Chronic non-cholestatic liver disease is not associated with an increased fracture rate in children.

J Bone Miner Metab

Department of Pediatrics and Developmental Disorders, Bone Densitometry Unit, Dr. Ludwik Zamenhof University Children's Hospital, Medical University of Bialystok, Waszyngtona St 17, 15274 Bialystok, Poland.

Published: May 2011

AI Article Synopsis

  • * The study involved 39 children with chronic hepatitis B, examining their fracture history, bone mass, and liver fibrosis severity; results showed no clear connection between liver fibrosis and bone density or fractures.
  • * Findings suggest that while children with chronic liver disease might have lower bone mineral density, this is not associated with liver fibrosis severity or increased fracture risk; they should be evaluated for fracture risk instead of solely relying on bone density tests.

Article Abstract

Chronic liver disease in adults is a risk factor of osteoporosis, but little is known about risk of fractures in children with non-cholestatic liver disease. The aim of this study was to investigate associations among the severity of liver fibrosis, bone mass and low-energy fractures in children. History of fractures, anthropometry, and bone mass and size were examined in 39 Caucasian children (25 boys, 14 girls) aged 7.1-18 years (mean 11.9 ± 3.1) with chronic hepatitis B and liver fibrosis evidenced by liver biopsy. Severity of liver fibrosis was based on histological classification according to the method of Batts and Ludwig (mild, 1-2 scores; advanced, 3 scores) and Ishak (1-3 and 4-5 scores, respectively). Bone mineral content (BMC), density (BMD) and body composition were determined in the total body and lumbar spine using dual energy X-ray absorptiometry. Seven subjects (4 girls, 3 boys; 18% of the sample) had low BMD in the total body and lumbar spine region (Z-scores below -2.0). No associations were found among BMC, BMD, bone size and the severity of liver fibrosis. Nine boys (36% of all boys) and one girl reported repeated fractures (forearm, wrist, tibia, ankle, humerus), showing trends similar to the prevalence in general population. Fractures were neither associated with lower BMD/BMC nor with scores of liver fibrosis. Deficits in BMD in children with chronic hepatitis B are not associated with the severity of liver fibrosis. This study suggests that non-cholestatic liver disease does not increase the risk of low-energy fractures during growth. From the practical perspective, however, children with chronic liver disease should be screened for history and clinical risk factors for fractures rather than referred to bone density testing.

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Source
http://dx.doi.org/10.1007/s00774-010-0219-7DOI Listing

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