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Specimen Atlas of Research Peptides81 plates · MIT
PeptidesDBan atlas
Side-by-side · Research reference

DermorphinvsTesamorelin

Side-by-side comparison across mechanism, dosage, evidence, side effects, administration, and stack synergies. Citations on every claim where available.

AAnimal-StrongHUMAN-REVIEWED20/47 cited
BFDA-ApprovedFlagship27/68 cited
Dermorphin
Opioid Peptide · μ-Receptor Agonist · Research Only
~30×Morphine potency
μ-selectiveReceptor typeNegri 1992
D-Ala²Unique featureAmiche 1998
Research only · ICV / SC (animal models)
Tesamorelin
GHRH Analogue · FDA-Approved
2 mgDaily doseEGRIFTA® (tesamorelin for inje 2010
15–20%VAT reductionFalutz 2010
~26 minHalf-lifeEGRIFTA® (tesamorelin for inje 2010
SQ · Abdomen · Once Daily

01Mechanism of Action

Parameter
Dermorphin
Tesamorelin
Primary target
μ-opioid receptors (central and peripheral)Negri 1992Steel 2014
Hypothalamic GHRH receptorsEGRIFTA® (tesamorelin for inje 2010
Pathway
μ-receptor activation → G-protein coupling → adenylyl cyclase inhibition → neuronal hyperpolarization
GHRH → Pituitary GH release → Liver IGF-1 synthesisFalutz 2007
Downstream effect
Potent analgesia, reduced nociceptive signaling, opioid-mediated CNS and peripheral effects
Increased GH pulsatility, elevated IGF-1, lipolysis of visceral adipose tissueFalutz 2010
Feedback intact?
N/A — exogenous opioid agonist
Yes — physiological pulsatility preserved
Origin
Phyllomedusa sauvagei and P. bicolor frog skin — gene-encoded with natural D-amino acid incorporationAmiche 1998Mignogna 1992
Synthetic 44-AA GHRH analogue with trans-3-hexenoic-acid modification for stabilityEGRIFTA® (tesamorelin for inje 2010
Antibody development
Site-directed antibodies produced for detection and purificationCucumel 1996
~50% after 26 wks (non-neutralising in most)Sévigny 2018

02Dosage Protocols

Parameter
Dermorphin
Tesamorelin
Legal status
Controlled substance in many jurisdictions · Research only
Not approved for human use.
Animal research (ICV)
Low nanomolar to picomolar range
Intracerebroventricular administration in rodent models.
Detection limit (doping)
5 pg/mL in equine plasma/urineSteel 2014
High-throughput LC-MS/MS screen developed for racing industry.
Duration of action
10–120 minutes (dose-dependent, intrathecal)
Evidence basis
Animal studies · In vitro assays
RCT / FDA-approvedFalutz 2007Falutz 2010
Human toxicity
Kambô ritual (P. bicolor skin) — violent emesis, vasodilation, fluid shifts, ADH dysregulationTran 2025
Standard dose
2 mg / dayEGRIFTA® (tesamorelin for inje 2010
FDA-approved protocol.
Frequency
Once daily (morning or pre-sleep)
Aligns with natural GH pulse.
Lower / starter dose
1 mg / dayFalutz 2010
1 mg still produces significant IGF-1 elevation.
Duration
12–52 weeks
VAT returns within months of stopping.
Reconstitution
Sterile water per labeling
Preserved at 2–8 °C after reconstitution.
Timing
Empty stomach, pre-sleep preferred
Half-life
~26 min (plasma)EGRIFTA® (tesamorelin for inje 2010
Modified vs native GHRH (7 min t½).

03Metabolic / Fat Loss Evidence

Parameter
Dermorphin
Tesamorelin
Primary fat target
Visceral adipose tissue (VAT) — abdominal
Quantified reduction
15–20% VAT ↓Falutz 2010
By CT at 26 weeks (Falutz et al., NEJM).
IGF-1 impact
+66 ng/mL (2 mg dose) · +81% mean elevationFalutz 2007
Effect on lean mass
Modest lean mass preservation / slight increase
Insulin sensitivity
Neutral to slight impairment (monitor HbA1c)Clarke 2018
Triglycerides
Significant TG reduction noted in Phase 3Falutz 2010
Glucose metabolism
Generally neutral; 4.5% HbA1c elevation riskClarke 2018
Effect reversibility
VAT returns within months of stopping
Key publication
Falutz et al. NEJM 2007 · Falutz JCEM 2010 · FDA approval 2010Falutz 2007Falutz 2010EGRIFTA® (tesamorelin for inje 2010

04Side Effects & Safety

Parameter
Dermorphin
Tesamorelin
Opioid effects
Respiratory depression, sedation, euphoria, tolerance, dependence risk
CNS effects
Analgesia (high-affinity sites), catalepsy (low-affinity sites)Negri 1992
Kambô ritual toxicity
Violent emesis, vasodilation, profound fluid shifts, hyponatremia, ADH dysregulation, brain death (case report)Tran 2025
Peripheral effects
GI motility inhibition (ileum > vas deferens in vitro)Negri 1992
Receptor selectivity caveat
Two μ-receptor subtypes — differential behavioral effects (analgesia vs. catalepsy)Negri 1992
Proteolytic stability
Tyr³-Pro⁶ bond relatively unstable; endogenous enzymes may produce tetrapeptide fragmentsCucumel 1996
Injection site reaction
Erythema, pruritus, redness (common)
Fluid retention / Edema
Peripheral edema, arthralgia, carpal tunnel (GH-axis effect)
Glucose intolerance
HbA1c ↑ in 4.5% vs 1.3% placebo; HbA1c ≥6.5% hazard OR 3.3Clarke 2018
IGF-1 elevation
Dose-dependent; supraphysiological levels = discontinue
Cancer risk
Contraindicated in active malignancy (GH/IGF-1 axis); theoretical tumour growth riskEGRIFTA® (tesamorelin for inje 2010
Antibody formation
~50% at 26 weeks; non-neutralising in most; rare hypersensitivity (<1%)Sévigny 2018
GI symptoms
Nausea, diarrhea (mild, transient)
Pregnancy / OB
ContraindicatedEGRIFTA® (tesamorelin for inje 2010
Absolute Contraindications
Dermorphin
  • ·Human use — not approved by any regulatory authority
  • ·Controlled substance status — possession illegal in many jurisdictions
  • ·Known opioid hypersensitivity or respiratory compromise
Tesamorelin
  • ·Active malignancy or history of treated cancer
  • ·Pregnancy
  • ·Hypersensitivity to tesamorelin or mannitol
  • ·Disruption of hypothalamic-pituitary axis (trauma, tumour, radiation)
Relative Contraindications
Dermorphin
  • ·Any context outside approved animal research protocols
  • ·CNS depressant co-administration
Tesamorelin
  • ·Untreated diabetes (monitor HbA1c)
  • ·Severe carpal tunnel syndrome
  • ·Acute critical illness

05Administration Protocol

Parameter
Dermorphin
Tesamorelin
1. Legal and ethical framework
Dermorphin is a controlled substance in many jurisdictions and is not approved for human use. Possession, synthesis, or distribution may be illegal. Use is restricted to licensed research settings under institutional review.
Add 2.1 mL sterile water to 2 mg lyophilised vial. Roll gently — do not shake. Solution should be clear.
2. Animal research protocols
In rodent models, intracerebroventricular (ICV) or intrathecal injection is used at nanomolar to picomolar concentrations. Subcutaneous administration also documented. All protocols require IACUC approval.
Subcutaneous — abdomen preferred. Rotate sites (avoid same spot within 2 cm). Avoid navel and waistband area.
3. Analytical detection
High-throughput LC-MS/MS screens developed for anti-doping programs detect dermorphin and 17 related peptides in equine and human urine/plasma at limits as low as 5 pg/mL.Steel 2014
Once daily. Preferred: evening, 2–3 hrs post-meal, before sleep — aligns with natural GH secretion pulse.
4. Kambô ritual (traditional use)
Application of Phyllomedusa bicolor skin secretions to superficial burns. Not recommended — associated with severe toxicity including violent emesis, hyponatremia, and documented case of brain death.Tran 2025
Lyophilised: room temp, light-protected. Reconstituted: refrigerate 2–8 °C, use within 21 days.
5. Needle
27–31G, 4–8 mm insulin syringe. Pinch skin, 45° angle for lean individuals.

06Stack Synergy

Dermorphin
— no documented stacks
Tesamorelin
+ Ipamorelin
Strong
View Ipamorelin

Tesamorelin (GHRH analogue) and ipamorelin (GHRP / ghrelin mimetic) act on two distinct receptor systems to amplify GH release synergistically — GHRH receptor + ghrelin receptor. This dual-axis stimulation produces a more robust, sustained GH pulse than either alone while maintaining physiological pulsatility. Ipamorelin is highly selective with minimal cortisol or prolactin elevation, making it the preferred GHRP pairing.

Tesamorelin
2 mg SQ · evening
Ipamorelin
200–300 mcg SQ · same injection
Frequency
Once daily, pre-sleep
Primary benefit
Maximal GH pulsatility, fat loss, recovery, sleep quality
Raun 1998