Dosage protocol

Pramiracetam dosage

Evidence-based dose range, timing, and adjustment guidance for Pramiracetam. Always start at the low end and titrate; individual response varies and dose-response curves are not always linear.

Standard range

300–600 mg

Frequency

2-3 doses

Half-life

Onset

30min

Starting dose

Start at 300 mg — the lower end of the clinical range — for the first 3–7 days to assess tolerance and individual response. Most people who do not feel the expected effect at the low end need to titrate up to the midpoint (~450 mg) over 1–2 weeks before evaluating whether Pramiracetam works for them. Some users — particularly those with smaller body mass or sensitive baseline neurochemistry — find the low end fully sufficient.

Timing

Recommended timing: AM/midday.

Half-life context: moderate — single morning dose usually adequate.

With or without food

with fat: Pramiracetam is fat-soluble — bioavailability improves substantially when taken with a meal containing some dietary fat. Empty-stomach dosing is wasteful at best and produces inconsistent effects at worst.

Protocol note

Lipophilic — take with fat.

Dose adjustment

·Body weight: Doses in the clinical literature are typically calibrated to a 70 kg adult. Smaller users (under 60 kg) often respond at 70–80% of the standard dose; larger users (over 90 kg) sometimes need 110–130%.
·CYP1A2/CYP2D6 metabolism: Caffeine, modafinil, and most racetams are CYP1A2-metabolised; slow metabolisers need lower doses and longer dose intervals. Yohimbine and several stimulants are CYP2D6-metabolised. Genotyping (23andMe raw data → Promethease) reveals these polymorphisms.
·Tolerance management: Receptor-binding compounds (stimulants, GABAergics, opioidergics) develop tolerance with daily use. Cycling 5 days on / 2 days off, or 4 weeks on / 1 week off, preserves response. Foundation supplements (omega-3, vitamin D, magnesium) do not require cycling.
·Concurrent stack: Effective dose can fall when stacked with synergistic compounds. The classic example is caffeine + L-theanine, where 50–100 mg caffeine often outperforms 200 mg solo on subjective focus measures.

When to reduce or stop

Persistent headache, GI upset, or sleep disruption that does not resolve over 5–7 days suggests a dose reduction or compound change.
Any cardiovascular symptoms (palpitations, chest tightness, blood pressure spikes) — stop immediately and reassess. Re-introduce only at half the original dose.
Mood changes — apathy, persistent anxiety, agitation, or depressive symptoms emerging during a new protocol warrant immediate review with a clinician.

Mechanism, safety, evidence, and citations for Pramiracetam are on the main reference page — see Pramiracetam. To check interactions with other compounds in your stack, use the interaction checker.

Dose ranges on this page reflect the clinical and supplement literature for healthy adults. They are not medical advice. Individual response varies; pregnancy, lactation, prescription medications, and pre-existing health conditions can all change the appropriate dose. Coordinate with a qualified clinician before establishing a personal protocol. See our full disclaimer.