A visual reference covering 18 widely-studied research compounds — what each one targets, which combinations are synergistic, and which pairings produce receptor competition or pharmacodynamic conflict.
Reference Map
Peptide Synergy & Conflict Map
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Research Use Only
Educational Resource
18 Compounds Reviewed
7 Stack Profiles
Peptide Synergy & Conflict Map
A visual reference covering 18 widely-studied research compounds — what each one targets, which combinations are synergistic, and which pairings produce receptor competition or pharmacodynamic conflict.
Research & Educational Use Only
This resource is intended for in vitro laboratory research and educational reference only. It is not medical advice and these compounds are not approved by the FDA for human consumption, therapeutic use, or clinical application. Real-world receptor pharmacology depends on dose, timing, route, and biological context. Researchers should consult primary literature and qualified professionals before designing protocols.
01 / Orientation
Three terms to know
A peptide is
A short chain of amino acids
Amino acids are the building blocks the body uses to make proteins. A peptide is just a short string of them — a brief signaling molecule.
A receptor is
A binding site on a cell
Cells display "locks" on their surface. A peptide is the matched "key" that fits — binding triggers a downstream signal: repair, grow, calm, fire.
A Dalton (Da) is
A unit of molecular weight
One Dalton ≈ the mass of a single hydrogen atom. So "1,419 Da" simply describes the molecule's size — bigger number, bigger molecule.
02 / Molecular Profile
Compound size and delivery
Molecular weight determines how a peptide can be delivered. Smaller peptides may be administered intranasally or sublingually; larger ones require subcutaneous injection because the gastrointestinal tract degrades them like food protein.
< 1,000 Da
Tiny
Class I
Small enough that some can be delivered as nasal sprays or sublingual drops. Cleared from the body quickly, so dosing is typically frequent.
EpitalonKPVPinealonGHK-CuSS-31IpamorelinSelankSemax
1,000–2,000 Da
Small
Class II
Still relatively small, but typically require injection for bioavailability.
Kisspeptin-10BPC-157
2,000–5,000 Da
Medium
Class III
Medium-sized and structurally complex. Injection only.
MOTS-cCJC-1295Thymosin α-1
> 5,000 Da
Protein-Sized
Class IV
Sensitive to heat and stomach acid. Strictly injectable, with cold-chain storage required to preserve tertiary structure.
TesamorelinTB-500 (full)
03 / Synergistic Stacks
Seven research stack profiles
A "stack" is a combination of compounds that target complementary mechanisms toward a unified research endpoint. Each profile below identifies the components, mechanism rationale, and timing considerations drawn from receptor pharmacology.
Stack 01 / Growth Hormone Axis
Amber
Growth Hormone Release
Two distinct receptors on the pituitary gland — GHRH and ghrelin (GHS-R1a) — engaged simultaneously for additive signaling rather than competition.
CJC-1295 (no DAC)
GHRH receptor agonist — sets the amplitude of the GH pulse.
Ipamorelin
Selective ghrelin receptor agonist — shapes pulse timing without raising cortisol or prolactin.
Mechanism: Each peptide binds a different pituitary receptor, so signals add rather than compete. CJC sets amplitude; Ipamorelin shapes timing.
Stack 02 / Tissue Regeneration
Forest
Tissue Repair
Three non-overlapping mechanisms targeting the recovery cascade: vascular supply, cell migration, and matrix synthesis.
BPC-157
Upregulates VEGFR2 to drive angiogenesis at the injury site — the supply infrastructure.
TB-500
Promotes actin-mediated cell migration to bring repair cells into position.
GHK-Cu (topical)
Modulates ~4,000 genes related to ECM remodeling and skin regeneration.
Pro tip: If running the GH stack at night, schedule the repair stack in the morning so each system has a clean signaling window.
Stack 03 / Mitochondrial Function
Brick
Mitochondrial Optimization
A multi-level approach: AMPK signaling, membrane integrity, cofactor pool, biogenesis, and salvage pathway protection.
MOTS-c
Activates AMPK — the cellular low-energy alarm that drives fuel utilization and autophagy.
SS-31
Binds cardiolipin in the inner mitochondrial membrane to prevent proton leak.
NAD+
Replenishes the cofactor pool that drives sirtuin activity and electron transport.
SLU-PP-332
ERR receptor agonist — drives mitochondrial biogenesis at the transcriptional level.
5-Amino-1MQ
Inhibits NNMT to preserve cellular NAD+ levels.
Pro tip: MOTS-c + fasted cardio is among the most-studied "exercise mimetic" pairings. Break the fast 30–60 min after dosing.
Stack 04 / Cognitive & Neuroprotective
Indigo
Neurocognitive Stack
Four non-competing mechanisms: stimulation, anxiolysis, antioxidant neuroprotection, and circadian alignment.
Semax
Raises BDNF and NGF; modulates dopamine and serotonin tone.
Selank
Gentle GABA-A modulation for anxiolysis without sedation.
Pinealon
Crosses the blood-brain barrier; protects neurons from oxidative damage.
Epitalon
Supports pineal gland function and melatonin rhythm.
Pro tip: Avoid Semax after ~3 PM if sensitive to stimulation — it can disrupt sleep onset like late-day caffeine.
Stack 05 / Bioregulator Longevity
Teal
Longevity Bioregulators
Two short peptides from the Khavinson/St. Petersburg bioregulator framework — pineal and thymic gland support.
Epitalon
Tetrapeptide (Ala-Glu-Asp-Gly) studied for telomerase activation and pineal restoration.
Thymosin α-1
Activates TLR2/TLR9; matures T-cells and natural killer cells.
Note: Khavinson's bioregulator hypothesis proposes direct peptide-DNA interaction rather than classical receptor signaling. Mechanism remains an area of active research.
Stack 06 / Body Composition
Terracotta
Lean Body Composition
Same dual-receptor logic as Stack 01, but with FDA-approved Tesamorelin as the GHRH-side agonist.
Tesamorelin
Stabilized GHRH analog — FDA-approved for visceral adipose tissue reduction.
Ipamorelin
Ghrelin receptor agonist — amplifies the GH pulse without receptor overlap.
Pro tip: A second fasted-morning dose of Ipamorelin alone can drive an additional pulse. Do not double-dose Tesamorelin — receptor desensitization results.
Stack 07 / Reproductive Axis
Rose
Sex-Hormone Reset
Endogenous reactivation of the HPG axis via KISS1R signaling — orthogonal to all other stacks on this list.
Kisspeptin-10
KISS1R agonist — triggers GnRH → LH/FSH cascade for endogenous testosterone or estrogen production.
Stacking note: KISS1R signaling is independent of every other system here, so Kisspeptin layers cleanly on top of any other stack.
04 / Pharmacodynamic Conflicts
Where combinations clash
Some pairings produce receptor competition, opposing signaling, or temporal conflicts. The following are documented points of caution drawn from receptor pharmacology.
Same Receptor
Tesamorelin + CJC-1295
Both are GHRH receptor agonists competing for the identical binding site. The result is not synergy — it's competitive antagonism risking receptor desensitization. Choose one, then layer Ipamorelin (different receptor) on top.
Opposing Effect
Thymosin α-1 vs. KPV
Thymosin α-1 upregulates immune signaling. KPV downregulates NF-κB-mediated inflammation. Different mechanisms, opposite directions — KPV may quiet the immune response Thymosin α-1 is meant to stimulate.
Wrong Timing
KPV in first 72 hr post-injury
Acute inflammation drives the recruitment of repair cells and angiogenic signaling. Suppressing it too early via KPV can blunt the very cascade that BPC-157 and TB-500 promote. Reserve KPV for chronic, not acute, inflammation.
Receptor Saturation
Multiple ghrelin-receptor releasers
Ipamorelin is the sole GHS-R1a agonist on this list. Adding a second (MK-677, GHRP-2, GHRP-6) does not amplify GH release — it desensitizes the receptor. Use one at a time.
Minor Note
Selank + Semax (high doses)
Both are degraded by prolyl endopeptidase. Most stacking protocols are uneventful, but very high concurrent doses may slow each other's clearance. Pharmacokinetic note rather than a true conflict.
Minor Note
SLU-PP-332 + GH stack
Overlapping downstream pathways for fat oxidation and energy production. Not a conflict, but expect diminishing returns rather than additive effect.
05 / Application Index
Goal-to-stack reference
Research Goal
Stack Profile
Avoid
GH axis modulation
CJC-1295 + Ipamorelin or Tesamorelin + Ipamorelin
CJC + Tesamorelin (same receptor)
Tissue repair
BPC-157 + TB-500 (+ topical GHK-Cu)
KPV in first 72 hr
Mitochondrial function
MOTS-c + SS-31 + NAD+ + SLU-PP-332 + 5-Amino-1MQ
—
Cognition + anxiolysis
Semax + Selank + Pinealon
—
Anti-aging / circadian
Epitalon + Thymosin α-1
—
HPG axis reset
Kisspeptin (mono or layered)
—
Immune support
Thymosin α-1
Concurrent KPV
Chronic inflammation
KPV
Active healing protocols
06 / Reference
Terminology glossary
- AMPK
- 5′ AMP-activated protein kinase — the cellular "low-energy alarm" that drives fuel utilization and autophagy when ATP is depleted.
- BBB
- Blood-brain barrier — selective interface protecting the CNS from circulating molecules. Smaller peptides (e.g., Pinealon) can cross.
- BDNF
- Brain-derived neurotrophic factor. Supports neuronal plasticity and survival.
- ECM
- Extracellular matrix — the structural network between cells. Modulated by GHK-Cu.
- GABA-A
- Major inhibitory ionotropic receptor in the CNS. Selank acts as a gentle modulator.
- GH
- Growth hormone — released by the anterior pituitary, primarily during slow-wave sleep.
- GHRH
- Growth hormone-releasing hormone — hypothalamic signal that triggers pituitary GH release. Mimicked by CJC-1295 and Tesamorelin.
- GHS-R1a
- Ghrelin receptor on the pituitary — second pathway for GH release. Activated by Ipamorelin.
- KISS1R
- Kisspeptin receptor. Triggers the GnRH → LH/FSH cascade upstream of testosterone/estrogen production.
- NAD+
- Nicotinamide adenine dinucleotide — essential cofactor for sirtuins and electron transport. Declines with age.
- NF-κB
- Master transcription factor regulating inflammatory gene expression. KPV suppresses its activation.
- NNMT
- Nicotinamide N-methyltransferase — enzyme that consumes NAD+ precursors. Inhibited by 5-Amino-1MQ.
- Telomerase
- Ribonucleoprotein enzyme that maintains telomeres (chromosome end caps). Studied as activated by Epitalon in human somatic cells.
- VEGFR2
- Vascular endothelial growth factor receptor 2 — drives angiogenesis. Upregulated by BPC-157.
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