Guest guest Posted December 28, 2007 Report Share Posted December 28, 2007 Presentation Number:242 Poster Board Number:242 Presentation Time:11/8/2007 8:00:00 AM Title: Bone Morbidity in Glucocorticoid-treated Children with Chronic Rheumatic Disease (CRD) Category:11. Pediatric rheumatology clinical and therapeutic disease Author(s). A. Cabral1, B. Lang2, P. B. Dent3, J. Ellsworth4, A. M. Huber2, C. LeBlanc5, P. M. Miettunen6, K. Oen7, S. E. Ramsey2, C. Saint-Cyr8, R. Scuccimarri9, J. Hay10, M. Matzinger5, N. Shenouda5, L. M. Ward5, and the STOPP Consortium. 1U of British Columbia, Vancouver, BC, Canada; 2Dalhousie Univ, Halifax, NS, Canada; 3McMaster Univ, Hamilton, ON, Canada; 4U of Alberta, Edmonton, AB, Canada; 5U of Ottawa, Ottawa, ON, Canada; 6U of Calgary, Calgary, AB, Canada; 7U of Manitoba, Winnipeg, MB, Canada; 8U de Montréal, Montréal, QC, Canada; 9McGill Univ, Montréal, QC, Canada; 10Brock Univ, St. Catharines, ON, Canada Aims Children with CRD are at risk for compromised bone health from factors that include underlying disease and glucocorticoid (GC) use. The STeroid-induced Osteoporosis in the Pediatric Population (STOPP) study involving 10 Canadian tertiary pediatric centres aims to prospectively evaluate the magnitude and rate of bone mineral density (BMD) and content (BMC) changes after initiating GC in CRD patients, and to identify and characterize atraumatic fractures. Methods Children (≤ 16y) initiating GC for treatment of CRD since Jan 2005 were eligible for inclusion. Enrolled patients had baseline (< 30 days) and 6-monthly (6m) BMD/BMC studies; x-rays of lateral spine at baseline and for clinically suspected fractures; baseline plus 3 monthly assessment of medications, disease activity (10 cm visual analog scale) and 2-day physical activity (Habitual Activity Estimation Scale). Results We report on 66 (20 male, mean (SD) age 9.6 (4.4) years) of 101 patients with 6m minimum followup whose diagnoses were juvenile idiopathic arthritis (JIA) 32%, juvenile dermatomyositis (JDM) 29%, systemic lupus erythematosus (SLE)/connective tissue disorders 21% and chronic vasculitis 18%. Median disease durations from symptom onset to enrollment were: 104, 134, 185 and 95 days respectively. At baseline 3 (4.5%) patients (JIA, SLE, JDM) had vertebral compression fractures, only JDM being symptomatic. By 6m there were no additional symptomatic fractures. The baseline mean areal spine BMD z score of -0.6 (1.1) was significantly below the healthy average despite normal height z scores. Changes between baseline and 6m included the following: a mean reduction of 2.8% in spine volumetric BMD; an absolute decrease in spine BMC in 39 (64%) patients (mean reduction of 7.4% ) in this subgroup); a decrease in median disease activity score from 6.4 to 1.6; an increase in overall median hours of physical activity from 11.9 to 16.2; and a decrease in median hours of inactivity from 15.2 to 11.5. The median daily prednisone dose fell from the first to the second 3 months from 1.4 to 0.3 mg/kg. Conclusions At the time of GC initiation children with CRD may already have atraumatic fractures and a lower than average BMD. By 6m despite reduced disease activity and increased physical activity they have further bone morbidity manifested by a drop in spinal volumetric BMD, and an absolute loss of spine BMC in a majority. The long term fracture risk versus potential for bone mass restitution remains to be determined. Disclosures: D.A. Cabral, None; B. Lang, None; P.B. Dent, None; J. Ellsworth, None; A.M. Huber, None; C. LeBlanc, None; P.M. Miettunen, None; K. Oen, None; S.E. Ramsey, None; C. Saint-Cyr, None; R. Scuccimarri, None; J. Hay, None; M. Matzinger, None; N. Shenouda, None; L.M. Ward, None. Quote Link to comment Share on other sites More sharing options...
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