| Literature DB >> 27617159 |
Esther Kinning1, Martin McMillan2, Sheila Shepherd2, Miep Helfrich3, Rob Vant Hof4, Christopher Adams5, Heather Read2, Daniel M Wall6, S Faisal Ahmed2.
Abstract
The purpose of this study was to investigate the association of a chromosome 4:20 imbalance with osteoporosis in three related children. Bone biochemistry, bone turnover markers, and dual-energy X-ray absorptiometry (DXA) scanning were performed in all three cases and bone biopsy and histomorphometry in one. The chromosome imbalance was delineated by array comparative genomic hybridization (aCGH) and analyzed for candidate genes. A potential candidate gene within the deleted region is caspase-3, previously linked to low bone mineral density (BMD) in heterozygous mice thus caspase-3 activity was measured in cases and controls. Routine bone biochemistry and markers of bone turnover did not reveal any abnormality. DXA showed reduced total and lumbar spine bone mineral content. aCGH showed an 8 megabase (Mb) deletion of terminal chromosome 4q incorporating a region previously linked to low BMD and a 15 Mb duplication of terminal chromosome 20p. Bone biopsy showed a high bone turnover state, trabecularisation of cortical bone and numerous small osteoclasts coupled with normal bone formation. Basal serum caspase-3 activity was lower in cases compared with controls. We conclude that the early-onset osteoporosis with low basal levels of caspase-3 and abnormal osteoclasts is a feature of this chromosomal translocation. Further investigation of the role of the deleted and duplicated genes and especially caspase-3 is required.Entities:
Keywords: bone histomorphometry; caspase; chromosome translocation; osteoclast; osteoporosis
Year: 2016 PMID: 27617159 PMCID: PMC4999330 DOI: 10.1055/s-0036-1584359
Source DB: PubMed Journal: J Pediatr Genet ISSN: 2146-460X