Relationship between biochemical markers of bone turnover and bone scintigraphic indices in assessment of Paget's disease activity
L Alvarez, P Peris, F Pons… - … : Official Journal of …, 1997 - Wiley Online Library
L Alvarez, P Peris, F Pons, N Guañabens, R Herranz, A Monegal, JL Bedini, R Deulofeu…
Arthritis & Rheumatism: Official Journal of the American College …, 1997•Wiley Online LibraryObjective. To evaluate the relationship between biochemical markers of bone turnover and
bone scan indices of disease activity, as well as to analyze their variations based on skeletal
involvement, in Paget's disease. Methods. Serum samples were obtained from 51 patients
with Paget's disease to determine the levels of total alkaline phosphatase (total AP), bone
alkaline phosphatase (bone AP), propeptide carboxyterminal of type I procollagen (PICP),
propeptide aminoterminal of type I procollagen (PINP), osteocalcin, tartrate‐resistant acid …
bone scan indices of disease activity, as well as to analyze their variations based on skeletal
involvement, in Paget's disease. Methods. Serum samples were obtained from 51 patients
with Paget's disease to determine the levels of total alkaline phosphatase (total AP), bone
alkaline phosphatase (bone AP), propeptide carboxyterminal of type I procollagen (PICP),
propeptide aminoterminal of type I procollagen (PINP), osteocalcin, tartrate‐resistant acid …
Abstract
Objective. To evaluate the relationship between biochemical markers of bone turnover and bone scan indices of disease activity, as well as to analyze their variations based on skeletal involvement, in Paget's disease.
Methods. Serum samples were obtained from 51 patients with Paget's disease to determine the levels of total alkaline phosphatase (total AP), bone alkaline phosphatase (bone AP), propeptide carboxyterminal of type I procollagen (PICP), propeptide aminoterminal of type I procollagen (PINP), osteocalcin, tartrate‐resistant acid phosphatase, and telopeptide carboxyterminal of type I collagen. Urine samples were analyzed for levels of hydroxyproline (HYP), pyridinoline (PYR), deoxypyridinoline (DPYR), C‐terminal telopeptide of type I collagen (CTx), and N‐terminal telopeptide of type I collagen (NTx). In addition, 2 semiquantitative scintigraphic indices, disease activity (AI) and disease extent (EI), were obtained. Pagetic skeletal locations were evaluated individually, with special attention to skull involvement.
Results. All biochemical markers correlated with the AI and the EI. Serum PINP, bone AP, and total AP showed the highest proportions of increased values among the bone formation markers (94%, 82%, and 76%, respectively). Among the bone resorption markers, urinary NTx showed the highest proportion of increased values in patients with Paget's disease (96%), compared with PYR (69%), DPYR (71%), CTx (65%), and HYP (64%). In patients with mild disease activity, serum PINP was the marker with the highest proportion of increased values (71%). In contrast, serum PICP and urinary CTx were the most discriminative markers for skull involvement. Except for higher values for most of the biochemical markers of bone turnover in flat bones, no major differences in other skeletal locations were observed.
Conclusion. The determination of serum PINP as a marker of bone formation and urinary NTx as a marker of bone resorption provided the best biochemical profile to ascertain the extent and activity of Paget's disease. In patients with skull involvement, serum PICP and urinary CTx were shown to be the most discriminative markers.
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