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

DermorphinvsTriptorelin

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-ApprovedHUMAN-REVIEWED16/64 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)
Triptorelin
GnRH Agonist · FDA-Approved
3.75–22.5 mgDepot dose rangeYee 2025Chen 2024
<50 ng/dLTestosterone target
1–6 monthsDepot durationYee 2025Chen 2024
IM · Depot Injection · Monthly to 6-MonthlyYee 2025

01Mechanism of Action

Parameter
Dermorphin
Triptorelin
Primary target
μ-opioid receptors (central and peripheral)Negri 1992Steel 2014
Pituitary GnRH receptorsUnknown 2012
Pathway
μ-receptor activation → G-protein coupling → adenylyl cyclase inhibition → neuronal hyperpolarization
GnRH receptor agonism → initial flare (LH/FSH spike) → receptor desensitization → sustained LH/FSH suppression
Downstream effect
Potent analgesia, reduced nociceptive signaling, opioid-mediated CNS and peripheral effects
Castration-level suppression of testosterone (men) and estrogen (women) within 2–4 weeks post-flare
Feedback intact?
N/A — exogenous opioid agonist
No — bypasses physiological pulsatility; continuous agonism produces paradoxical suppression
Origin
Phyllomedusa sauvagei and P. bicolor frog skin — gene-encoded with natural D-amino acid incorporationAmiche 1998Mignogna 1992
Synthetic decapeptide analogue of native GnRH with amino acid substitutions for enhanced receptor affinity and stability
Antibody development
Site-directed antibodies produced for detection and purificationCucumel 1996

02Dosage Protocols

Parameter
Dermorphin
Triptorelin
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
Multiple Phase 3 RCTs · FDA-approved 1999
Human toxicity
Kambô ritual (P. bicolor skin) — violent emesis, vasodilation, fluid shifts, ADH dysregulationTran 2025
1-month depot
3.75 mg IM
Most common formulation for prostate cancer.
3-month depot
11.25 mg IMYee 2025
Reduced injection frequency.
6-month depot
22.5 mg IMYee 2025Chen 2024
Long-acting formulation; improved adherence in real-world use.Yee 2025
Administration route
Intramuscular (IM) — gluteal or deltoid
Frequency
Every 1, 3, or 6 months per formulation
Indication: Prostate cancer
Advanced (metastatic or locally advanced)
Androgen deprivation therapy (ADT) backbone.
Indication: Endometriosis
3.75 mg monthly
FDA-approved; typically 6-month course.
Indication: Central precocious puberty
Pediatric use (≥2 years)Jia 2025
Weight-based dosing per FDA label.
Duration (prostate cancer)
Continuous or intermittent ADT protocolsPreston 2024
Intermittent ADT may reduce side effects; cardiovascular risk similar to continuous.
Monitoring
Serum testosterone, PSA (prostate cancer), bone density, lipids, glucose

04Side Effects & Safety

Parameter
Dermorphin
Triptorelin
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
Initial flare symptoms
Bone pain, urinary obstruction, spinal cord compression (first 2 weeks)
Antiandrogen co-treatment (bicalutamide) mitigates flare in metastatic disease.
Cardiovascular events
MI, stroke, arrhythmia — GnRH agonists show higher CV risk vs antagonists in meta-analysesPatel 2025Preston 2024
Hot flashes
Very common (>60%); vasomotor instability
Bone loss / Osteoporosis
Accelerated bone mineral density decline; fracture risk ↑Friedrich 2025
Baseline DEXA scan recommended; bisphosphonates or denosumab may be indicated.
Metabolic syndrome
Weight gain, insulin resistance, dyslipidemia, diabetes risk
Sexual dysfunction
Erectile dysfunction, loss of libido (expected pharmacological effect)Jia 2025
Injection site reactions
Pain, erythema, sterile abscess (rare with depot formulations)
Gynecomastia / Breast tenderness
Common (10–20%); peripheral aromatization of residual androgens
Fatigue / Mood changes
Anemia, depression, cognitive changes reported in long-term ADT
Hepatotoxicity
Transient transaminase elevations; clinically apparent liver injury rare
Racial differences (ADT)
Black veterans show higher CV event rates vs White veterans on GnRH agonists
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
Triptorelin
  • ·Hypersensitivity to triptorelin, GnRH, or GnRH agonist analogues
  • ·Pregnancy (Category X)
Relative Contraindications
Dermorphin
  • ·Any context outside approved animal research protocols
  • ·CNS depressant co-administration
Triptorelin
  • ·Active cardiovascular disease — consider GnRH antagonist alternative
  • ·Metastatic vertebral disease with spinal cord compression risk (flare hazard)
  • ·Severe urinary obstruction — may worsen during flare
  • ·Osteoporosis or high fracture risk (requires bone-protective therapy)

05Administration Protocol

Parameter
Dermorphin
Triptorelin
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.
Choose 1-month (3.75 mg), 3-month (11.25 mg), or 6-month (22.5 mg) depot based on adherence needs and clinical context. 6-month formulation shows improved real-world adherence in Asia-Pacific cohorts.
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.
Intramuscular — gluteal or deltoid muscle. Use 21–23G needle. Aspirate to confirm non-vascular placement. Rotate sites with repeat injections.
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
For metastatic prostate cancer: co-administer antiandrogen (e.g., bicalutamide 50 mg daily) starting 1 week before first injection and continuing 2–4 weeks to prevent tumor flare.
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
Baseline: testosterone, PSA, bone density (DEXA), lipids, glucose. Follow-up: testosterone at 4 weeks (confirm <50 ng/dL castration), PSA monthly × 3, then quarterly. Annual DEXA for bone loss.
5. Storage
Store vials at room temperature (20–25 °C), protect from light. Do not freeze. Reconstituted suspension should be used immediately.
6. Intermittent ADT protocol (optional)
Some protocols use on-treatment periods (9–12 months) alternating with off-treatment intervals until PSA rises. Cardiovascular risk appears similar to continuous ADT.