PeptidesCategoriesResearch

Leu-Enkephalin

Leu-enkephalin (YGGFL) is an endogenous opioid pentapeptide and preferential delta-opioid receptor agonist involved in pain modulation, mood regulation, immune function, and stress response.

Leu-enkephalin (leucine-enkephalin, Tyr-Gly-Gly-Phe-Leu) is one of two endogenous enkephalin pentapeptides discovered by John Hughes and Hans Kosterlitz in 1975. As a preferential delta-opioid receptor (DOR) agonist, leu-enkephalin plays fundamental roles in endogenous pain modulation, mood regulation, reward processing, and immune system function.

Overview

Leu-enkephalin and met-enkephalin were the first endogenous opioid peptides identified, fundamentally changing our understanding of pain perception and reward neuroscience. Their discovery in pig brain extracts by Hughes, Kosterlitz, and colleagues demonstrated that the brain produces its own morphine-like compounds, explaining why opiate drugs are effective -- they mimic endogenous signaling molecules. Leu-enkephalin differs from met-enkephalin only at the C-terminal position (leucine versus methionine), yet this single substitution confers distinct receptor selectivity, metabolic stability, and biological roles. Leu-enkephalin is derived from the proenkephalin gene product but also from prodynorphin processing, giving it a broader distribution pattern than met-enkephalin.

Mechanism of Action

Leu-enkephalin exerts its primary effects through activation of delta-opioid receptors (DOR), with lower affinity for mu-opioid receptors (MOR) and minimal kappa-opioid receptor (KOR) activity. The peptide's N-terminal tyrosine residue is critical for opioid receptor binding -- the free amine and phenolic hydroxyl groups form essential hydrogen bonds with conserved receptor residues in the binding pocket.

Delta-opioid receptor signaling: DOR activation by leu-enkephalin triggers Gi/Go protein coupling, leading to (1) inhibition of adenylyl cyclase and reduced cAMP production, (2) opening of G protein-coupled inwardly rectifying potassium channels (GIRKs) producing membrane hyperpolarization, and (3) inhibition of voltage-gated calcium channels, reducing neurotransmitter release. In pain circuits, this presynaptic inhibition reduces substance P and glutamate release from nociceptive primary afferents in the spinal dorsal horn (Stein et al., 2003).

Immune modulation: Leu-enkephalin enhances natural killer (NK) cell cytotoxic activity and modulates T cell proliferation through opioid receptors expressed on immune cells. DOR activation on lymphocytes influences cytokine production and cell migration, establishing enkephalins as neuroimmune mediators (Plotnikoff et al., 1986).

Enzymatic degradation: Leu-enkephalin is rapidly inactivated by two primary peptidases: neutral endopeptidase (NEP/enkephalinase, EC 3.4.24.11), which cleaves the Gly3-Phe4 bond, and aminopeptidase N (APN, EC 3.4.11.2), which removes the N-terminal tyrosine. This dual degradation pathway produces an in vivo half-life of approximately 2-3 minutes, severely limiting therapeutic utility of the native peptide.

Reconstitution Calculator

Reconstitution Calculator

Calculate your peptide dosing

Draw Volume
0.100mL
Syringe Units
10units
Concentration
2,500mcg/mL
Doses / Vial
20doses
Vial Total
5mg
Waste / Vial
0mcg
Syringe Cap.
100units · 1mL
How to reconstitute
Gather & prepare
1/6Gather & prepare

Set up a clean workspace with all supplies ready.

1.Wash hands thoroughly, put on disposable gloves
2.Your 5mg peptide vial (lyophilized powder)
3.Bacteriostatic water (you'll need 2mL)
4.A 3–5mL syringe with 21–25 gauge needle for reconstitution
5.Alcohol swabs (70% isopropyl)
Use bacteriostatic water (0.9% benzyl alcohol) for multi-dose vials. Sterile water is only safe for single-use.
Supply Planner

7x / week for weeks

·
40%
2vials
28 doses20 days/vial12 leftover
Cost Breakdown
Vial price
$0.00per dose
$0.00 /week$0 /month
Store 2-8°C30 day shelf lifeSwirl gentlyFor research purposes only

Research

Pain Modulation

Leu-enkephalin contributes to descending pain inhibition through DOR activation in the periaqueductal gray (PAG), rostral ventromedial medulla (RVM), and spinal dorsal horn. DOR-selective agonism produces analgesia with reduced respiratory depression and constipation compared to mu-opioid agonists, making delta-selective compounds an active area of analgesic drug development. Ossipov et al. (2004) demonstrated that DOR activation modulates chronic pain states particularly effectively, suggesting enkephalin-based approaches may be better suited for persistent rather than acute pain.

Mood and Reward

Enkephalinergic neurons are densely distributed in the nucleus accumbens, ventral tegmental area, and amygdala -- key nodes of the reward and emotional regulation circuits. Leu-enkephalin release in these regions contributes to natural reward processing, hedonic experience, and stress buffering. DOR knockout mice show increased anxiety-like behavior and depressive phenotypes, confirming the role of delta-opioid signaling in mood regulation (Filliol et al., 2000).

Immune Function

Leu-enkephalin enhances NK cell activity at low concentrations (10^-12 to 10^-10 mol/L) through DOR expressed on NK cells. This immunostimulatory effect is blocked by the opioid antagonist naloxone, confirming receptor-mediated action. Research has also demonstrated that leu-enkephalin modulates T cell responses, macrophage chemotaxis, and antibody production, establishing it as a bidirectional immunomodulator whose effects depend on concentration and immune activation state (Plotnikoff et al., 1986).

Cardioprotection

DOR activation by leu-enkephalin and related agonists provides cardioprotection during ischemia-reperfusion injury. DOR activation preconditions cardiomyocytes by activating mitochondrial KATP channels and reducing intracellular calcium overload during reperfusion. Schultz et al. (1997) demonstrated that endogenous enkephalin release contributes to ischemic preconditioning in cardiac tissue.

Safety Profile

As an endogenous peptide, leu-enkephalin operates within established physiological signaling systems. The primary limitation is its extremely short half-life (~2-3 minutes), which restricts exogenous therapeutic use. At supraphysiological concentrations, DOR activation can produce seizure-like activity in rodent models, though this effect is less pronounced than with delta-selective non-peptide agonists. Unlike mu-opioid agonists, DOR-selective compounds produce minimal respiratory depression, constipation, and physical dependence at analgesic doses. Tolerance to delta-opioid analgesia develops more slowly than to mu-opioid analgesia. The rapid degradation of native leu-enkephalin by NEP and aminopeptidases serves as a built-in safety mechanism preventing accumulation.

Pharmacokinetic Profile

Leu-Enkephalin — Pharmacokinetic Curve

0%25%50%75%100%0m3m5m7m10m12mTimeConcentration (% peak)T_max 1mT_1/2 3m
Half-life: 3mT_max: 1mDuration shown: 12m

Molecular Structure

2D Structure
Leu-Enkephalin molecular structure
Molecular Properties
Formula
C28H37N5O7
Weight
555.6 Da
CAS
58822-25-6
PubChem CID
443363
Exact Mass
573.2257 Da
LogP
-2.1
TPSA
225 Ų
H-Bond Donors
7
H-Bond Acceptors
9
Rotatable Bonds
16
Complexity
847
Identifiers (SMILES, InChI)
InChI
InChI=1S/C27H35N5O7S/c1-40-12-11-21(27(38)39)32-26(37)22(14-17-5-3-2-4-6-17)31-24(35)16-29-23(34)15-30-25(36)20(28)13-18-7-9-19(33)10-8-18/h2-10,20-22,33H,11-16,28H2,1H3,(H,29,34)(H,30,36)(H,31,35)(H,32,37)(H,38,39)/t20-,21-,22-/m0/s1
InChIKeyYFGBQHOOROIVKG-FKBYEOEOSA-N

Research Protocols

intranasal Injection

Intranasal delivery has been explored as a route to CNS access, bypassing the blood-brain barrier through olfactory nerve transport.

GoalDoseFrequency
Rodents producing analgesia equivalent to40-160 mg, 3-5 mgPer protocol

intravenous Injection

Following intravenous administration, the peptide is immediately available systemically but is degraded within minutes.

GoalDoseFrequency
Rodents producing analgesia equivalent to40-160 mg, 3-5 mgPer protocol

oral

Absorption Leu-enkephalin is not orally bioavailable due to rapid degradation by gastrointestinal peptidases and first-pass hepatic metabolism.

GoalDoseFrequency
Rodents producing analgesia equivalent to40-160 mg, 3-5 mgPer protocol

intrathecal Injection

Intrathecal leu-enkephalin at 10-100 microg produces spinal analgesia lasting 15-30 minutes in rodent models. Continuous intrathecal infusion at 1-5 microg/hour maintains analgesia but requires implanted pumps due to the short half-life.

GoalDoseFrequency
RB101 at 40-160 mg/kg IV40-160 mg, 3-5 mgPer protocol

Interactions

Peptide Interactions

Enkephalinase Inhibitorssynergistic

The most pharmacologically rational approach to enhancing leu-enkephalin signaling is co-administration with NEP and/or APN inhibitors. Thiorphan (NEP inhibitor) and bestatin (APN inhibitor) individually extend enkephalin half-life 2-3 fold; combined, they extend it 5-10 fold and produce robust a...

Met-Enkephalinsynergistic

Leu-Enkephalin + Met-Enkephalin (Endogenous Synergy) Both enkephalins are co-released from proenkephalin-expressing neurons.

Selanksynergistic

Selank, a synthetic tuftsin analogue, modulates enkephalin metabolism by influencing carboxypeptidase activity and may indirectly enhance endogenous enkephalin levels. The anxiolytic effects of selank may partially operate through potentiation of enkephalinergic signaling.

What to Expect

What to Expect

Onset

Rapid onset expected; half-life of ~2-3 minutes (plasma) indicates fast-acting pharmacokinetics

23 minutes

Intrathecal leu-enkephalin at 10-100 microg produces spinal analgesia lasting 15-30 minutes in rodent models.

Daily Use

Due to short half-life (~2-3 minutes (plasma)), effects are expected per-dose; consistent daily administration maintains therapeutic levels

Ongoing

Regular administration schedule required; effects are dose-dependent and do not persist between doses

Quality Indicators

What to look for

  • Multiple peer-reviewed studies available
  • Oral administration available

Caution

  • Short half-life may require frequent dosing

Frequently Asked Questions

References (11)

  1. [1]
    Hughes et al *Nature* Nature (1975)
  2. [9]
    Dripps et al -- Delta opioid receptor agonists as novel analgesics with improved safety profiles Trends Pharmacol Sci (2023)
  3. [10]
    Gendron et al -- Delta opioid receptor-mediated analgesia: from molecular mechanisms to clinical translation Pain (2022)
  4. [11]
    Cahill et al -- Enkephalin regulation of pain and affect: implications for therapeutic development Neuropsychopharmacology (2022)
  5. [2]
    Konig et al *Proc Natl Acad Sci USA* Proc Natl Acad Sci USA (1996)
  6. [3]
    Stein et al *Pharmacol Rev* Pharmacol Rev (2003)
  7. [4]
    Filliol et al *Nat Genet* Nat Genet (2000)
  8. [5]
    Plotnikoff et al *Ann NY Acad Sci* Ann NY Acad Sci (1986)
  9. [6]
    Roques et al *Pharmacol Ther* Pharmacol Ther (2012)
  10. [7]
    Ossipov et al *Life Sci* Life Sci (2004)
  11. [8]
    Schultz et al *Am J Physiol* Am J Physiol (1997)
Updated 2026-03-08Reviewed by Tides Research Team8 citationsSources: peptide-wiki-mdx, pubchem, peptide-wiki-mdx-v2

Larazotide (AT-1001)

Larazotide acetate (AT-1001) is a synthetic tight junction regulatory peptide derived from Vibrio cholerae zonula occludens toxin that modulates intestinal permeability by antagonizing the zonulin pathway, primarily investigated for celiac disease and intestinal barrier dysfunction.

LIV Tripeptide (Leu-Ile-Val)

LIV tripeptide (Leu-Ile-Val) is a branched-chain amino acid-derived bioactive peptide that activates muscle satellite cells and stimulates mTOR-mediated protein synthesis, investigated for muscle recovery, exercise-induced muscle damage repair, and sarcopenia prevention.

On this page

Overview
Reconstitution Calculator
Mechanism of Action
Research
Pain Modulation
Mood and Reward
Immune Function
Cardioprotection
Safety Profile
Pharmacokinetic Profile
Quick Start
Molecular Structure
Research Protocols
Interactions
What to Expect
Quality Indicators
FAQ
References
Related Peptides