Elagolix
Elagolix
Generic Name
Elagolix
Mechanism
Elagolix is a non‑peptide, oral GnRH (gonadotropin‑releasing hormone) antagonist.
• Competitive inhibition at the GnRH receptor on the pituitary gland blocks the release of LH (luteinizing hormone) and FSH (follicle‑stimulating hormone).
• Resulting hypoestrogenicity reduces endometrial stimulation and uterine fibroid growth.
• The effect is rapid, reversible, and does not rely on receptor desensitization (unlike GnRH agonists).
Pharmacokinetics
- Absorption: Rapid oral absorption; peak plasma concentration (*Cmax*) reached in 0.5–2 h.
- Bioavailability: ~53 % (dose‑dependent, reduced when taken with food).
- Distribution: High plasma protein binding (~99 %).
- Metabolism: Predominantly hepatic, mainly via CYP3A4 and to a lesser extent CYP2D6.
- Elimination: Renal and biliary routes; elimination half‑life ≈4–5 h.
- Drug interactions: Potentiated by strong CYP3A4 inducers (e.g., rifampin); decreased concentrations with strong CYP3A4 inhibitors (e.g., ketoconazole).
Indications
- Endometriosis‑related pelvic pain (moderate to severe) in reproductive‑age women.
- Uterine fibroids (symptomatic uterine bleeding or bulk symptoms) when paired with add‑back therapy.
Contraindications
- Contraindications:
- Known hypersensitivity to elagolix or its excipients.
- Pregnancy or lactation.
- Severe hepatic impairment (Child‑Pugh B/C).
- Warnings:
- Hypoestrogenic side effects: bone mineral density loss, vasomotor symptoms, hot flashes.
- Consideration in estrogen‑dependent tumors (breast, endometrial).
- Potential cardiovascular effects (elevated triglycerides, LDL, blood pressure in some patients).
Dosing
| Indication | Dose | Frequency | Required Add‑Back |
| Endometriosis | 200 mg or 150 mg | BID or daily | 5 mg estradiol 10 mg norethindrone acetate (or 2.5 mg ethinyl‑estradiol 2.5 mg dienogest) |
| Uterine fibroids | 200 mg | BID | Same add‑back options as above |
• Take with food to enhance absorption (especially for the 200 mg dose).
• Steady‑state achieved ~14 days.
• Discontinuation: Rapid return of endogenous gonadotropin‑estradiol axis activity; monitor for flare of symptoms.
Adverse Effects
- Common (≥10 %):
- Hot flashes, flushing
- Nausea, vomiting
- Headache, dizziness
- Violation of upper‑limb (liver enzymes↑)
- Fatigue
- Serious (≤1 %):
- Hypersensitivity reactions (rash, angioedema)
- Osteoporosis‑related fractures (with prolonged use without add‑back)
- Severe hepatic injury (rare)
- CV events (elevated lipids, hypertension)
Monitoring
- Bone health: Dual‑energy X‑ray absorptiometry (DEXA) at baseline, 12 mo, then annually if >3 years.
- Liver function tests: ALT/AST at baseline, 1 mo, then 3 mo.
- Lipid panel: Baseline, 3 mo, then annually.
- Pregnancy test: Prior to initiation, then regularly during therapy.
- Contraception counseling (due to risk of fetal harm).
Clinical Pearls
- Add‑back therapy is key: Avoid cumulative bone loss and hot flashes; choose formulation based on patient preference and safety profile.
- Short‑term use for acute flare (≤2 weeks) may relieve severe pain without long‑term risks.
- Use caution in patients with pre‑existing osteopenia – consider baseline DEXA and early add‑back.
- Non‑pregnant female patients: Discuss fertility implications; elagolix does not affect ovarian reserve beyond the hypoestrogenic window.
- Drug‑drug interaction pearls: Check for CYP3A4 inducers (e.g., phenytoin, carbamazepine) that can lower elagolix levels; similarly, potent inhibitors can raise systemic exposure and side‑effect risk.
--
• References
Key clinical trials: REPOSE 1 & 2 (endometriosis), AMBITION (fibroids).
FDA prescribing information (2023).
Clinical pharmacology reviews in *Obstetrics & Gynecology* and *Pharmacologic Reports*.