What is Vyvanse® used for?

Vyvanse® (Lisdexamfetamine) is a CNS Stimulant manufactured by Takeda. FDA-approved indications include: ADHD (adults and children 6+); Moderate-to-severe binge eating disorder (adults).

What are the common side effects of Vyvanse®?

Common side effects of Vyvanse® include: Decreased appetite (39%); Insomnia (27%); Dry mouth (26%); Increased heart rate (20%); Irritability / mood swings (18%).

How much does Vyvanse® cost?

Vyvanse® list price is approximately $450. With insurance it typically costs $50-100; without insurance approximately $350-400.

How strong is the clinical evidence for Vyvanse®?

Key studies: SPD489 studies, binge eating disorder trials. ADHD symptom reduction 60-70%; abuse risk marketed as lower than Adderall (debated) Potential conflicts of interest: ADHD researchers receive extensive pharma funding. Vyvanse won approval for binge eating disorder — an entirely new marketing segment — expanding $2.5B revenue..

CNS StimulantSchedule II Black Box Warning

Vyvanse®

Lisdexamfetamine

Takeda·FDA 2007·

20mg30mg40mg50mg60mg70mg

Version 2025-04 · Last reviewed April 1, 2025 · Methodology

List Price

$450

With Insurance

$50-100

FDA Black Box Warning

HIGH POTENTIAL FOR ABUSE

Schedule II controlled substance. Risk of dependence, cardiovascular events.

Strict Contraindications

Advanced arteriosclerosisCardiovascular diseaseHypertensionMAOIsGlaucoma

How It Works

Vyvanse (lisdexamfetamine) is an inactive prodrug. After swallowing, it is cleaved by enzymes in the gut and blood cells into d-amphetamine — identical to half the active ingredient in Adderall. The key difference is that this cleavage step creates a controlled, gradual release of active drug.

CleavesEnzymatic conversion (gut/red blood cells)

Lisdexamfetamine → d-amphetamine; the conversion rate controls onset and limits how fast the drug can be absorbed even if crushed or injected

ReversesDAT and NET transporters (via d-amphetamine)

Same mechanism as Adderall — dopamine and norepinephrine flood into synapse, correcting ADHD neurotransmitter deficit

Why the side effects happen

Identical side effect mechanism to amphetamine. The slower, smoother onset means less "crash" when the drug wears off and less initial cardiovascular spike. The inability to abuse IV or inhalation routes is the key design feature — crushing Vyvanse does not produce a faster high.

When Will I Feel It?

Slower onset than Adderall IR — requires enzymatic conversion. Effect builds over 1–2 hours and lasts 10–14 hours. One of the longest-acting ADHD medications available.

1–2 hoursFirst 2 hours

Gradual onset as lisdexamfetamine is converted to d-amphetamine. Less "hit" than Adderall IR.

3–5 hours3–5 hours

Peak effect — focus, executive function, impulse control maximized.

10–14 hoursFull day

Smooth, extended coverage through work or school day. Less afternoon drop-off than Adderall XR for many patients.

Adherence Note

Take Vyvanse in the morning — it can cause insomnia if taken after 10am. Not eating breakfast does not meaningfully affect onset, though eating may slightly slow it. Avoid taking with vitamin C (ascorbic acid) within 1 hour — acidic urine accelerates excretion.

Medical Disclaimer

The information on this page is compiled from publicly available clinical trial data, FDA prescribing information, and peer-reviewed literature. It is provided for educational purposes only and does not constitute medical advice, diagnosis, or treatment recommendations. Individual responses to medications vary. Always consult a qualified healthcare provider before starting, stopping, or changing any medication.

FDA Drug Database MedlinePlus (NIH) Cochrane Reviews How we rate evidence

Common Side Effects

While taking this medication, you may experience the following common side effects. We've included tips on how to manage them.

Decreased appetite

39%

Eat a nutritious breakfast before medication takes effect

Insomnia

27%

Take early in the morning; the drug lasts 12-14 hours

Dry mouth

26%

Sip water throughout the day; sugar-free gum helps

Increased heart rate

20%

Monitor pulse; inform doctor if consistently over 100 bpm at rest

Irritability / mood swings

18%

Often occurs as drug wears off ("rebound"); talk to doctor

Headache

16%

Stay well hydrated; usually improves over time

Upper abdominal pain

14%

Take with food or a light snack

Anxiety

12%

Report to doctor; dose may need adjustment or alternative considered

Nausea

10%

Take with food; improves with time

Weight loss

Ensure adequate nutrition; eat when hungry, even if no appetite

Serious Adverse Effects

• Sudden cardiac death
• Stroke
• Serious cardiovascular events
• Psychiatric episodes
• Serotonin syndrome (with other drugs)
• Growth suppression in children

Drug Interactions

Major Interactions (Avoid)

MAOIsPotentially fatal hypertensive crisis — contraindicated

Serotonergic drugsSerotonin syndrome

Moderate Interactions (Caution)

AntacidsIncreases absorption and effects

Tricyclic antidepressantsCardiovascular effects amplified

Food Interactions

Vitamin C / citrusReduces absorption and duration

AlcoholMasks intoxication; dangerous combination

When to Contact Your Doctor

This medication requires ongoing medical supervision. The following situations warrant a prompt conversation with your prescribing physician — do not wait for your next scheduled appointment.

Contact soon if you notice

Sudden cardiac death
Stroke
Serious cardiovascular events
Psychiatric episodes
Extreme fatigue and hypersomnia

Also discuss if you want to

Review whether this medication is still appropriate for you
Consider dosage adjustments based on response
Explore lifestyle or non-drug alternatives
Understand stopping or tapering options
Plan monitoring labs and follow-up

In the US, call 911 or go to the nearest emergency room for severe symptoms. Poison Control: 1-800-222-1222.

Special Populations

Safety classifications for specific groups — discuss with your provider before use.

Category C — AvoidPregnancy

Risk of premature birth, neonatal withdrawal.

Not RecommendedBreastfeeding

Passes into milk; developmental risk to infant.

Perimenopause Overlap — Know the DifferenceMenopause / Hormonal

Estrogen directly fuels the brain's dopamine system — the same system stimulant medications work on. As estrogen drops during perimenopause, many women experience new brain fog, poor focus, mood instability, and low motivation. Some receive an ADHD diagnosis in their 40s when hormonal change — not a lifelong attention disorder — is the actual driver. Ask your doctor about ruling out perimenopause before starting a stimulant.

Approved 6+ — Dietary Factors Often MissedChildren & Teens

Monitor growth; drug holidays considered. Important: excess sugar and processed carbs cause a blood sugar spike, followed by an insulin overcorrection, followed by a blood sugar crash. The body then releases adrenaline — causing shakiness, anxiety, restlessness, and inattention that can look exactly like ADHD. Dietary clean-up should always be explored before or alongside stimulant medication in children.

Use CautionOlder Adults

Higher cardiovascular risk; start low.

FDA Adverse Event Reports

Patient-filed reports from the FDA FAERS database · refreshed daily

Anecdotal data. Reports are not confirmed causation. Always consult your provider.

Community Reports

User-reported experiences — anonymous & anecdotal

Medical Disclaimer

FDA Drug Database MedlinePlus (NIH) Cochrane Reviews How we rate evidence

Metabolic & Lifestyle Alternatives

Non-Drug & Behavioral ADHD/BED Approaches

Behavioral therapy is comparable to medication long-term for ADHD; has established evidence for binge eating disorder

Important context: Evidence quality varies across these approaches. Some are well-studied with randomized controlled trial data; others are based on observational or smaller studies. These interventions are not guaranteed to replace medication for all patients. Discuss with your doctor whether any of these are appropriate for your clinical situation.

CBT for ADHD

Skills training + coaching

Equal to medication in long-term MTA follow-up

Exercise

30+ min aerobic daily

Acute improvement in executive function

CBT for BED

16-20 sessions

Remission in 50-60%

Mindfulness eating (BED)

Mindful eating practice

Reduces binge frequency significantly

Key Studies

MTA Long-Term: Behavioral therapy equal to stimulants at 14 months CBT for BED: 50-60% remission rate

Global Prescribing & Pricing

Vyvanse is priced at 6–15× more in the US than in comparable countries with pharmaceutical price negotiation

🇺🇸

United States

$350–400 (brand only until 2023)/mo

Rate

6M+ prescriptions in 2022 — heavy DTC advertising drove growth

Policy

No behavioral therapy prerequisite; marketed directly to consumers

Cover

Often requires prior authorization

🇬🇧

United Kingdom

~$190/mo

Rate

Restricted — specialist-only prescribing

Policy

NICE requires behavioral intervention before medication for children; specialist must initiate

Cover

Covered by NHS with specialist approval

🇫🇷

France

~$88/mo

Rate

Very low prescribing rate

Policy

Neuropsychological evaluation and therapy required first; extremely limited prescribing

Cover

Partially covered by Assurance Maladie

🇩🇪

Germany

~$132/mo

Rate

Low prescribing — methylphenidate preferred

Policy

Multimodal evaluation required; behavioral treatment must be concurrent with medication

Cover

Covered by GKV with evaluation

🇦🇺

Australia

~$27 (PBS)/mo

Rate

Lower prescribing — PBS restricts access

Policy

PBS requires specialist initiation (pediatrician or psychiatrist); PBS negotiates price down to AUD 40/mo

Cover

Covered by PBS with restrictions

Australia's PBS pays AUD 40/month (~$27) for the same drug that costs $350–400 in the US — the difference is government negotiating power. No clinical difference in the drug; 13× price difference explained entirely by policy.

Clinical Trials & Funding

Understanding who funds research helps contextualize results. Industry-funded trials are not automatically invalid — they undergo the same FDA review — but declared conflicts and sponsor effects are worth knowing. All linked trials can be verified on ClinicalTrials.gov.

Funding Sources

Original ADHD registration trials were primarily funded by Shire (now Takeda). The binge eating disorder indication was subsequently developed following initial ADHD approval.

Declared Conflicts of Interest

ADHD researchers receive extensive pharma funding. Vyvanse won approval for binge eating disorder — an entirely new marketing segment — expanding $2.5B revenue.

Key Efficacy Results

ADHD symptom reduction 60-70%; abuse risk marketed as lower than Adderall (debated)

Referenced Studies

Each study carries a Cochrane RoB-2 risk-of-bias badge — tap the badge for details.

Vyvanse ADHD Adults (Shire)

BED Trial (Shire)

Evidence & Transparency

Cochrane RoB-2 (Risk of Bias)

Badges reflect an editorial assessment using Cochrane's RoB-2 tool domains: randomization, intervention deviation, missing data, outcome measurement, and selective reporting. These are not certified Cochrane reviews. Learn more ↗

CMS Open Payments

Manufacturer payment disclosures are reported via the CMS Sunshine Act. Disclosure is legally required and does not imply bias or misconduct. Language uses "may," "suggests," or "appears" — never definitive clinical claims. CMS Open Payments ↗

Live Clinical Trials

Live from ClinicalTrials.gov · refreshed every 4 hours

Currently enrolling, active, and recently completed studies involving Lisdexamfetamine. Data is pulled directly from the U.S. National Library of Medicine.

Recent Research

Live from PubMed · peer-reviewed literature · refreshed every 4 hours

Most recently indexed clinical trials and systematic reviews mentioning Lisdexamfetamine in PubMed.

Source Documentation

Structured citations for referenced clinical trials

Each referenced trial is listed with its registry ID, funding source, and bias assessment. Use the copy button to generate a formatted citation.

Trial	Registry ID	Funder	Publication	Bias Rating	Cite
Vyvanse ADHD Adults (Shire)	NCT00877487	Shire/Takeda	J Clin Psychiatry 2011; 72:903-912	Some Concerns
BED Trial (Shire)	NCT01718483	Shire/Takeda	JAMA Psychiatry 2015; 72:235-246	Some Concerns

Bias ratings use Cochrane RoB-2 methodology. Editorial assessment — not a certified Cochrane review.

Our Methodology

Medical Disclaimer

FDA Drug Database MedlinePlus (NIH) Cochrane Reviews How we rate evidence

Stopping This Medication Safely

Taper CautiouslyDocumented timeframe: 4–8 weeks

As a Schedule II stimulant, Vyvanse discontinuation causes pronounced fatigue, low mood, increased appetite, and motivational deficits as the dopamine system readjusts.

What Published Research Shows About Stopping This Medication

This summarizes what published research documents — it is not personal medical advice. Any changes to your medication require discussion with your prescribing physician.

·Published tapering protocols describe dose reduction of 10–20mg every 2 weeks (e.g., 60mg → 50mg → 40mg → 30mg → stop)
·Research supports beginning regular aerobic exercise before stopping, which may help with dopamine system readjustment
·Research supports establishing a consistent sleep schedule (7–9 hrs) before stopping
·Clinical guidance suggests planning discontinuation during a lower-demand period
·Research supports having behavioral therapy or executive function coaching in place before stopping

Warning Symptoms — Contact Your Doctor If You Experience:

Extreme fatigue and hypersomnia
Low motivation or anhedonia (inability to feel pleasure)
Significant increase in appetite
Difficulty focusing beyond pre-medication baseline

Never change or stop a medication without consulting your prescribing physician.

Questions for Your Doctor

Questions to Ask

1.Has the child's diet been evaluated? Sugar and processed carbs spike blood sugar, then insulin overcorrects and the blood sugar crashes. The body releases adrenaline to fix the crash — causing shakiness, anxiety, restlessness, and inability to focus. This can look exactly like ADHD. Has a real-food, lower-sugar dietary trial been done first?
2.Have we tried behavioral therapy?
3.What cardiovascular monitoring will we do?
4.Is there a generic alternative that costs less?
5.Are drug holidays appropriate?

Lab Tests to Request

Blood pressure
Heart rate
Weight/height (children)
Fasting blood sugar — screen for reactive hypoglycemia
Mood/anxiety screening

Medical Disclaimer

FDA Drug Database MedlinePlus (NIH) Cochrane Reviews How we rate evidence

Frequently Asked Questions About Vyvanse®

What is Vyvanse® used for?: Vyvanse® (Lisdexamfetamine) is a CNS Stimulant manufactured by Takeda. FDA-approved indications include: ADHD (adults and children 6+); Moderate-to-severe binge eating disorder (adults).
What are the common side effects of Vyvanse®?: Common side effects of Vyvanse® include: Decreased appetite (39%); Insomnia (27%); Dry mouth (26%); Increased heart rate (20%); Irritability / mood swings (18%).
How much does Vyvanse® cost?: Vyvanse® list price is approximately $450. With insurance it typically costs $50-100; without insurance approximately $350-400.
Who funded the clinical trials for Vyvanse®?: Original ADHD registration trials were primarily funded by Shire (now Takeda). The binge eating disorder indication was subsequently developed following initial ADHD approval.
How strong is the clinical evidence for Vyvanse®?: Key studies: SPD489 studies, binge eating disorder trials. ADHD symptom reduction 60-70%; abuse risk marketed as lower than Adderall (debated) Potential conflicts of interest: ADHD researchers receive extensive pharma funding. Vyvanse won approval for binge eating disorder — an entirely new marketing segment — expanding $2.5B revenue..
Are there non-drug alternatives to Vyvanse®?: Behavioral therapy is comparable to medication long-term for ADHD; has established evidence for binge eating disorder See the Alternatives tab for full details.

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