Generic Name

Femara

Mechanism

• Target: Cytochrome P450 aromatase (CYP19A1), the enzyme catalyzing the conversion of androgens to estrogens.
• Binding: Reversibly binds to the heme‑iron center as an irreversible inactivator.
• Outcome: Decreases systemic estrogen levels by 85‑95 %, limiting estrogen‑dependent proliferation of breast cancer cells.

Pharmacokinetics

Indications

• Post‑menopausal female breast cancer
• Adjuvant therapy after surgery ± radiation for early‑stage, estrogen‑receptor positive disease.
• Extended adjuvant (up to 10 years) past 5 years of tamoxifen.
• Metastatic breast cancer refractory to tamoxifen/letrozole, or as part of second‑line endocrine therapy.
• Pre‑clinical evidence suggests use in male hormone‑responsive breast cancer; not FDA‑approved.

Contraindications

• Contraindications
• Hypersensitivity to anastrozole or any excipients.
• Known estrogen‑dependent gynecologic malignancies (e.g., uterine sarcoma).
• Warnings
• Osteoporosis/osteopenia: chronic estrogen suppression increases bone turnover.
• Severe hepatic impairment: reduced metabolism, increased plasma levels.
• Pregnancy: may cause fetal estrogen deficiency—use only if maternal benefit > risk.
• Bone‑pain or fractures: consider concurrent bone‑sparing therapy.

Dosing

• Standard regimen:
• 1 mg orally once daily, taken at the same time each day.
• Alternative: 0.5 mg daily may be used when tolerability issues arise.
• Initiation: Take on an empty stomach; food does not significantly alter absorption.
• Duration: Typically 5–10 years for adjuvant therapy; until progression for metastatic disease.
• Compliance: Pill‑box reminder and routine pill counts help maintain adherence.

Adverse Effects

Monitoring

• Baseline:
• Blood chemistry (CBC, CMP).
• Bone mineral density (DEXA).
• Calcium & alkaline phosphatase.
• During therapy:
• DEXA every 12–24 months.
• Bone turnover markers (serum CTX, P1NP) annually.
• Liver function tests every 6 months if hepatic impairment present.
• Adverse events:
• Prompt assessment of hot flashes, arthralgia, fractures.
• Evaluate bone‑sparing therapy if indicated.

Clinical Pearls

1. Bone protection is essential: Concomitant bisphosphonate or denosumab is recommended for patients with a baseline DEXA T‑score ≤ –1.5 or osteopenia.

2. Hot flashes can be dose‑shifted: Switching 1 mg to 0.5 mg daily may reduce severity without compromising efficacy.

3. Adjuvant sequencing matters: Post‑tamoxifen, anastrozole improves overall survival better than extended tamoxifen alone.

4. Drug–interaction vigilance: Co‑prescribing strong CYP3A4 inducers (e.g., rifampin) can reduce Femara exposure and undermine efficacy; consider dose adjustment or alternative endocrine therapy.

5. Gender‑specific caution: Though off‑label for males, Femara can precipitate gynecomastia or osteoporosis; use with caution and monitor bone density.

6. Non‑adherence risk: The lack of overt side‑effects in early months can lead to complacency; use patient education and scheduled clinic visits to reinforce daily intake.

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• Key pharmacology terms: aromatase inhibitor, estrogen suppression, post‑menopausal breast cancer, bone mineral density, DEXA, bisphosphonate.