Journal Facts

Journal
BoneKEy Knowledge Environment
ISSN
1940-8692
Volume
11
Year
2014

Article Facts

Title
Report on the ASBMR 2014 congress
DOI
10.1038/bonekey.2014.88
Authors

Adolfo Diez-Perez

Online Date
11/05/2014

Article Links

IBMS BoneKEy | Meeting Reports

Report on the ASBMR 2014 congress

Adolfo Diez-Perez


DOI:10.1038/bonekey.2014.88

Meeting Report from the ASBMR 2014 Annual Meeting, Houston, TX, USA, 12–15 September 2014.

Different aspects of clinical assessment and management of osteoporosis were communicated during the ASBMR 2014 congress. Among them we highlight several related to epidemiology, assessment and treatment.

Good influences on bone

In general, exercise interventions have provided little benefit in terms of bone mass. However, exercise by repetitive hopping selectively improves bone density in critical areas of the femoral neck and shaft. Vitamin D deficiency is endemic in patients with osteoporosis and in the general population. As a consequence of multiple factors, Vitamin D levels, the universal basso continuo for bone health, have improved over 11 years in the large cohort study SWAN (Study of Women’s Health Across the Nation). In the same study a 25% decrease in fracture risk was associated with each increase of 10 ng ml−1 in vitamin D levels across the menopause transition.

Fracture risk

Hypnotics and selective serotonin reuptake inhibitors are associated with fracture risk increases, further corroborating previous studies. The risk of subsequent fracture is also higher in the year after suffering one of such events. Proton pump inhibitors (PPI) use has also been described as associated with increased fracture risk, perhaps by increasing histamine release. However, the described association with the use of PPIs is mainly due to the underlying comorbidities rather than the drug itself. Not surprisingly, more thickness of the soft tissue covering the trochanter decreases the risk of hip fracture and can be measured on dual-energy X-ray absorptiometry (DXA) images.

Diabetes is a fracture risk assessment tool (FRAX)-independent risk factor for fracture with an added risk of 40% for hip and 32% for major osteoporotic fractures. Increased cortical porosity and lower cortical bone density may account, at least in part, for this increased risk, more specifically in the midcortical region, and these changes are independent of the presence of concomitant obesity.

Refining the measurement of bone strength

A novel technique for the direct measurement of bone material strength in patients, microindentation, detects bone mineral density (BMD)-independent deterioration of bone quality in patients with osteoporosis. This same derangement is present in patients with osteopenia who suffer fragility fracture. Similarly, subjects with stress fractures show impaired bone material strength also measured by microindentation. Trabecular Bone Score (TBS), a technique for DXA-based measurement of the bone microstructure, shows higher values for men than for women and their values decline with aging. Assessment of the microstructure by high-resolution peripheral quantitative computed tomography (pQCT) measurements in the OFELY study confirmed that it is predictive of fracture risk and, also with this technique, individual trabecular segmentation analysis corroborates that plate-like structures offer mechanical advantage over rod-like structures in terms of mechanical strength. Cortical bone is a critical element of fracture resistance, but its measurement by pHR QCT underestimates porosity by ∼50% and, therefore, its contribution to bone fragility.

Refining the diagnosis of osteoporosis

The National Bone Health Alliance Clinical Diagnosis of Osteoporosis Working Group presented their proposal for expanding the clinical diagnosis of osteoporosis beyond BMD-based criteria to patients who suffer a hip fracture, to those with osteopenia suffering a vertebral, proximal humerus, pelvis or some distal radius fractures as well as to those with osteopenia and a FRAX score that exceeds the National Osteoporosis Foundation thresholds of intervention.

Osteoporosis treatment with available…

There is debate on the duration of treatment with bisphosphonates and the need for discontinuing the drug after 3–5 years. A retrospective study of a large database revealed that there was no increase in fracture risk in women treated with bisphosphonates for 3 years if they took a 12-month ‘drug holiday’ in comparison with those treated continuously. Denosumab treatment shows a distinctive effect on cortical bone, and this efficacy is further stressed by the restoration of BMD at the radius with decreased wrist fracture incidence. Its use for up to 8 years results in a significant 82% of treated individuals reaching BMD levels above the osteoporosis threshold. Zoledronic acid treatment has a long-lasting effect, and this has been the basis for treating patients with Paget’s disease with a single infusion. In a parallel approach, a single infusion of zoledronic acid in elderly individuals with cognitive impairment showed positive effects on BMD for 3 years with no undesirable effects.

…with combined…

Combination of denosumab and teriparatide has been evaluated as a possible way to improve bone efficacy in the treatment of osteoporosis. This combined regime offers a superior effect on volumetric BMD than either drug alone after 2 years with improvements in the cortical microstructure and in peripheral density and microarchitecture.

…and with new agents

Romosozumab, an antisclerostin mAb tested in the treatment of osteoporosis, shows superior effects over teriparatide in cortical mass, density and thickness in the vertebral body. Blosozumab, another antisclerostin mAb in development, strikingly increases BMD over 1 year but this effect is greatly reversed when the drug is discontinued for an additional year. Abaloparatide, an hPTHrP analog, restores cortical and trabecular bone loss in ovariectomized Cyno monkeys without an effect on cortical porosity. Expanding the treatment of osteoporosis-related fracture risk beyond bone to sarcopenia, the results of a phase 2 RCT with antimyostatin antibody in elderly individuals with frequent falls showed improvement in lean body mass and physical performance after 6 months.

Odanacatib is a cathepsin K inhibitor already tested in phase 2 for the treatment of osteoporosis. Undoubtedly, the most awaited news was the report of the results of the phase 3 study, the LOFT trial. A total of 16 713 women with osteoporosis (T-score at the hip −2.5 to −4 without previous vertebral fracture or −1.5 to −4 without vertebral fracture), of age 65 years or older, were enrolled in 40 countries in a randomized, double blind, event-driven trial. Participants received either 50 mg of odanacatib once a week or placebo. All participants received calcium supplements and 5600 IU of vitamin D a week. After a mean treatment duration of 34 months, there was significant relative risk reduction in the active arm of 54% for morphometric vertebral fractures, 47% for hip and 23% for non-vertebral fractures. BMD increased by 11.2% at the spine and 9.5% in total hip vs placebo over 5 years. NTX decreased rapidly and remained low while P1NP decreased less markedly and returned to baseline.

Adverse events (AEs) were not statistically different between active treatment and placebo arms, with no cases of osteonecrosis of the jaw. However, there was a numerical imbalance, although nonsignificant, in some AEs. Odanacatib-treated patients suffered 5 cases of atypical femoral fracture versus none in the placebo group (P<0.05), none of them spontaneous and all in patients with severe osteoporosis in terms of BMD. Furthermore, the hazard ratio (95% confidence interval ) for major cardiovascular events was 1.12 (0.93–1.36), that for investigator-reported cerebrovascular events was 1.06 (0.91–1.25), that for stroke was 1.28 (0.97–1.70) and for death was 1.13 (0.95–1.35), all slightly, nonsignificantly increased compared with placebo. A few more cases of atrial fibrillation (92 vs 80, HR 1.17 (0.87–1.58)) were also observed in the treatment group. Twelve patients in the odanacatib group and 3 in the placebo arm developed morphea-like lesions, which resolved or improved after discontinuation of treatment. Similar results in terms of BMD were reported for men (1149) in a small-sized trial.

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