Anadrol vs SLU-PP-332

FDA Approved vs Emerging

avoid Mechanism-based · 53% Both Anadrol and SLU-PP-332 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently.

Molecular Data

Anadrol SLU-PP-332

Weight 332.48 Da 290.32 Da

Half-life ~8-9 hours Under investigation (no human PK data)

Chain — Non-peptide small molecule

Type 17-alpha alkylated anabolic steroid (C21H32O3) Synthetic ERR agonist

Key Benefits

Anadrol

01 Rapid and dramatic increases in muscle mass and bodyweight

02 Exceptional strength gains, often noticeable within the first week

03 Potent stimulation of erythropoietin and red blood cell production

04 Increased appetite and nutrient partitioning in some users

05 Improved recovery between training sessions

06 Full, round muscle appearance due to intramuscular water and glycogen retention

07 FDA-approved treatment for various forms of anemia

SLU-PP-332

01 Exercise mimetic effects without physical activity

02 12% weight loss in 28 days

03 70% increased endurance

04 25% enhanced fatty acid oxidation

05 Improved insulin sensitivity

06 Reduced hepatic steatosis

07 Cardiac protection

08 Reversal of age-related mitochondrial dysfunction

Dosing Protocols

Anadrol

25-50 mg/day / Once or twice daily (oral)

SLU-PP-332

NO HUMAN DOSE ESTABLISHED (animal studies: 50 mg/kg IP) / Research only - not approved for human use

Standard Metabolic Protocol 50 mg/kg (animal dosing) Twice daily

Acute Exercise Enhancement 50 mg/kg (animal dosing) Single dose 1 hour pre-exercise

Extended Treatment 50 mg/kg (animal dosing) Twice daily for 4-8 weeks

Side Effects

Anadrol

Significant water retention and bloating (estrogenic, not aromatase-mediated)

Elevated blood pressure (fluid volume and RBC increase)

Severe liver stress and elevated liver enzymes (AST/ALT)

Back pumps and lower back pain during exercise

Headaches (often blood pressure-related)

Appetite suppression (paradoxical for a mass-building compound)

Lethargy and fatigue (hepatic strain-related)

Acne and oily skin

Suppression of natural testosterone production

SLU-PP-332

Animal studies show favorable safety with no severe effects at therapeutic doses

Well-tolerated in rodents and canines

No liver, kidney, or cardiac toxicity documented

No lean mass loss

Does not suppress hormones or act as stimulant

Minor plasma cholesterol and liver enzyme changes in some studies

Contraindications

Pre-existing liver disease or significantly elevated liver enzymes

Prostate cancer or breast cancer in males

Nephrotic phase of nephritis

Hypercalcemia (Anadrol can exacerbate calcium levels)

Pregnancy (Category X - causes virilization of the female fetus)

Known hypersensitivity to oxymetholone

Concurrent use of other 17-alpha alkylated oral steroids (compounded liver toxicity)

NOT FOR HUMAN USE - no approved human dose

No human clinical trials conducted

Potential interaction with diabetes medications

Research Evidence

Anadrol SLU-PP-332

Status FDA Approved Emerging

References 5 studies 4 studies

Latest 2018 2025

FDA Approved Yes No

Full Anadrol profile Full SLU-PP-332 profile Anadrol calculator SLU-PP-332 calculator

More comparisons: Testosterone Raloxifene 5-Amino-1MQ NAD+Ipamorelin

This comparison is for educational and research purposes only. Consult a healthcare professional before use.