Table 2.
Comparison of major characteristics of bisphosphonates (alendronate and zoledronic acid) versus denosumab.
| Bisphosphonates
|
Denosumab
|
||
|---|---|---|---|
| Alendronate | Zoledronic Acid | ||
|
|
|||
| Efficacy | Vertebral and hip fracture reduction: ~ 50% (STAND and DECIDE trials comparing alendronate to denosumab showed greater BMD gains with denosumab at 12 months) | Vertebral fracture reduction: 70%. Hip fracture reduction: 41%. (Ongoing trial comparing efficacy of ZA vs denosumab) | Vertebral fracture reduction: 68%. Hip fracture reduction: 40% |
| Pivotal Trial | FIT [54] | HORIZON-PFT [55] | FREEDOM [20] |
| Safety | Risk for AFF and ONJ with prolonged exposure | Risk for AFF and ONJ with exposure to high doses and/or prolonged exposure | Risk for AFF and ONJ. Increased risk of serious skin infections |
| Administration | Oral, patient administered weekly | Intravenous administration once a year. Requires IV catheter placement | Subcutaneous injection every 6 months. Can be administered in office |
| Pharmacokinetics | Poor oral bioavailability. Non-uniform drug accumulation within bone matrix, with elimination half-life of ~ 10 years | Non-uniform drug accumulation within bone matrix, with prolonged suppression of bone turnover | No bone accumulation, effects reversible by 9 – 12 months post-dose |
| Pharmacodynamics | Slow suppression of bone turnover | More rapid suppression of bone turnover than oral (within days) | Rapid suppression of bone turnover (within 12 h) |
| Use in renal impairment | Contraindicated for GFR < 35 | Contraindicated for GFR < 35 | No restriction for use in renal impairment, though close monitoring of serum calcium in patients with GFR < 30 recommended |
| Relative cost | Low (generic available) | Moderate/High (generic available) | High |
AFF: Atypical femur fractures; GFR: Glomerular filtration rate; ONJ: Osteonecrosis of the jaw.