Skip to content
BiologicalX

Comparison

Berberine vs GHRP-6

Side-by-side of Berberine and GHRP-6. Every row below is pulled from the compound schema and will update as our data grows. For deeper reads, follow through to each compound page.

natural

Berberine

Berberine supplement guide: 1500 mg/day lowers fasting glucose and HbA1c, AMPK activation, metformin parity in RCTs, dihydroberberine absorption.
peptide

GHRP-6

First-generation hexapeptide ghrelin-receptor agonist. Pioneered the GHS-R1a pathway in the 1980s. Produces the strongest hunger response among GHRPs and a mo.

Effects at a glance

Berberine

  • Lowers HbA1c by ~0.7% versus placebo at 1500 mg/day across 27-trial meta-analysis (Lan 2015)
  • Roughly comparable to metformin on fasting glucose and HbA1c in small head-to-head RCTs (Yin 2008)
  • Reduces LDL cholesterol 10-20% and triglycerides 15-25% via PCSK9 inhibition
  • Activates AMPK, the cellular energy sensor that drives insulin-independent glucose uptake
  • Oral bioavailability under 1%; dihydroberberine is the higher-absorption alternative at lower doses
  • GI side effects affect 10-30% at 1500 mg/day; split dosing with meals reduces incidence

GHRP-6

  • First-generation hexapeptide ghrelin-receptor agonist; foundational to the GHRP class
  • Strongest appetite stimulation of any synthetic GHRP at equivalent GH doses
  • Produces measurable cortisol and prolactin rise alongside the GH pulse
  • Anecdotal protocols use 100 to 200 mcg subcutaneously 2 to 3 times daily on an empty stomach
  • Largely superseded by ipamorelin (cleaner profile) and GHRP-2 (stronger pulse) for body-composition use
  • Banned by WADA under S2; detection methods validated in accredited labs

Side-by-side

Attribute Berberine GHRP-6
Category natural peptide
Also known as berberine HCl, berberine hydrochloride Growth Hormone Releasing Peptide 6, SKF-110679, Histidyl-D-Tryptophyl-Alanyl-Tryptophyl-D-Phenylalanyl-Lysinamide
Half-life (hr) 3 0.5
Typical dose (mg) 1500 0.1
Dosing frequency 3x daily with meals 2-3x daily
Routes oral subcutaneous, intravenous
Onset (hr) 2 0.25
Peak (hr) 3 0.5
Molecular weight 336.36 872.44
Molecular formula C20H18NO4+ C46H56N12O6
Mechanism Activates AMP-activated protein kinase (AMPK), suppressing hepatic gluconeogenesis and lipogenesis while increasing peripheral glucose uptake. Inhibits PCSK9 transcription, modulates bile acid signaling, and shifts gut microbiome composition. Hexapeptide agonist of GHS-R1a (ghrelin receptor). Suppresses hypothalamic somatostatin and stimulates pituitary somatotrophs, with strong central NPY/AgRP appetite signaling and modest cortisol and prolactin release.
Legal status Dietary supplement (US, EU, UK, Canada); Rx in some Asian jurisdictions Not FDA approved; research-use-only grey market; banned by WADA
WADA status allowed banned
DEA / Rx Not scheduled Not scheduled (research chemical)
Pregnancy Contraindicated (kernicterus risk in neonates) Insufficient data; not recommended
CAS 2086-83-1 87616-84-0
PubChem CID 2353 9919072
Wikidata Q411435 Q5519921

Safety profile

Berberine

Common side effects

  • constipation
  • diarrhea
  • abdominal cramping
  • flatulence
  • nausea

Contraindications

  • pregnancy
  • lactation
  • neonatal jaundice
  • severe liver disease

Interactions

  • metformin: additive HbA1c reduction; additive GI side effects(moderate)
  • insulin or sulfonylureas: additive hypoglycemia risk; dose adjustment may be required(major)
  • statins (simvastatin, atorvastatin): CYP3A4 inhibition raises statin plasma levels(moderate)
  • cyclosporine: raises cyclosporine levels through CYP3A4 and P-gp inhibition(major)
  • calcium channel blockers (amlodipine): elevated plasma levels via CYP3A4 inhibition(moderate)

GHRP-6

Common side effects

  • intense hunger
  • water retention
  • vivid dreams
  • head pressure or flushing
  • tingling at injection site
  • transient lethargy

Contraindications

  • pregnancy
  • active malignancy
  • history of pituitary tumor
  • uncontrolled diabetes
  • prolactin sensitivity

Interactions

  • CJC-1295: synergistic GH release; commonly co-administered(minor)
  • sermorelin: additive GH release via parallel GHRH and ghrelin pathways(minor)
  • insulin: sustained GH can blunt insulin sensitivity over weeks(moderate)
  • corticosteroids: blunt GH response and amplify cortisol load(moderate)

Which Should You Take?

Berberine comes out ahead for most readers on the criteria we weight: 3 catalogued goals, OTC dietary supplement, oral dosing, with a Tier-B outcome catalogued. GHRP-6 is the right call when one of the conditionals below applies.

  • If your priority is metabolic health and glucose control, pick Berberine.
  • If your priority is healthspan extension, pick Berberine.
  • If your priority is growth-hormone axis, pick GHRP-6.
  • If your priority is appetite regulation, pick GHRP-6.

Edge case: If you want to avoid research-only / gray-market sourcing, Berberine is the more accessible choice.

Default choice: Berberine. Lower friction to source, and broader goal coverage. Reach for GHRP-6 only if your priority sits squarely in the goals it owns above.

This verdict is generated from each compound's schema (goals, legal status, evidence outcomes, dosing route). It updates automatically as our compound data evolves; the deeper read sits on each individual compound page.

Common questions

What is the difference between Berberine and GHRP-6?

Berberine and GHRP-6 differ in category (natural vs peptide), mechanism, and typical dosing. See the side-by-side table for full details.

Which has a longer half-life, Berberine or GHRP-6?

Berberine half-life is 3 hours; GHRP-6 half-life is 0.5 hours.

Can you stack Berberine with GHRP-6?

Stack compatibility depends on mechanism overlap, legal status, and individual response. Check each compound page for specific interactions and contraindications before combining.

Go deeper

Berberine full profile → GHRP-6 full profile → All compounds →