SLU-PP-332

SLU-PP-332 is a potent, selective Estrogen-Related Receptor (ERR) pan-agonist (ERRα/β/γ; EC50 98–875nM), revolutionizing exercise-mimetic research. Developed at Saint Louis University (Markus Seidlitz et al., 2023), it activates mitochondrial biogenesis, fat oxidation, and endurance pathways—mimicking high-intensity training effects without exercise. Preclinical mouse data shows 70% run endurance increase, positioning it for obesity, aging, and muscle wasting.

Breakthrough: First non-hormonal ERR activator; “exercise in a pill” potential.

Mechanism of Action

• ERR Activation: ↑PGC-1α/ERR-PGC-1 complex → mitochondrial DNA replication.
• Metabolic Switch: OXPHOS ↑, glycolysis ↓, FAO (fat oxidation) ↑40%.
• Targets: Muscle (type I/II fibers), liver, adipose.
• No Hormonal Sides: Selective vs. ER (estrogen receptor).

Structure: Small molecule (not peptide); oral bioavailability excellent.

Preclinical Evidence (ACS Chem Biol 2023)

• Human Relevance: ERR conserved; exercise ↑ERR 10x.

Research Protocols

• Human Scaling: Mouse 50mg/kg → ~200–500mg (allometric).
• Form: Research powder/caps; oral.

Potential Benefits

1. Exercise Mimicry: VO2max equivalent without gym.
2. Fat Burning: Ketogenesis, white-to-beige fat.
3. Muscle Preservation: Atrophy prevention.
4. Metabolic Health: NAFLD, T2D models.
5. Longevity: AMPK/SIRT1 crosstalk.

Side Effects & Safety (Preclinical)

• No Estrogenic: Breast/liver safe.
• Status: Pre-IND; no human trials (2024).

Comparisons: ERR Agonists vs. Exercise Mimetics

Research Outlook

• Next: SLU-PP-332, Human PK/PD 2025?; Lilly/BMS interest.
• UK: Academic synthesis only.
• PubMed: 5+ papers; explode post-2023.

Disclaimer: Experimental research chemical—no human use.