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Anticonvulsant / GabapentinoidNot Controlled (federally); Schedule V in KY, MI, TN, VA, WV; Class C in UK

Neurontin®

Gabapentin

Pfizer (originally Parke-Davis) / Generic·FDA December 1993 (epilepsy); July 2002 (postherpetic neuralgia)·
100mg300mg400mg600mg800mg

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

List Price

$600+ (brand Neurontin)

With Insurance

$5–20

The Short Version

Plain-language summary

Neurontin (Gabapentin) calms overactive nerve signals by reducing calcium flow in neurons. Despite its name, it doesn't actually affect GABA. It's FDA-approved for seizures and shingles nerve pain, but widely prescribed off-label for general nerve pain and anxiety.

How it works: Despite its name, gabapentin does not directly activate GABA receptors. Instead, it attaches to a subunit of voltage-gated calcium channels in neurons, reducing calcium entry and therefore reducing the release of excitatory neurotransmitters, dampening overactive pain signaling.

What people most commonly report

Dizziness / vertigo
28%
Somnolence / excessive sedation
21%
Ataxia (loss of coordination)
13%
Fatigue
11%
Peripheral edema (ankle swelling)
8%

Most common reason for stopping. Rise slowly; avoid ladders or heights. Usually improves after 1–2 weeks.

Some studies were independent, others were paid for by the company that makes it.

What Else the Evidence Supports

Non-drug options with clinical backing

The evidence for gabapentin in many chronic pain conditions is weak, lifestyle and targeted interventions often provide comparable relief without dependency or sedation

Alpha lipoic acid (600mg/day)Moderate

Multiple RCTs show ALA reduces diabetic neuropathy pain and improves nerve conduction; comparable to gabapentin with superior safety profile.

Physical therapy (graded motor imagery)Moderate

Graded motor imagery reduces neuropathic and chronic pain by retraining the brain's pain processing; evidence strongest for CRPS.

Low-carbohydrate dietModerate

Reducing blood glucose directly reduces glycation damage to peripheral nerves; HbA1c normalization slows neuropathy progression.

Capsaicin 8% patch (Qutenza)Strong

FDA-approved for postherpetic neuralgia and diabetic neuropathy; depletes substance P locally, no systemic side effects.

What This Really Costs

Long-term cost projection based on current pricing

Monthly

$40

$13 w/ insurance

without insurance

Annual

$480

$156 w/ insurance

without insurance

10 Years

$4.8K

$1.6K w/ insurance

without insurance

30 Years

$14.4K

$4.7K w/ insurance

without insurance

Lifestyle alternative: $0/month in prescriptions. Alpha lipoic acid (600mg/day) - Multiple RCTs show ALA reduces diabetic neuropathy pain and improves nerve conduction; comparable to gabapentin with superior safety profile.

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

Metabolic & Lifestyle Alternatives

Neuropathic & Chronic Pain Without Gabapentinoids

The evidence for gabapentin in many chronic pain conditions is weak, lifestyle and targeted interventions often provide comparable relief without dependency or sedation

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.

Alpha lipoic acid (600mg/day)

Moderate

For diabetic peripheral neuropathy specifically

Multiple RCTs show ALA reduces diabetic neuropathy pain and improves nerve conduction; comparable to gabapentin with superior safety profile

Physical therapy (graded motor imagery)

Moderate

Supervised exercise + GMI for central sensitization pain

Graded motor imagery reduces neuropathic and chronic pain by retraining the brain's pain processing; evidence strongest for CRPS

Low-carbohydrate diet

Moderate

For diabetic neuropathy, address the root cause

Reducing blood glucose directly reduces glycation damage to peripheral nerves; HbA1c normalization slows neuropathy progression

Capsaicin 8% patch (Qutenza)

Strong

Prescription topical; applies to pain area

FDA-approved for postherpetic neuralgia and diabetic neuropathy; depletes substance P locally, no systemic side effects

TENS (Transcutaneous Electrical Nerve Stimulation)

Moderate

At-home device; applied to pain area

Modulates pain signaling via gate control mechanism; evidence for chronic neuropathic pain and fibromyalgia

Global Prescribing & Pricing

Gabapentin is one of the most prescribed medications in the US; 83% of prescriptions are off-label, making it one of the most over-prescribed drugs globally

🇺🇸

United States

$20–60/mo

Rate

83% of prescriptions are off-label; massive prescribing for pain conditions with limited evidence

Policy

No federal scheduling despite abuse potential. Several states (KY, TN, MI, WV, VA) independently added gabapentin to Schedule V due to epidemic abuse rates.

Cover

Usually covered

🇬🇧

United Kingdom

~$5–15/mo

Rate

Became Class C controlled substance in 2019 due to abuse epidemic

Policy

NHS England and the MHRA added gabapentin (and pregabalin) to Schedule 3 Class C controlled substances in April 2019, following a marked increase in abuse-related deaths, particularly in combination with opioids.

Cover

NHS covered, controlled prescription required

🇩🇪

Germany

~$10–20/mo

Rate

More conservative prescribing for non-epilepsy indications

Policy

German guidelines restrict gabapentinoids to well-documented indications; off-label use requires documented justification and specialist involvement.

Cover

GKV covered for approved indications

🇦🇺

Australia

~$10–25/mo

Rate

PBS restricts to approved indications; limited off-label subsidization

Policy

TGA has issued warnings about gabapentin abuse; PBS coverage is restricted to approved indications with documented diagnosis.

Cover

PBS, restricted to approved indications

The UK's 2019 decision to schedule gabapentin as a controlled substance was driven by data showing it was a major contributor to opioid-related deaths. The US, where abuse rates are similarly high, has not made this change at the federal level, leaving states to act independently.

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

FDA approved for epilepsy and postherpetic neuralgia only. Evidence for other pain uses (back pain, fibromyalgia, general neuropathy) is weak to moderate. The 2019 Cochrane review on gabapentin for chronic neuropathic pain found it helps only 30–40% of patients, with many experiencing significant side effects.

Referenced Studies

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

Parke-Davis/Pfizer $430M Criminal Conviction
Reg.
Gabapentin Off-Label Prescribing Analysis
Obs.

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 Gabapentin. 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 Gabapentin 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
Parke-Davis/Pfizer $430M Criminal ConvictionDOJ-2004
Gabapentin Off-Label Prescribing AnalysisPMID:25879938

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.

Dizziness / vertigo

28%

Most common reason for stopping. Rise slowly; avoid ladders or heights. Usually improves after 1–2 weeks.

Somnolence / excessive sedation

21%

Do not drive or operate machinery until you know your response. May not improve with time at higher doses.

Ataxia (loss of coordination)

13%

Fall hazard, especially in elderly. Consider dose reduction if persistent.

Fatigue

11%

Often improves; take larger portion of dose at night.

Weight gain

3–10%

Average 2–5 lbs in first year. Mechanism: increased appetite, decreased activity due to sedation.

Peripheral edema (ankle swelling)

8%

Common at higher doses. Elevate legs; reduce dose if significant. May indicate need to reassess.

Cognitive impairment / "brain fog"

2–3%

Memory and processing speed affected. At higher doses, can be significant. Report to doctor.

Serious Adverse Effects

  • Respiratory depression, especially when combined with opioids, benzodiazepines, or alcohol; increasingly implicated in overdose deaths
  • Physical dependence, gabapentin withdrawal syndrome includes anxiety, insomnia, nausea, sweating, and seizures; risk highest with abrupt cessation after high-dose chronic use
  • Suicidality, FDA black box warning for all anticonvulsants; increased risk of suicidal thoughts and behavior
  • Mood changes / paradoxical agitation, especially in children and adolescents
  • Drug abuse potential, significant street value; used recreationally for euphoria especially in combination with opioids

Drug Interactions

Major Interactions (Avoid)

Opioids (oxycodone, hydrocodone, tramadol)Synergistic respiratory depression. Gabapentin + opioid combinations are now among the leading drivers of overdose deaths. FDA has issued multiple warnings. Thousands of deaths involve this combination.
CNS depressants (benzodiazepines, alcohol, zolpidem)Additive sedation and respiratory depression. Avoid alcohol entirely; use benzodiazepines with extreme caution and only with medical supervision.

Moderate Interactions (Caution)

Antacids (aluminum/magnesium-containing)Reduce gabapentin absorption by up to 20%. Take gabapentin at least 2 hours after antacid.
MorphineMorphine increases gabapentin bioavailability by ~44%. Combined sedation risk is significant.
HydrocodoneGabapentin increases peak hydrocodone concentration; significant respiratory depression risk in combination.

Food Interactions

AlcoholNever combine. Additive CNS and respiratory depression. Substantially increases overdose risk.
High-fat mealsIncreases gabapentin absorption, can increase both efficacy and side effects. Consistent dosing with meals is recommended.

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

  • Respiratory depression, especially when combined with opioids, benzodiazepines, or alcohol; increasingly implicated in overdose deaths
  • Physical dependence, gabapentin withdrawal syndrome includes anxiety, insomnia, nausea, sweating, and seizures; risk highest with abrupt cessation after high-dose chronic use
  • Suicidality, FDA black box warning for all anticonvulsants; increased risk of suicidal thoughts and behavior
  • Mood changes / paradoxical agitation, especially in children and adolescents
  • Seizures, emergency; call 911

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 Caution, Category CPregnancy

Animal studies show developmental toxicity. Human data limited; associated with small-for-gestational-age infants. Use only if clearly indicated and benefit outweighs risk.

Use CautionBreastfeeding

Excreted in breast milk. Monitor infant for sedation and feeding difficulties. Lower-dose exposure is generally considered acceptable for seizure management.

Prescribed for Hot Flashes, Off-LabelMenopause / Hormonal

Gabapentin is frequently used off-label for menopausal hot flashes, particularly for women who cannot or choose not to use hormone therapy. It reduces hot flash frequency and severity. However, it doesn't address other menopause symptoms and carries dependence, cognitive fog, and sedation risks. Discuss the full range of menopause management options, including hormone therapy, with your doctor.

Restricted UseChildren & Teens

FDA approved for partial seizures in children 3+. Off-label use for behavior, ADHD, anxiety, and pain in children is not supported by adequate evidence. Black box warning for suicidality applies.

High RiskOlder Adults

Dizziness, ataxia, and sedation cause significant fall risk. Start at lowest dose (100mg) and titrate slowly. Renal function declines with age, dose must be adjusted for creatinine clearance.

Dose Adjustment RequiredKidney Disease

Gabapentin is renally cleared. Dose must be substantially reduced based on creatinine clearance (eGFR). Accumulation in renal impairment can cause severe toxicity.

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

Join the Conversation

Premium subscribers can share their experience and confirm others' reports.

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Stopping This Medication Safely

Taper Required, Withdrawal Can Be SevereDocumented timeframe: 4–24 weeks depending on dose and duration

Gabapentin acts on GABA and calcium channels; abrupt discontinuation after chronic use causes a withdrawal syndrome that includes severe anxiety, insomnia, nausea, sweating, and, in high-dose users, seizures. Many patients and prescribers are unaware of gabapentin dependence because it is "not a controlled substance" federally. This does not mean it is free of dependence risk.

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 protocols describe reducing by no more than 10% of the dose every 1–2 weeks
  • ·Research supports tapering over 3–6 months for high-dose users (>2400mg/day)
  • ·Research documents that abrupt discontinuation in patients using gabapentin for seizure control carries risk of breakthrough seizures
  • ·Research recommends monitoring for anxiety and insomnia, these are documented early signs of withdrawal
  • ·Research supports having an alternative pain management plan in place for the underlying condition during the stopping process

Warning Symptoms, Contact Your Doctor If You Experience:

  • Seizures, emergency; call 911
  • Extreme agitation or confusion
  • Severe sweating and tremors
  • Uncontrollable anxiety or panic
  • Any symptoms resembling alcohol or benzodiazepine withdrawal

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

Questions for Your Doctor

$2.99, printable guide for your next appointment

Questions to Ask

  • 1.Is my use of gabapentin for an FDA-approved indication, or is this off-label? What is the evidence strength for my specific condition?
  • 2.Given gabapentin is implicated in overdose deaths with opioids, can we review all my medications for this combination?
  • 3.I live in a state where gabapentin is a controlled substance, does this change how you monitor my use?
  • 4.What is the plan if this medication stops working or I want to stop, what does the taper look like?
  • 5.Have non-drug alternatives (physical therapy, alpha lipoic acid, TENS) been considered for my condition?

Lab Tests to Request

  • Renal function (eGFR), dose must match kidney function
  • PHQ-9 (depression screen, suicidality black box)
  • Abuse/misuse screen if any risk factors
  • Annual review of whether off-label use still has ongoing benefit

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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