SLU-PP-332 vs Tamoxifen

Emerging vs FDA Approved

avoid Mechanism-based · 53% Both SLU-PP-332 and Tamoxifen 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

SLU-PP-332 Tamoxifen

Weight 290.32 Da 371.51 Da

Half-life Under investigation (no human PK data) ~5-7 days

Chain Non-peptide small molecule —

Type Synthetic ERR agonist Triphenylethylene-derived selective estrogen receptor modulator

Key Benefits

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

Tamoxifen

01 Blocks estrogen receptor signaling in breast tissue, preventing and treating gynecomastia

02 Stimulates LH and FSH production by antagonizing hypothalamic estrogen receptors

03 Restores endogenous testosterone production during post-cycle therapy

04 Partial estrogen agonist activity in bone preserves bone mineral density

05 Extremely long half-life allows for flexible dosing schedules

06 Decades of clinical use with a well-characterized safety and efficacy profile

07 Oral administration with no injections or reconstitution required

Dosing Protocols

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

Tamoxifen

20-40mg oral daily / Once daily

Side Effects

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

Tamoxifen

Hot flashes and night sweats

Nausea or gastrointestinal discomfort

Mood swings, irritability, or emotional lability

Fatigue during initial weeks of use

Headache

Contraindications

NOT FOR HUMAN USE - no approved human dose

No human clinical trials conducted

Potential interaction with diabetes medications

History of deep vein thrombosis, pulmonary embolism, or other thromboembolic events

Known hypersensitivity to tamoxifen citrate or any excipients

Concurrent warfarin or coumarin-type anticoagulant therapy (increased bleeding risk)

Pregnancy or planned pregnancy (category D -- known teratogenic risk)

Pre-existing endometrial hyperplasia or uterine cancer

Severe hepatic impairment

Research Evidence

SLU-PP-332 Tamoxifen

Status Emerging FDA Approved

References 4 studies 5 studies

Latest 2025 —

FDA Approved No Yes

Full SLU-PP-332 profile Full Tamoxifen profile SLU-PP-332 calculator Tamoxifen calculator

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