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Semaglutide vs SLU-PP-332

A side-by-side research comparison of Semaglutide and SLU-PP-332 across mechanism, dosing, half-life, benefits, side effects and research status.

Comparison table

AttributeSemaglutideSLU-PP-332
Full nameSemaglutide (GLP-1 Receptor Agonist)SLU-PP-332 (ERR Agonist)
CategoryWeight ManagementWeight Management
StatusFDA ApprovedResearch compound (preclinical)
MechanismBinds GLP-1 receptors in the pancreas to stimulate insulin secretion, in the brain to reduce appetite, and in the GI tract to slow gastric emptying. 94% homology to native GLP-1.A pan-ERR (estrogen-related receptor alpha/beta/gamma) agonist. ERRs are master regulators of mitochondrial biogenesis and oxidative metabolism, so activation upregulates fat oxidation and the genetic program normally triggered by endurance exercise.
Molecular weight4,114 Da~426 Da (small molecule, not a peptide)
Half-life7 days (168 hours)Not well characterized in humans
BioavailabilityHigh (SubQ ~89%), Moderate (oral ~1% with SNAC)Studied via injection in animals; oral activity under investigation
Typical dose0.25 mg → titrate up to 2.4 mgNo established human dose
FrequencyOnce weeklyUnknown
RouteSubcutaneous injectionInjection (preclinical)

Semaglutide reported benefits

  • Significant weight loss (15-17%)
  • Improved glycemic control
  • Cardiovascular risk reduction
  • Reduced food cravings
  • Lower HbA1c

SLU-PP-332 reported benefits

  • Increases mitochondrial fat-burning (preclinical)
  • Improved endurance in animals
  • Reduced fat gain without appetite change (animals)
  • Acts as an "exercise mimetic"

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Research and educational reference only. Not medical advice.