Anastrozole and LGD-4033 Interaction

Avoid

Mechanism-based 64% confidence

Anastrozole and LGD-4033 have a potentially harmful interaction with 64% confidence. Both Anastrozole and LGD-4033 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently. Both compounds affect the gonads and liver and heart, so monitoring these systems is recommended.

Compound Profiles

Anastrozole

Aromatase Inhibitor | Estrogen Management

Anastrozole competitively binds to the heme group of the aromatase enzyme (cytochrome P450 19A1), reversibly inhibiting its catalytic activity. Aromatase is responsible for the final step in estrogen biosynthesis, converting testosterone to estradiol and androstenedione to estrone in peripheral tissues including adipose, muscle, liver, and brain.

Half-life: ~40-50 hours Typical dose: 0.25-0.5mg EOD or E3D (estrogen management) pct, anabolic

aromatase androgenicaromatase inhibitorestrogenichepatotoxic

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LGD-4033

Selective Androgen Receptor Modulator | Lean Mass

LGD-4033 binds to the androgen receptor with high affinity (Ki of approximately 1 nM), functioning as a potent and selective agonist in muscle and bone tissue. Like other SARMs, its tissue selectivity is mediated by differential cofactor recruitment: upon binding to the AR, LGD-4033 induces a receptor conformation that preferentially recruits coactivators expressed in skeletal muscle and bone, while showing minimal agonist activity in androgen-sensitive tissues such as the prostate and skin.

Half-life: ~24-36 hours Typical dose: 5-10 mg/day sarm, anabolic

androgen receptorepo receptor androgenicblood pressure raisingcarcinogenic riskestrogenic

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Combined Organ Load

Gonads

elevated

Liver

elevated

Heart

moderate

Pituitary

low

Shared Safety Flags

2x 2 androgenic compounds (Anastrozole, LGD-4033). Additive androgenic load — increased risk of hair loss, acne, prostate effects.

2x 2 estrogenic compounds (Anastrozole, LGD-4033). Combined estrogen elevation — monitor E2 and consider aromatase inhibitor.

2x 2 hepatotoxic compounds (Anastrozole, LGD-4033). Liver damage risk significantly increased. Include liver support (TUDCA/NAC) and monitor ALT/AST.

2x 2 HPTA-suppressive compounds (Anastrozole, LGD-4033). Deep hormonal shutdown expected — plan extended PCT.

2x 2 compounds disrupt lipids (Anastrozole, LGD-4033). Get lipid panel mid-cycle — consider adding lipid support.

2x 2 compounds share the teratogenic safety flag (Anastrozole, LGD-4033). Monitor accordingly.

Frequently Asked Questions

Can I take Anastrozole with LGD-4033?

Combining Anastrozole with LGD-4033 is not recommended. Both Anastrozole and LGD-4033 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently.

Is Anastrozole and LGD-4033 safe together?

This combination carries significant risk. Both Anastrozole and LGD-4033 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently. Consult a healthcare professional before combining.

What are the interactions between Anastrozole and LGD-4033?

Both Anastrozole and LGD-4033 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently. This assessment has 64% confidence and is inferred from pharmacological mechanism analysis.

How should I time Anastrozole and LGD-4033?

Anastrozole has a half-life of ~40-50 hours and LGD-4033 has a half-life of ~24-36 hours. No specific timing requirements identified for this combination, but separating administration can help monitor individual effects.

Check this pair in the full Interaction Checker Full comparison: Anastrozole vs LGD-4033

This interaction analysis is compiled from research literature and pharmacological mechanism data. This assessment is inferred from known mechanisms and may not reflect all real-world outcomes. Always consult a healthcare professional before combining compounds.