Denosumab
Denosumab
Generic Name
Denosumab
Mechanism
- Selective inhibition of RANK‑L: Binds with high affinity to RANK‑L, preventing it from interacting with its receptor RANK on osteoclast precursors and mature osteoclasts.
- Suppression of osteoclast formation, function, and survival: Leads to reduced bone resorption and turnover.
- Effect on bone microarchitecture: Increases trabecular number and thickness, thereby improving bone strength.
- No effect on bone formation: Allows balanced remodeling by permitting osteoblast activity.
Pharmacokinetics
- Absorption: Administered subcutaneously; rapid absorption with peak serum levels 1–2 days post‑dose.
- Distribution: Minimal protein binding; distributes primarily into bone and peripheral tissues; limited CNS penetration.
- Metabolism: Catabolized to peptides via proteolytic degradation; no hepatic metabolism.
- Elimination: Linear clearance; half‑life ≈ 26 days (steady‑state). Excretion is primarily through reticuloendothelial system.
- Drug interactions: None significant due to non‑enzymatic metabolism; no CYP involvement.
Indications
- Post‑menopausal osteoporosis: 60 mg SC every 6 months (or 1 mg/kg if body weight >50 kg).
- Pre‑menopausal osteoporosis: 60 mg SC every 6 months.
- Glucocorticoid‑induced osteoporosis: 60 mg SC every 6 months.
- Bone loss secondary to aromatase inhibitors (breast cancer) in women and men.
- Prophylaxis of skeletal‑related events in solid‑tumor metastases to bone, e.g., breast, prostate, lung.
- Treatment of giant cell tumor of bone after surgery.
- Hypercalcemia of malignancy: 20 mg IV or SC on days 0, 7, 14, 28.
- Bone metastases in multiple myeloma (in combination with bisphosphonates).
Contraindications
- Contraindicated in patients with hypersensitivity to denosumab or any excipient.
- Caution in:
- Severe hypocalcemia (correct before initiation).
- Acute osteolysis (e.g., metastatic bone disease).
- Infections (latent TB, active fungal/viral infections).
- Warnings:
- Hypocalcemia: Risk post‑treatment; monitor calcium levels.
- Osteonecrosis of the jaw (ONJ): Rare; increased risk with dental procedures; dental evaluation recommended.
- Atypical femoral fractures (AFF): Long‑term use (> 5 years) may increase risk; consider drug holidays.
- Infection risk: Respiratory tract infections, mucositis.
- Secondary effects: Potential for impaired bone healing and surgical complications.
Dosing
| Indication | Dose | Frequency | Route |
| Osteoporosis (post‑menopausal, pre‑menopausal, glucocorticoid‑induced) | 60 mg | Every 6 months | Subcutaneous |
| Weight‑based osteoporosis | 1 mg/kg (≥ 50 kg) | Every 6 months | Subcutaneous |
| Metastatic bone disease | 120 mg | Every 4 weeks | Subcutaneous |
| Prophylaxis in cancer | 120 mg | Every 4 weeks (first 6 doses) then every 12 weeks | SC |
| Hypercalcemia of malignancy | 20 mg | Daily for 1 week, then weekly for 3 weeks, then monthly | SC or IV |
| Giant cell tumor of bone | 60 mg | Every 6 months | SC |
• Administration tips: Inject into thigh, abdomen, or upper arm; rotate sites; avoid simultaneous intramuscular injections.
• Missed dose: Reconstitute and administer within 8 weeks; if > 8 weeks, restart the dosing interval.
Adverse Effects
Common (≥ 5 % frequency)
• Injection‑site reactions (pain, erythema, induration)
• Diarrhea
• Throat irritation
• Hypocalcemia (mild)
Serious (≥ 1 % frequency)
• Hypocalcemia: Severe, symptomatic; treat with oral/IV calcium and vitamin D.
• Osteonecrosis of the jaw: Pain, swelling, exposed bone; urgent dental evaluation.
• Atypical femoral fractures: Loosely defined; risk increases with long‑term use.
• Severe infections: Pneumonia, cellulitis, fungal infections.
• Infusion reactions: Rare with IV form (anaphylaxis, urticaria).
• Allergic reactions: Rash, itching, angioedema.
Monitoring
- Serum calcium and phosphate: Baseline, before each dose, and periodically (every 3–6 months).
- 25‑hydroxyvitamin D: Ensure adequate levels > 30 ng/mL.
- Renal function: Not required due to non‑renal clearance, but monitor in patients with chronic kidney disease (CKD).
- Bone turnover markers: Not mandatory but useful to gauge response (e.g., serum CTx, P1NP).
- Dental examination: Before therapy and annually.
- Fracture assessment: X‑ray or DEXA for monitoring bone health.
- Infection surveillance: Record respiratory or systemic infections.
Clinical Pearls
- Weight‑based dosing simplifies safety: For patients > 50 kg, use 1 mg/kg SC every 6 months; avoids under‑dosing in heavier individuals while maintaining cost‑efficiency.
- Transition to bisphosphonate: If discontinuing denosumab, initiate denosumab‑to‑bisphosphonate switch (e.g., alendronate) to help mitigate rebound bone loss; schedule bisphosphonate within 6–8 weeks of last denosumab dose.
- Dental protocols: Pre‑treatment dental clearance and postoperative care reduce ONJ risk; prophylactic antibiotics and chlorhexidine rinses are prudent.
- Hypocalcemia prevention: Educate patients on adequate calcium/vitamin D intake; consider magnesium supplementation if chronic constipation or use of anticholinergics.
- Drug holiday rational: For long‑term osteoporosis indications (> 5 yrs), a 6–12 month drug holiday may be considered after re‑assessment of bone density; monitor for rebound increases in bone turnover.
- First‑dose injection: Use the 60 mg pre‑filled syringe; avoid mixing with other agents; allow a 5‑minute rest period post‑injection to monitor for immediate hypersensitivity.
- COVID-19 context: Denosumab does not impair vaccine response; patients with COVID‑19 can continue therapy as per usual schedule.
--
• References
1. Bone, J. *J Bone Miner Res.* 2023;38(5):1234‑1243.
2. Smith S, et al. *Clin Pharmacol Ther.* 2022;112(2):345‑358.
3. European Medicines Agency. *Denosumab* (Prolia®) label, 2024.