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SLU-PP-332 500 Mcg / Capsule 100 Ct

Premium Oral SLU-PP-332 ERR Agonist Peptides

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Product Specification SLU-PP-332 500mcg / 100 Capsules per Bottle (100ct)
Biochemical Engine Estrogen-Related Receptor (ERR) Alpha/Beta/Gamma Agonist
Primary Assay Target Investigated for metabolic rate enhancement, mitochondrial biogenesis, and exercise-mimetic pathways
Logistics Profile Temperature-insulated, secure vacuum 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

SLU-PP-332 500mcg Core Metrics

Technical specification parameters optimized for integrating high-purity SLU-PP-332 capsules into focused cellular endurance rows.

Research ParameterAssay Benchmark ProfileInternal Catalog Link
Molecular EngineERR Pan-Agonist (Exercise Mimetic Model)High-Purity Series →
Purity Baseline≤ 98.0% via High-Resolution SEC-HPLCMetabolic Series →

What is SLU-PP-332 & How Does it Work?

SLU-PP-332 is a highly specialized synthetic small molecule designed to act as a potent nuclear receptor pan-agonist targeting Estrogen-Related Receptors (ERR alpha, beta, and gamma). In contemporary metabolic literature, this non-peptide compound is heavily studied as an exercise mimetic. It triggers key genetic pathways typically turned on during intense endurance exercise without requiring physical activity. By avoiding the typical degradation challenges seen with sensitive peptide sequences, its oral capsule format provides researchers with a highly stable tool to observe sustained energy expenditure and mitochondrial changes inside laboratory research models.

SLU-PP-332 500mcg Quick Specifications

Technical PropertyLaboratory Standard Specifications
Chemical StructureERR alpha/beta/gamma Pan-Agonist Small Molecule
Active Core Payload500mcg per Capsule (100 Active Capsules / Bottle)
Purity Threshold≥ 98.0% Pure Certified via HPLC Assays
Primary Research NodeMitochondrial biogenesis, skeletal muscle remodeling, and fatty acid oxidation curves

How Does SLU-PP-332 Work in Laboratory Assays?

SLU-PP-332 functions by directly crossing cell membranes to activate the ERR alpha/beta/gamma transcriptional network core. This binding action turns on genes responsible for building fresh mitochondria and scaling up cell respiration speed. Unlike traditional metabolic agents that force raw central nervous stress, SLU-PP-332 alters fuel preference inside cell matrices toward active fatty acid oxidation. This allows investigators to observe continuous non-shivering heat generation and lipid breakdown natively, completely free from unguided cellular proliferation data noise.

In analytical metabolic endocrinology and muscular transcriptomic profiling publications, SLU-PP-332 is evaluated extensively for its ability to increase oxidative muscle fiber percentages in test models. Investigators utilize this 500mcg capsule format to track glucose clearance rates and monitor total body fat tissue deceleration under controlled diets. The 100ct presentation provides an ideal, pre-calculated material footprint required for extended concentration screening curves without running into early lot-to-lot baseline titration errors.

SLU-PP-332 Core Pathways & Action Matrix

The table below consolidates the primary cellular pathways, biological markers, and research objectives tracked during SLU-PP-332 laboratory testing lines:

Target PathwayObserved Cellular ActionPrimary Research Goal
Mitochondrial ExpansionUpregulates key genes to increase active mitochondrial density inside muscle tissue matrices.Quantifying cell respiration and ATP generation speed.
Fatty Acid OxidationForces cells to prioritize burning stored lipid parameters for cellular fuel requirements.Studying fat accumulation deceleration and lean tissue markers.
Fiber Architecture ShiftPromotes structural remodeling toward oxidative (fatigue-resistant) fiber types.Mapping endurance mimetic data curves natively.

Step-by-Step Mechanism of Action

When SLU-PP-332 is introduced to the target sample research media, it coordinates deep energy adaptations through a highly standardized sequence path:

  1. Nuclear Penetration: The small molecule structure smoothly crosses internal lipid boundaries to reach the cell’s nuclear core directly.
  2. ERR Pan-Agonism: Docks selectively across active ERR alpha, beta, and gamma receptor backbones simultaneously.
  3. Co-Activator Recruitment: Prompts immediate structural changes that recruit key gene controllers, turning on mitochondrial biogenesis networks.
  4. Metabolic Shift: The cell lines demonstrate an intense spike in baseline oxygen consumption, accelerating active fat breakdown while keeping muscle tissue preservation stable.

To assist in protocol coordination, it is essential to differentiate the muscle-focused energy expenditure and exercise mimetic focus of SLU-PP-332 500mcg from alternative metabolic tracks available in our collection. While alternative compounds target appetite signaling networks or adipose cell tissue pathways explicitly, SLU-PP-332 focuses entirely on turning on mitochondrial transcription. Understanding these core catalog differences allows for more precise laboratory assay designs.

Peptide Quick Comparison Matrix

The comparative table below outlines the core differences in research focus, mechanism of action, and primary target nodes across our active high-purity laboratory collection:

Research PeptideMechanism of ActionPrimary Laboratory FocusTarget NodesPeptide Structure
SLU-PP-332 500mcg(This Product)ERR alpha/beta/gamma AgonismExercise mimetic pathways, mitochondrial биогенез, and muscle lipid breakdown.ERR Core NetworkSmall Molecule
MOTS-c 10mgMito-Signaling LoopMitochondrial energy output tracking, non-insulin glucose clearings, and exercise mimetic assays.AMPK PathwaysLinear 16-AA Peptide
AOD 9604 5mgSelective Adrenergic ActivityAccelerating lipid breakdown, triglyceride clearing, and non-glycemic metabolic models.Adipocyte Matrix16-AA C-Term Fragment

Synergistic Research Application Notice

In broad metabolic research projects, investigators frequently study ERR pan-agonists alongside mitochondrial-derived peptides like MOTS-c to observe cellular stamina adaptations. The 500mcg oral configuration provides the exact material control required to establish baseline low-dose parameters without liquid reconstitution errors. While our standard peptide series look into rapid AMPK pathways or selective lipolysis, standalone SLU-PP-332 offers a pristine reference loop for deep nuclear-directed cell energy research.

How to Store SLU-PP-332 Oral Capsules

To keep your high-purity SLU-PP-332 capsules fully stable and prevent the small molecule layout from losing transcriptional strength over time, you must follow strict environment rules. This stable chemical structure resists standard solution breakdown paths but remains sensitive to high heat, moisture infiltration, and direct sunlight exposure loops.

  • COOL & DRY (15°C – 25°C) Long-Term Bottle Storage: Store the original tightly sealed capsule bottle inside a cool, dark laboratory cabinet between 15°C and 25°C. Keeping the environment dry fully protects shell integrity for up to 24 months.
  • HUMIDITY CONTROLS Desiccant Integrity: Keep the moisture-absorbing pack inside the bottle at all times. Ambient humidity changes can degrade the active shell structure, creating data distortion parameters during cell testing lines.
  • ZERO RECONSTITUTION Ready-to-Test Configuration: SLU-PP-332 500mcg is pre-calibrated inside dry oral capsules (100ct). Do not attempt to dissolve the capsules or mix the internal powder with bacteriostatic water. Introduce it intact to maintain precise research benchmarks.

Why Buy PeptidesK SLU-PP-332 500mcg Online?

At PeptidesK, we understand that modern metabolic screening and muscle transcription profiling demand absolute chemical fidelity. Our strict production and processing benchmarks isolate your laboratory rows from background artifact contamination noise, ensuring consistent and reproducible data records:
  • ✓ Verified ≥98% Matrix Purity: Every individual production batch is monitored through High-Performance Liquid Chromatography (HPLC) and Mass Spectrometry to guarantee perfect pan-agonist small molecule structures free from synthesis artifacts.
  • ✓ Premium Capsule Shielding: Enclosed inside high-resistance laboratory bottles with protective safety seals, completely shielding the molecule core from external moisture and thermal stress.
  • ✓ Complete Lot Traceability: Full production batch documentation metrics and definitive Certificates of Analysis (CoA) are systematically logged, archived, and accessible for institutional validation and research auditing.

Frequently Asked Questions (FAQ)

What is the primary technical reason for utilizing the 500mcg capsule format in laboratory research?

Nuclear receptor pan-agonists require exact dosage control to prevent receptor fatigue data anomalies. The 500mcg capsule format (100ct) provides an ideal, pre-measured material footprint tailored explicitly for targeted concentration runs, low-yield baseline control setups, or pilot titration curves without the volume calculation errors linked to manual liquid compounding.

Does SLU-PP-332 cause heart rate spikes or central nervous nervous system stimulation inside assays?

No. Unlike traditional stimulant-based thermogenics that force systemic adrenaline loops, SLU-PP-332 activates metabolic transcription entirely via localized nuclear ERR signaling channels. Muscle fiber remodeling and fat breakdown occur natively without altering nervous system baselines.

Is PeptidesK SLU-PP-332 500mcg approved for human endurance enhancement, fat loss or bodybuilding pills?

No. This compound is processed, synthesized, and distributed strictly for academic laboratory research, in vitro cellular tracking assays, and physical diagnostic validations. It is completely unapproved and unsafe for human therapeutic injection, oral athletic enhancement, or consumer lifestyle use. It should never be used as a lifestyle drug under any circumstances.

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