| Literature DB >> 21702989 |
François-Emery Cotté1, Gérard De Pouvourville.
Abstract
BACKGROUND: During the last decade, oral bisphosphonates (BP) became the most widely prescribed pharmacologic class for post-menopausal osteoporosis. However, many surveys revealed the important issue of poor persistence with those drugs resulting in a failure of treatment to reduce fracture risk sufficiently. Using a published Markov model, this study analyses the economic impact of non-persistence with bisphosphonates in the context of the introduction of generics in France.Entities:
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Year: 2011 PMID: 21702989 PMCID: PMC3141385 DOI: 10.1186/1472-6963-11-151
Source DB: PubMed Journal: BMC Health Serv Res ISSN: 1472-6963 Impact factor: 2.655
Figure 1Markov model structure.
Model inputs
| Clinical inputs for transition probabilities | Values | Sources | ||
|---|---|---|---|---|
| Age distribution (mean in years) | 70.5 | |||
| Prior fracture (%) | 59.7 | |||
| 50-54 years | 3.10 | 0.00 | 2.99 | |
| 55-59 years | 3.59 | 0.06 | 3.20 | |
| 60-64 years | 4.15 | 0.20 | 3.18 | |
| 65-69 years | 4.81 | 0.34 | 2.06 | |
| 70-74 years | 5.56 | 0.65 | 1.97 | |
| 75-79 years | 6.44 | 1.04 | 1.17 | |
| 80-84 years | 7.45 | 1.62 | 0.92 | |
| > 84 years | 8.62 | 3.52 | 0.92 | |
| associated with any prior fracture at baseline | 2.0 | 2.0 | 1.9 | |
| post-vertebral fracture health state | 4.4 | 2.3 | 1.4 | |
| post-hip fracture health state | 2.5 | 2.3 | NA | |
| post-wrist fracture health state | 1.7 | 1.9 | 3.3 | |
| for any women at baseline | 0.526 | 0.672 | 0.833 | |
| from post-vertebral fracture health state | 0.575 | 0.620 | NA | |
| from post-hip fracture health state | NA | 0.620 | NA | |
| from post-wrist fracture health state | 0.575 | 0.620 | 0.566 | |
| Treatment duration ( | ||||
| Start | 100 | |||
| 6 | 65 | *Source data were fitted to an exponential function to generate persistence curve over 24 months: | ||
| 12 | 51 | |||
| 24 | 41 | |||
| 36 | 30* | |||
| 48 | 24* | |||
| 60 to simulation ending time | 20* | |||
| Treatment duration ( | ||||
| Start | 0 | |||
| 12 | 24 | **Residual effect of BP was modeled as follow: | ||
| 24 | 43 | |||
| 36 | 76 | |||
| 48 | All simulation period | |||
| 60 to simulation ending time | All simulation period | |||
Direct costs of osteoporotic fractures management in France (euros 2010)
| Fracture site | Hip | Wrist | Vertebra |
|---|---|---|---|
| Codes | S720-S7200 | S525-S526 | M485(0-9); S22(0-1); S2200; S2210; S320(0); S327(0); S328(0) |
| Number | 53,376 | 10,394 | 26,490 |
| Median cost | €7,170 | €2,615 | €2,085 |
| Min-Max costs | €1,992 - €15,720 | €614 - €3,363 | €640 - €15,720 |
| All fractures | €372,849,923 | €18,775,427 | €93,325,278 |
| Weighted average cost per unit | €7,308 | €1,844 | €3,523 |
*DRGs associated with less than 1% of all cases were not taking into account (PMSI 2008).
**Assumption of 40.0%, 36.0% and 44.2% of rehabilitation cost proportion for vertebral, hip and wrist fractures respectively [35]
10-year Monte-Carlo simulation outcomes
| No-treatment | Real-world persistence | Ideal persistence | ||
|---|---|---|---|---|
| 8,193 | 6,308 | 3,912 | ||
| 5,534 | 4,462 | 3,313 | ||
| 6,674 | 5,941 | 5,153 | ||
| 20,401 | 16,711 | 12,378 | ||
| 20,131 | 17,996 | 14,715 | ||
| 1,816 | 1,466 | 1,015 | ||
Figure 2Distribution of 10-year fracture cost management.
Cost-effectiveness of bisphosphonates for real-world and ideal persistence alternatives
| Alternatives | No-treatment | Real-world persistence | Ideal persistence | |
|---|---|---|---|---|
| Average per patients | €3,402 | €3,110 | €2,833 | |
| Incremental | -- | -€293* | -€277** | |
| Proportion | 0.671 | 0.600 | 0.491 | |
| Incremental | -- | -0.071† | -0.109†† | |
| Discounted | -- | (Dominated) | (Dominated) | |
| Proportion | 0.061 | 0.049 | 0.034 | |
| Incremental | -- | -0,012† | -0,015†† | |
| Discounted | -- | (Dominated) | (Dominated) | |
* μcReal-world persistence--μcNo treatment; ** μcIdeal persistence--μcReal-world persistence
† μEReal-world persistence--μENo treatment; †† μEIdeal persistence--μEReal-world persistence
Figure 3Change in drug and nondrug costs in function of persistence.