE release.
In Postsynapse:  blood flow in prefrontal context (memory).

✓ Clonidine (Catapres ®, Kapvay®-ER ) t1/2- 12 hr
✓ Guanfacine (Tenex®, Intuniv®-ER)- longer acting; less sedating than clonidine t1/2 -18 hr

ADR: sedation, hypotension (should be withdrawn slowly to avoid rebound HTN)
bradycardia, HA, fatigue, tremor, sweating, anxiety

▪ Transdermal patches may enhance compliance.
▪ Pregnancy C
Indication:
▪ Benefit in hyper-aroused pts, extremely overactive ,and pts with overactive or irritable,
impulsive, aggressive conduct disorders
▪ Used at bedtime to counteract insomnia effects of stimulants.
▪ Tourette’s syndrome , tic disorder

DDI: CYP3A4 substrate, inducer or inhibitor
CYP2D6 inhibitor (paroxetine, fluoxetine)
Need 14 days wash out period with MAOI
 Condition of excessive daytime
Drugs:
sleepiness; sudden daytime “sleep 1. Dextroamphetamine,
attacks” due to poor control of normal
Methylphenidate
sleep wake cycles.
 The sleep attacks last a few seconds to
2. Modafinil, armodafinil
several minutes.

 Cataplexy (sudden loss of muscle tone) 3. Sodium Oxybate
and sleep paralysis
 Sleep quality is poor, but can fall asleep 4. H3 antagonist
while at work, school or in the middle of
conversation 5. Dopamine and
norepinephrine reuptake
 Treatment: psycho stimulants inhibitor (DNRI)
MOA: mechanism unclear. May decrease GABA, not altering NE nor DA

Methylphenidate or amphetamine: widespread CNS activation
Modafinil works in discrete brain regions, with specific receptors

 It is not a typical stimulant and is often described as a "wakefulness promoting agent“ to improve
"alertness" and reducing excessive sleepiness, narcolepsy, sleep apnea
 Off-label use for ADHD.
 Class: IV

ADR: rash can be life threatening, anxiety, headache, agitation, aggressive, confused, or excited, fever,
nausea, vomiting, diarrhea chills, cough, sore throat, and body aches, mood or mental, changes,
numbness, tingling, or burning pain in hands, arms, or feet

Armodafinil (Nuvigil ®)- R isomer of modafanil- similar profile like modafinil
MOA: derivative of GABA
Indication: narcolepsy with cataplexy
 Help with sleep at night, and use with stimulants during daytime

This is “date rape” drug (CI, illicit use).
 Require REMS program to unsure only used by pts- class: CIII

Contraindication: sedative hypnotic, alcohol
Warning: depression, suicide, psychosis, anxiety, sleep walking
ADR: dizziness, confusion ,nausea
MOA: Block histamine subtype 3
 It works as inverse agonist

Indications: adult patients with excessive
daytime sleepiness associated with
narcolepsy

Contraindication: severe hepatic impairment

ADRs: insomnia, nausea, anxiety,
headache, and QT prolongation

Harvey RA, Champe PC, 2012
 MOA: dopamine and norepinephrine reuptake inhibitor (DNRI)

 Indications: adult with excessive daytime sleepiness associated with
narcolepsy or obstructive sleep apnea

 Contraindication: use with monoamine oxidase inhibitor (MAOI) or
within 14 days of d/c

 ADRs: headache, nausea,  BP and heart rate, anxiety, psychiatric
symptoms,  appetite

https://sunosihcp.com/mechanism-of-action
1) Straterra  (______________) is useful as ______________ stimulant, works
by _______________. Can cause ____________, ________________,
__________________, __________________, ________,

2) Clonidine (Catapres®, Kapvay ®) works as ______________, causing
________________. It cause ________ blood flow in cortex, thus _____
memory.
 It is useful for ______________, _______________. Should be given at
______________. It can cause ____________, ___________, ___________
✓ Dipiro et al. Pharmacotherapy: A Pathophysiologic Approach, 8th ed. 2011
✓ RxPrep Course book NAPLEX 2020 edition.
✓ ADHD Practice Parameters. J Am Acad Child Adolesc Psychiatry. 1997;36:85S.
✓ Greenhill LL, et al. J Am Acad Child Adolesc Psychiatry. 1999;38:503-512.
✓ Various internet sources as cited
✓ Goodman and Gilman’s The Pharmacological Basis of Therapeutics, 14th edition Editors:
Brunton, Hilal-Dandan, Knollmann. Publisher: McGraw-Hill, 2023
✓ Katzung BG et al. Basic & Clinical Pharmacology. 15th ed. 2021
 FYI
Wednesday, January 21,
2009

What children say about taking their
ADD drugs
“When I take my medication, it is
like my teacher is in my head”
“On my medicine I feel calm,
without it I’m in hyperspace”
“Before I was looking through a
door that had frosted glass, but now
it is all clear”

https://www.youtube.com/watch?v=
5GBMS7WPFSs
by: David Gutierrez, staff writer
 A specific neuroanatomic, physiologic, biochemical or psychologic origin that
has not been identified, despite extensive investigations
o Boys are identified to have more of hyperactive-impulsive and inattentive type
disorder in comparison to girls. Some have learning disabilities, neurological
signs, or Tourette’s disorder. As they grow older can become OCD
 75% of child / adolescent with ADHD cases continue to adulthood

 Signs: Lack of social skills, unpopular, need to be first;
Needs are imperative, now, can not wait;
Problem in writing, reversal of letters

 3 components of treatment: education interventions,
psychosocial interventions,
pharmacotherapeutic interventions
▪ Establish a treatment program that recognizes ADHD as a
chronic condition
▪ Specify appropriate target outcomes to guide management
▪ Prescribe stimulant medication and/or behavior therapy to
improve target outcomes in children with ADHD
▪ If the treatment program has not met target outcomes,
evaluate:
✓ Original diagnosis
✓ Use of all appropriate treatments
✓ Adherence to the treatment plan
✓ Presence of coexisting conditions
▪ Using information from parents, teachers, and the child,
follow-up to evaluate target outcomes and adverse effects
Parent and Child Interviews
▪ Consider using DSM-IV symptoms checklist
▪ General Past Medical History with attention, from birth History , due to trauma
▪ ‘Onset’ before 7 years of age?
▪ Specific queries about Family History of ADHD, other psychiatric disorders, neurologic
disorders and psychosocial adversity, Social History, Developmental History
▪ Medications ( RX, OTC, illicit substances),
▪ Parent completed rating scales;
▪ Target questions to ascertain 2 or more settings for functional impairment

School-Related Assessment
▪ Obtain reports of behavior, learning, attendance, grades and test scores
▪ Psychoeducational testing is indicated to assess intellectual ability and to learning disabilities
▪ Teacher completed rating scales
 DEX-
dextroamphetamine
 DMPH-
dexmethylphenidate
 MPH-
methylphenidate
 MXA-mixed
amphetamine salt
 TCA-tricyclic
antidepressant

Dipiro et al., 2011
1. Fish oil
 Omega 3 FA
 If use with evening primrose oil (omega 6 FA)- may improve cognitive function and behavior in
children. Need to take 6 capsules

2. St. John’s wort
 May inhibit reuptake of NE, DA, 5HT
 DDI: CYP3A4 and CYP2C9 inducers

3. Ginkgo
 May have neuroprotective effect
 DDI: warfarin. ADRs: GI, HA, dizziness

4. S-adenosyl L methionine (SAMe)
 Endogenous substance made from L-methionine and ATP produce in liver. May increase NE, DA, 5HT in
brain
 ADR: ND, heartburn, dry mouth