RANKL:Osteoprotegerin ratio and bone mineral density in children with untreated juvenile dermatomyositis
β Scribed by Kelly A. Rouster-Stevens; Craig B. Langman; Heather E. Price; Roopa Seshadri; Richard M. Shore; Kathy Abbott; Lauren M. Pachman
- Publisher
- John Wiley and Sons
- Year
- 2007
- Tongue
- English
- Weight
- 130 KB
- Volume
- 56
- Category
- Article
- ISSN
- 0004-3591
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β¦ Synopsis
Abstract
Objective
To determine bone mineral density (BMD) in patients at the time of diagnosis of juvenile dermatomyositis (DM), to compare the RANKL:osteoprotegerin (OPG) ratio in patients with juvenile DM with that in healthy control subjects, and to evaluate whether BMD is associated with the RANKL:OPG ratio and the duration of untreated disease.
Methods
Thirtyβseven children with juvenile DM were enrolled. Dual xβray absorptiometry (DXA) was performed before treatment, and Z scores for the lumbar spine (L1βL4) were determined. The duration of untreated disease was defined as the period of time from the onset of rash or weakness to the time at which DXA was performed. Serum specimens obtained at the time of DXA were analyzed for concentrations of RANKL and OPG, using enzymeβlinked immunosorbent assay. The RANKL:OPG ratio was also determined in 44 ageβmatched healthy control subjects.
Results
At the time of diagnosis of juvenile DM, patients had a significantly increased RANKL:OPG ratio compared with that in healthy children (mean Β± SD 2.19 Β± 3.03 and 0.13 Β± 0.17, respectively; P < 0.0001). In patients with a lumbar spine BMD Z score of β1.5 or lower, the RANKL:OPG ratio was significantly higher than that in patients with a lumbar spine BMD Z score higher than β1.5 (P = 0.038). Lumbar spine BMD Z scores (mean Β± SD β0.13 Β± 1.19 [range β2.10 to 2.85]) were inversely associated with the duration of untreated disease (R = β0.50, P = 0.003).
Conclusion
Children with juvenile DM have an elevated RANKL:OPG ratio at the time of diagnosis, resulting in expansion of the number of osteoclasts and activation of the bone resorptive function. This may lead to a lack of normal bone mineral accretion and a subsequent reduction in the lumbar spine BMD Z score. Patients with a longer duration of untreated juvenile DM have reduced lumbar spine BMD Z scores. These data suggest that early diagnosis could reduce the likelihood of reduced lumbar spine BMD in these patients by prompting intervention strategies at an early stage.
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