Short-Term Urine Deoxypyridinoline Biological Variability in the First 5 Years After Menopause (Technical Briefs) Short-Term Urine Deoxypyridinoline Biological Variability in the First 5 Years After Menopause (Technical Briefs)

Short-Term Urine Deoxypyridinoline Biological Variability in the First 5 Years After Menopause (Technical Briefs‪)‬

Clinical Chemistry 2005, Nov, 51, 11

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Publisher Description

There is evidence that bone turnover in women is more rapid during the first years after menopause than in subsequent years. The assessment of deoxypyridinoline (DPD) cross-links in a fasting urine sample is considered a specific index of bone resorption by osteoclasts and also can be used for monitoring the response to pharmacologic antiresorption treatment. The interpretation of results, however, is hampered by biological and other preanalytical variability (1-4). Specific degradation products of the bone matrix, such as DPD and pyridinoline (PYD), closely reflect the rate of bone metabolism. Vesper et al. (1) reported mean withinday variabilities of 67% for DPD (range, 53%-75%) and 71% for PYD (57%-78%). The mean between-day variability was 16% for both PYD and DPD (ranges, 5%-24% and 12%-21% for DPD and PYD, respectively). The mean between-person variabilities across different studies were 34% for DPD (8%-98%) and 26% for PYD (12%-63%) in healthy premenopausal women and 40% (27%-54%) and 36% (22%-61%), respectively, in postmenopausal women. Specimen instability and errors in creatinine measurements were additional sources of variability (1). Some authors have reported that the variability can be reduced by collecting urine for 24 h (or longer) instead of using single voids and by expressing the results as ratios to creatinine (5, 6).

GENRE
Science & Nature
RELEASED
2005
November 1
LANGUAGE
EN
English
LENGTH
8
Pages
PUBLISHER
American Association for Clinical Chemistry, Inc.
SELLER
The Gale Group, Inc., a Delaware corporation and an affiliate of Cengage Learning, Inc.
SIZE
179.2
KB
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