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SLU-PP-332 5 Mg

Advanced 5mg Pan-ERR Receptor Agonist

$33.00

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Product Specification SLU-PP-332 5mg / Lyophilized Powder Vial
Biochemical Engine Selective Estrogen-Related Receptor (ERRα, ERRβ, ERRγ) Pan-Agonist Small Molecule
Primary Assay Target Investigated for exercise-mimetic pathways, skeletal muscle oxidative capacity enhancement, and mitochondrial biogenesis acceleration
Logistics Profile Temperature-insulated, light-shielded moisture-resistant dispatch with complete tracking

STRICTLY FOR LABORATORY RESEARCH: This synthetic agent is processed strictly for institutional R&D, high-precision in vitro metabolic calibrations, and testing lines. Not for human therapeutic or diagnostic use.

Description

Quick-Reference Overview Matrix

For efficient laboratory evaluation, the matrix below consolidates the core analytical, storage, and cross-reference parameters of SLU-PP-332 5mg.

Core ParameterTechnical Summary & Quick DataInternal Cross-Reference
Purity & Grade≥ 98% HPLC Certified
Sterile filtered, vacuum-sealed lyophilized formulation optimized for metabolic tracking assays.
View High-Purity Series →
Primary Target PathERR Pan-Agonism: Activates Estrogen-Related Receptors to stimulate oxidative muscle fiber transitions and enhanced fatty acid lipolysis.Metabolic Research Series →
Storage ProtocolLyophilized: -20°C to -80°C (Up to 24 months).
Reconstituted: 2°C to 8°C (Must use within 10–14 days).
Buy Reconstitution Diluents →
Synergistic AssaysFrequently co-evaluated with other bioenergetic or fat-loss modulators like SR-9009 or Cardarine alternatives for metabolic research models.Explore Tissue Repair Series →

What Is SLU-PP-332?

SLU-PP-332 is a highly innovative, non-steroidal synthetic compound that acts as a potent pan-agonist for the Estrogen-Related Receptors (ERRs), specifically targeting the ERRα, ERRβ and ERRγ nuclear receptor isoforms. In structural biological models, it acts as a robust exercise mimetic by directly inducing genetic transcriptions usually triggered by intensive endurance training. It is heavily utilized in contemporary laboratory setups to explore treatments for metabolic syndrome, muscle atrophy models, and advanced lipid oxidative pathways.

SLU-PP-332 5mg Overview

Our SLU-PP-332 5mg formulation is manufactured to elite analytical research standards, ensuring complete structural definition and zero baseline contamination during cellular screenings. Each vial is freeze-dried (lyophilized) and vacuum-sealed, keeping the active compound fully isolated from kinetic and environmental stress variables.

Parameter Specification
Product Format 5mg Vial (Lyophilized Powder)
Chemical Name N-(5-(trifluoromethyl)pyridin-2-yl)-2-(3-(trifluoromethyl)phenyl)acetamide derivative
Molecular Formula C16H11F6N3O2 (Core complex variant)
Molecular Weight 407.3 g/mol
Purity Level ≥ 98% (HPLC Monitored)
Physical Appearance Sterile filtered, off-white to white lyophilized solid
Core Research Focus ERRα/β/γ Transcription, Mitochondrial Volume Density, Skeletal Muscle Oxidative Capacity

Regulatory Compliance Notice: This product is synthesized, distributed, and intended solely for laboratory research and development purposes. It is strictly not for human therapeutic use, clinical trials, or agricultural applications. Analytical verification sheets (HPLC/MS) arelogged systematically per batch.

In analytical endocrinology and metabolic disease publications, SLU-PP-332 is evaluated extensively across performance-simulation and energetic expenditure assays. Researchers utilize this compound to analyze:

  • Skeletal Muscle Remodeling: Studying how active pan-agonism promotes a structural shift from glycolytic (Type II) toward oxidative (Type I) muscle fiber profiles in vivo.
  • Mitokondriyal Volume Regulation: Investigating the upregulation of genes connected to mitochondrial replication, augmenting overall cellular respiratory velocity.
  • Obesity Resistance Models: Tracking metabolic rate changes and fat mass accumulation ratios during targeted lipid saturation diets in laboratory animal subjects.

SLU-PP-332 Mechanism of Action

SLU-PP-332 functions by serving as a high-affinity ligand that binds simultaneously to **ERRα, ERRβ, and ERRγ** orphan nuclear receptors, mimicking the downstream genetic signals typically triggered by PGC-1α activation during exercise:

  1. Upon receptor docking, it activates the transcription of specific gene arrays controlling fatty acid oxidation (such as Cpt1b) and mitochondrial structural enhancement.
  2. Upregulates the expression of **Skeletal Muscle Pyruvate Dehydrogenase Kinase 4 (Pdk4)**, driving cellular networks to prioritize lipid burning over carbohydrate consumption.
  3. This metabolic modification leads to high physical fatigue resistance and lowered systemic lipid levels within evaluated cellular and physiological lineages.

Research Overview: Benefits vs. Technical Risks

Observed Research Benefits Technical Risks & Limitations
• Complete ERR Coverage: Simulates global exercise adaptations more effectively than single-isoform agonists by hitting all three ERR pathways (α, β, γ). • Substrate Solubility Limits: Being non-steroidal, raw molecular reconstitution requires precise lab diluents to prevent sudden precipitation out of liquid phases.
• High Genetic Potency: Triggers measurable changes in metabolic biomarkers at lower micro-concentrations inside muscle tissue assays. • Cellular Adaptability Noise: Prolonged receptor saturation in long assays can cause secondary gene adaptations that alter original baseline controls.

To assist in experimental optimization, the table below differentiates SLU-PP-332 5mg from other metabolic regulatory and energetic pathway research compounds available in our catalog:

Peptide CompoundPrimary MechanismCore Research FocusTarget ReceptorsMolecular Weight
SLU-PP-332 5mg(This Product)ERR Pan-AgonismExercise simulation, mitochondrial replication, lipid breakdown upregulation.ERRα / β / γ407.3 g/mol
MOTS-c 10mgMito-SignalingInsulin response mapping, baseline glucose tracking assays.AMPK Pathways2174.6 g/mol
Tesamorelin 10mgGHRH AnalogueVisceral adipose tissue breakdown, endogenous growth hormone tracking.GHRH Receptor5135.9 g/mol

To avoid crystal lattice structural faults and keep the pan-agonist compound safe from early degradation pathways, apply the following climate protocols:

  • LONG-TERM Lyophilized State: Store inside calibrated laboratory freezing units at -20°C or -80°C. Stable for up to 24 months.
  • SHORT-TERM Logistics Cushion: The dry formulation is resilient during active transport up to 25°C for 3 weeks max. Deep-freeze post-delivery.
  • POST-RECONSTITUTION Solubilized State: Store strictly in refrigeration between 2°C and 8°C. Exhaust the testing solution within 10–14 days. Do not re-freeze mixed liquid.

Reconstitution Guidelines

  1. Allow the SLU-PP-332 vial to naturally settle to room temperature equilibrium before removing its seal.
  2. Wipe the core rubber injection stopper thoroughly with an isopropyl sterile swab.
  3. Slowly introduce your lab diluent (such as sterile bacteriostatic water or target assay buffering liquids) against the interior glass structure.
  4. Do not shake. Gently swirl the vial horizontally in small concentric pathways until the 5mg cake dissolves completely into a clear, residue-free fluid layer.

Why Choose PeptidesK?

At PeptidesK, we identify that cutting-edge metabolic disease research depends heavily on elite chemical fidelity. Our strict synthesis standards prevent baseline distortion in your genetic assays:
  • ✓ Premium Purity Certified (≥98%): Subjected to meticulous HPLC and Mass Spectrometry tracking to eliminate impurities that could alter nuclear receptor readings.
  • ✓ Vacuum-Sealed Solid Desiccation: Lyophilized under advanced clinical vacuum levels to eliminate atmospheric water moisture interaction paths during long-term storage.
  • ✓ Direct Traceability Logistics: Complete batch documentation and Certificates of Analysis (CoA) are fully cataloged and available upon validation request.

Frequently Asked Questions

Why is SLU-PP-332 referred to as an "exercise mimetic" in recent literature?

It earns this designation because its pan-agonism on ERR targets directly upregulates Pdk4 and lipid-burning gene scripts. This triggers the identical physiological and mitochondrial adaptions in muscle tissue assays that normally require extensive mechanical aerobic training paths.

Is SLU-PP-332 5mg cleared for human evaluation or metabolic clinical therapy?

No. This compound is processed, synthesized, and listed strictly for laboratory research, academic biochemistry, and in vitro diagnostic assays. It is completely unapproved and unsafe for direct human therapeutic injection or oral consumption.

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