Levonorgestrel
Levonorgestrel
Generic Name
Levonorgestrel
Mechanism
Levonorgestrel is a synthetic progestin that functions through multiple pathways:
• Prevents follicular maturation by down‑regulating LH and FSH release.
• Induces endometrial decidualization and thickening, rendering the endometrium less receptive to implantation.
• Slows cervical mucus secretion, forming a barrier to sperm penetration.
• In emergency contraception, a high single dose suppresses or delays ovulation and may impede implantation if ovulation has already occurred.
Pharmacokinetics
- Absorption: Rapid oral uptake; peak plasma concentration (Cmax) at ~2–3 h post‑dose.
- Bioavailability: ~60 %, largely unchanged by food.
- Distribution: High protein binding (~90 % to albumin/bound globulins).
- Metabolism: Hepatic via CYP3A4 → multiple metabolites, some active.
- Half‑life: ~24 h (oral), ~33–35 h (IUD‑releasing system).
- Excretion: Primarily biliary (fecal) with minimal renal elimination.
- Drug interactions: Inducers (rifampin, carbamazepine) lower systemic levels; inhibitors (ketoconazole, itraconazole) may increase exposure.
Indications
- Combined oral contraceptives (≤30 μg estrogen + 0.15 mg levonorgestrel).
- Single‑dose emergency contraception (0.75 mg × 1 within 24 h; 1.5 mg × 1 within 120 h).
- Levonorgestrel‑releasing intrauterine system (LNG‑IUD) in >99 % effective, 6‑year progestin‑only contraception.
- Treatment of endometriosis‑related pain in low‑dose formulations.
- Amenorrhea or dysfunctional uterine bleeding (low‑dose progestin therapy).
Contraindications
- Known or suspected pregnancy – contraindicated.
- History of thromboembolic disease (deep vein thrombosis, pulmonary embolism, stroke) or significant thrombophilia.
- Unexplained abnormal uterine bleeding or pregnancy.
- Breast, uterine, ovarian, cervical, or liver cancer (hormone‑sensitive tumors).
- Severe hepatic disease (Child‑Pugh C).
- Uncontrolled hypertension, migraine with aura, or smoking >35 pack‑years in women >35 yr – increased cardiovascular risk.
> Warning: Monitor for signs of VTE; advise patients to seek immediate care if leg swelling, shortness of breath, or chest pain occurs.
Dosing
| Formulation | Dose | Schedule | Notes |
| Combined oral contraceptive | 0.3 µg ethinyl estradiol + 0.15 mg levonorgestrel | 21 days on, 7 days off (or 24/4‑day regimen) | Take at same time daily; rescue contraceptive not needed. |
| Emergency contraception (tablets) | 0.75 mg levonorgestrel (single dose) | Within 24 h of unprotected sex | For ≤2 days of menstrual cycle. |
| 1.5 mg levonorgestrel (single dose) | Within 120 h of unprotected sex | Most effective within 24 h; dosing error may reduce efficacy. | |
| LNG‑IUD | 52 µg/day release | Insertion → lifelong (up to 6 yrs) | Insert after cervical exam; removal within <24 h if side effects. |
| Low‑dose progestin | 200–300 µg/day | Oral | For endometriosis or irregular bleeding. |
Administration tips:
• Swallow tablets whole with water; no need to chew.
• Avoid concurrent use of potent CYP3A4 inducers unless a backup contraceptive method is arranged.
Adverse Effects
- Common (≤10 %):
- Menstrual irregularities (spotting, breakthrough bleeding)
- Nausea/vomiting, headache, dizziness
- Breast tenderness, weight gain, mood change
- Acne/skin changes (rare, high‑dose).
- Serious (≤0.1 %):
- Venous thromboembolism (VTE)
- Myocardial infarction / stroke (especially in >35 yr smoking women)
- Hepatic adenoma or carcinoma (rare)
- Severe allergic reactions (anaphylaxis).
Monitoring
| Parameter | Frequency | Rationale |
| Body weight, BMI | Every 3–6 mo | Significant weight gain correlates with side‑effects. |
| Blood pressure | Every visit | Hypertension ↑ VTE risk. |
| Vascular risk assessment | At initiation, then annually | Screen for diabetes, smoking, family history. |
| Pregnancy test | After missed menstrual cycle or if contraception failure is suspected | Avoid misuse. |
| Menstrual pattern | At first visit and 1‑month post‑initiation | Detect breakthrough bleeding early. |
| Liver function tests | Baseline and if symptoms arise | Hepatotoxicity possible with high‑dose or hepatic disease. |
Clinical Pearls
- Quick‑Start LRC: Initiating a levonorgestrel‑releasing IUD within 5 days post‑insertion requires no additional backup contraception; the device itself provides >99 % efficacy.
- Emergency Contraception Window: The 0.75 mg dose is most effective when given ≤12 h after intercourse; delayed dosing shifts efficacy dramatically (≈20 % decline per hour).
- Smoking and Age: In women >35 yr who smoke >10 cig/day, the cardiovascular risk exceeds the benefits of combination therapy; a progestin‑only approach is advised.
- Metabolic Caution: Levonorgestrel can mask symptoms of diabetes (e.g., polyuria, polydipsia); check glucose if risk factors present.
- Post‑Surgical Contraception: In patients undergoing uterine surgery (e.g., myomectomy), the LNG‑IUD should be inserted within 5–10 days to provide rapid, effective contraception and reduce uterine bleeding.
- Drug‑Drug Interaction Alerts: If a patient is prescribed rifampin or carbamazepine, the systemic levonorgestrel level falls <50 %, necessitating a backup method or a higher‑dose progestin form (e.g., LNG‑IUD).
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• Levonorgestrel remains one of the most widely used progestins, offering versatile options—from short‑term emergency contraception to long‑term intrauterine delivery—while maintaining a favorable safety profile when patient risk factors are appropriately considered.