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SNRI (Serotonin-Norepinephrine Reuptake Inhibitor)Not Controlled Black Box Warning

Cymbalta®

Duloxetine HCl

Generic (originally Eli Lilly)·FDA 2004·
20mg30mg60mg90mg120mg

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

List Price

$75

With Insurance

$10-30

The Short Version

Plain-language summary

Cymbalta (Duloxetine HCl) boosts both serotonin and norepinephrine in the brain. This dual action treats depression and anxiety, but also dampens pain signals — which is why it's prescribed for nerve pain and fibromyalgia too.

How it works: Duloxetine inhibits the reuptake of both serotonin (a brain chemical that affects mood) and norepinephrine (a brain chemical that affects alertness) in the brain and spinal cord. In depression, it increases the availability of both neurotransmitters in synaptic gaps. In chronic pain, the norepinephrine component activates descending pain inhibition pathways in the spinal cord — this dual action explains its use for both depression and pain.

What people most commonly report

Nausea
23-25%
Dry mouth
13-15%
Drowsiness / fatigue
10-12%
Constipation
10-11%
Insomnia
10%

Most common side effect; usually improves after 1-2 weeks. Take with food.

Most studies were paid for by the company that makes this drug.

What Else the Evidence Supports

Non-drug options with clinical backing

Exercise has strong evidence for both depression and chronic pain — the two primary reasons duloxetine is prescribed. For mild-to-moderate depression, therapy and lifestyle changes show comparable efficacy to medication in many studies.

Exercise (for depression)Emerging

Effect size comparable to antidepressants (Cohen's d = 0.

Cognitive Behavioral Therapy (CBT)Emerging

NNT ~4 for depression; significant functional improvement in chronic pain.

Anti-inflammatory dietEmerging

SMILES trial: Dietary improvement produced remission in 32% vs 8% control.

Sleep optimizationEmerging

CBT-I reduces depression severity by 50% in comorbid insomnia-depression.

What This Really Costs

Long-term cost projection based on current pricing

Monthly

$35

$20 w/ insurance

without insurance

Annual

$420

$240 w/ insurance

without insurance

10 Years

$4.2K

$2.4K w/ insurance

without insurance

30 Years

$12.6K

$7.2K w/ insurance

without insurance

Lifestyle alternative: $0/month in prescriptions. Exercise (for depression)Effect size comparable to antidepressants (Cohen's d = 0.

The average American retiree spends $165,000 on healthcare after retirement (Fidelity, 2024). Informed choices today compound over decades.

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SSRI (Selective Serotonin Reuptake Inhibitor)

Same drug class

FDA Black Box Warning

SUICIDALITY IN CHILDREN AND YOUNG ADULTS

Antidepressants increased the risk of suicidal thinking and behavior in children, adolescents, and young adults (ages 18-24) in short-term studies. Monitor closely for clinical worsening and suicidal ideation, especially during the first few months and dose changes.

Strict Contraindications

Use with MAOIs or within 14 days of stoppingUncontrolled narrow-angle glaucomaSevere hepatic impairmentUse with thioridazine

Metabolic & Lifestyle Alternatives

Evidence-Based Alternatives for Depression and Chronic Pain

Exercise has strong evidence for both depression and chronic pain — the two primary reasons duloxetine is prescribed. For mild-to-moderate depression, therapy and lifestyle changes show comparable efficacy to medication in many studies.

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.

Exercise (for depression)

Aerobic exercise 3-5x/week has robust evidence for depression. The SMILE trial found exercise equivalent to sertraline at 16 weeks, with lower relapse rates at 10-month follow-up.

Effect size comparable to antidepressants (Cohen's d = 0.5-0.8) for mild-to-moderate depression

Cognitive Behavioral Therapy (CBT)

CBT is the most studied psychotherapy for depression and chronic pain. For depression, it performs as well as medication in many trials. For chronic pain, CBT improves function even without reducing pain intensity.

NNT ~4 for depression; significant functional improvement in chronic pain

Anti-inflammatory diet

Depression is increasingly linked to systemic inflammation. Diets rich in omega-3s, vegetables, and whole foods and low in ultra-processed food show antidepressant effects.

SMILES trial: Dietary improvement produced remission in 32% vs 8% control

Sleep optimization

Insomnia is both a symptom and a driver of depression. CBT for insomnia (CBT-I) can improve depression even without directly targeting mood.

CBT-I reduces depression severity by 50% in comorbid insomnia-depression

Omega-3 fatty acids (EPA)

EPA-predominant fish oil supplements have modest evidence for depression as adjunctive therapy. The evidence is stronger for EPA than DHA.

Small-to-moderate effect (Cohen's d = 0.2-0.4) as adjunctive treatment

Global Prescribing & Pricing

Duloxetine is widely prescribed globally for both depression and chronic pain; one of the most multi-indication antidepressants

🇺🇸

United States

$40-80/mo

Rate

Heavily prescribed for pain + depression overlap; 5 FDA-approved indications

Policy

No therapy requirement before prescribing

Cover

Usually covered

🇬🇧

United Kingdom

~$3-8/mo

Rate

NICE recommends for depression, GAD, and diabetic neuropathy

Policy

CBT or counseling typically offered alongside

Cover

Covered by NHS

🇫🇷

France

~$5-12/mo

Rate

Used for depression and chronic pain

Policy

Psychotherapy reimbursed alongside

Cover

Covered by Sécurité Sociale

🇩🇪

Germany

~$8-15/mo

Rate

Widely prescribed for multimorbid patients

Policy

Psychotherapy often preferred as first-line

Cover

Covered by GKV

🇯🇵

Japan

~$20-40/mo

Rate

Increasingly used; approved for depression and pain

Policy

Often combined with psychotherapy

Cover

Covered by JHIS

Duloxetine is one of the most "multi-purpose" antidepressants — approved for 5 different conditions in the US. This breadth of indications, all established through industry-funded trials, expanded the market enormously. Other countries tend to use it more selectively and pair it with psychotherapy.

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.

Key Efficacy Results

Modest efficacy for depression (NNT ~7); more compelling for chronic pain conditions (NNT ~5 for neuropathy). Discontinuation syndrome is notably severe compared to other antidepressants.

Referenced Studies

Each study shows its evidence level and Cochrane RoB-2 risk-of-bias rating — tap the bias badge for details.

Duloxetine vs Placebo (Depression - Lilly)
RCT
Duloxetine for GAD (Lilly)
RCT
Duloxetine for Diabetic Neuropathy (Lilly)
RCT

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 Duloxetine HCl. 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 Duloxetine HCl 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.

TrialRegistry IDCite
Duloxetine vs Placebo (Depression - Lilly)PMID:11950987
Duloxetine for GAD (Lilly)PMID:15169693
Duloxetine for Diabetic Neuropathy (Lilly)PMID:15128046

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

Our Methodology

Common Side Effects

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

Nausea

23-25%

Most common side effect; usually improves after 1-2 weeks. Take with food.

Dry mouth

13-15%

Sip water frequently; sugar-free gum may help

Drowsiness / fatigue

10-12%

May improve over weeks; consider bedtime dosing

Constipation

10-11%

Increase fiber and water intake

Decreased appetite

8-10%

Monitor weight; some patients lose weight on duloxetine

Dizziness

9-10%

Rise slowly; usually improves after first week

Insomnia

10%

Take in the morning if sleep is disrupted

Sexual dysfunction

3-10%

May affect desire, arousal, or orgasm. Often underreported. Tell your doctor — alternatives exist.

Excessive sweating

6-7%

Common with SNRIs; manage with breathable clothing

Increased blood pressure

2-5%

SNRIs can raise BP via norepinephrine effect — monitor regularly

Serious Adverse Effects

  • Suicidal ideation (FDA black box — age <25)
  • Serotonin syndrome (with serotonergic drugs)
  • Hepatotoxicity (liver damage — avoid in heavy drinkers)
  • Severe discontinuation syndrome
  • Hyponatremia (low sodium — especially in elderly)
  • Mania activation in bipolar disorder

Drug Interactions

Major Interactions (Avoid)

MAOIs (phenelzine, selegiline)Serotonin syndrome — potentially fatal. 14-day washout required.
ThioridazineFatal cardiac arrhythmias — contraindicated
Linezolid (antibiotic)Serotonin syndrome risk — avoid combination

Moderate Interactions (Caution)

TramadolSeizure risk and serotonin syndrome
Triptans (sumatriptan)Serotonin syndrome risk — use cautiously
Blood thinners (warfarin, aspirin, NSAIDs)Increased bleeding risk — SNRIs impair platelet function
CYP1A2 inhibitors (fluvoxamine, ciprofloxacin)Increases duloxetine levels up to 5-6x — avoid
AlcoholIncreases liver damage risk — avoid heavy drinking

Food Interactions

AlcoholLiver damage risk increased; avoid heavy or regular alcohol use
GrapefruitMinimal interaction — no significant concern

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

  • Suicidal ideation (FDA black box — age <25)
  • Serotonin syndrome (with serotonergic drugs)
  • Hepatotoxicity (liver damage — avoid in heavy drinkers)
  • Severe discontinuation syndrome
  • Brain zaps (electric shock sensations in the head)

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.

Use With CautionPregnancy

Category C. Third-trimester use associated with neonatal withdrawal syndrome. Weigh risk vs benefit with doctor.

Use With CautionBreastfeeding

Present in breast milk. Monitor infant for sedation, poor feeding, irritability.

Often Prescribed for Menopause SymptomsMenopause / Hormonal

Duloxetine is sometimes prescribed off-label for hot flashes and mood changes during menopause. It is also used for the musculoskeletal pain that can accompany perimenopause. Ask whether your symptoms might have a hormonal component that could be addressed differently.

Approved ≥7 for GADChildren & Teens

FDA-approved for GAD in children 7-17. Black box warning for suicidality applies. Not approved for depression in children.

Use CautionOlder Adults

Greater risk of hyponatremia, falls, and bleeding. Start at lower dose.

Avoid in Severe ImpairmentKidney Disease

Not recommended if CrCl <30. Active metabolites accumulate.

Contraindicated in Severe DiseaseLiver Disease

Hepatotoxicity risk; duloxetine levels increase significantly with liver impairment.

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

Stopping This Medication Safely

Extremely Difficult — Taper Very SlowlyDocumented timeframe: 2-6 months or longer for safe discontinuation

Duloxetine discontinuation syndrome is among the most severe of any antidepressant. Symptoms include "brain zaps," extreme dizziness, nausea, irritability, insomnia, and electric shock sensations. The capsule formulation makes precise dose reduction difficult because capsules should not be opened or crushed.

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.

  • ·Duloxetine has one of the most challenging discontinuation profiles — do NOT stop abruptly
  • ·Published tapering approaches describe extremely gradual reductions: 120mg → 90mg → 60mg → 30mg → 20mg, with each step lasting 2-4 weeks minimum
  • ·Some clinicians use bead-counting methods (opening capsules and removing beads gradually) — this is off-label but widely practiced when standard dose steps are too large
  • ·Cross-tapering to fluoxetine (which has a very long half-life) before discontinuing is another published approach to reduce withdrawal severity
  • ·Research shows that the 30mg → 0 step is often the most difficult — consider holding at 20mg for 4+ weeks

Warning Symptoms — Contact Your Doctor If You Experience:

  • Brain zaps (electric shock sensations in the head)
  • Severe dizziness or vertigo
  • Extreme irritability or emotional lability
  • Nausea, vomiting, diarrhea
  • Insomnia
  • Flu-like symptoms (muscle aches, chills, sweating)

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

Questions for Your Doctor

Questions to Ask

  • 1.Would therapy alone be enough for my level of depression?
  • 2.What is the plan for eventually coming off this medication?
  • 3.How bad is the discontinuation syndrome — and how will we manage it?
  • 4.Is my pain better addressed by treating the underlying cause?
  • 5.Are there non-SNRI options with fewer withdrawal issues?

Lab Tests to Request

  • Blood pressure monitoring (SNRIs can raise BP)
  • Liver function tests
  • Sodium level (risk of hyponatremia in elderly)
  • Mood and suicidality screening (first 3 months)

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

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