Are activated T cells regulators of bone metabolism in children with Crohn disease

2006 
Objectives To test the hypothesis that circulating activated T cells may release cytokines that decrease bone turnover in children with Crohn disease. Study design Newly diagnosed Crohn disease and healthy controls of similar age were compared for bone age, bone mineral content and density, markers of bone remodeling, and serum concentration and in vitro T-cell production of receptor activator of nuclear factor κB ligand (RANKL), interferon (INF)-γ, and osteoprotegerin (OPG). Results Newly diagnosed children with Crohn disease (n = 23) had similar bone mineral density (BMD) z -scores and body mass index as the controls (n = 40). Biochemical markers of bone remodeling indicated a state of low bone turnover in the Crohn disease patients compared with controls. Serum OPG (pmol/L; mean ± SD, median) was higher (4.24 ± 1.74, 3.98 vs 3.38 ± 0.83, 3.41; P P P Conclusions The newly diagnosed children with Crohn disease exhibited reduced bone remodeling, possibly due to T-cell INF-γ and OPG.
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