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Chapter 80 - Macroimaging

This chapter reviews in vivo imaging techniques used in the field of osteoporosis for diagnosis of osteoporosis, fracture prediction, or monitoring of therapeutic interventions and age-related changes. Standard techniques include radiography to diagnose fractures, quantitative computed tomography (QCT) to determine bone mineral density (BMD) and cortical geometry, and finite element analysis to measure bone strength. New developments include advanced dual-energy X-ray absorptiometry (DXA) analysis to obtain the trabecular bone score for assessing vertebral bone texture and the possibility of generating CT-like volumetric data from DXA scans[VK1] . High-resolution peripheral QCT can be used to measure trabecular structure and cortical porosity at the distal forearm and tibia. Magnetic resonance imaging (MRI) offers the unique possibility of determining cortical water to characterize collagen content and cortical porosity. Another application of MRI is the measurement of bone marrow fat content and composition, marrow perfusion, and marrow molecular diffusion. Most recent applications of CT include opportunistic screening, the reuse of existing CT images obtained for routine clinical purposes such as tumor diagnosis, to identify patients at high risk for osteoporotic fracture. Another emerging field is the combination of muscle parameters determined either by MRI or by CT with standard BMD and geometry parameters to improve fracture risk prediction by potentially addressing the components of a fall, which are related to muscle characteristics

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Chapter 15 - Secreted noncollagenous proteins of bone

Bone differs from soft connective tissues in that it is composed of a mineralized hydroxyapatite phase and an organic phase. Although the organic matrix of bone consists primarily of collagen(s) (as reviewed early in this volume), the existence of other secreted noncollagenous components was first postulated by Herring and co-workers in the 1960s. Historically, using degradative techniques, a variety of carbohydrate-containing moieties were extracted and partially characterized. A major breakthrough in the isolation and characterization of noncollagenous proteins of bone came with the development of “dissociative” techniques whereby proteins could be extracted in an intact, nonaggregated form. Although they are not as abundant as so-called structural components such as collagen, their importance in bone physiology cannot be underestimated. This is emphasized by the identification of mutations in a number of these proteins that result in abnormal bone. This chapter discusses secreted noncollagenous proteins found in bone matrix. Since the publication of the previous edition of this work in 2008, substantial additions have been made to include recently reported functional studies, inclusion of noncollagenous proteins that were not previously considered, and new information regarding the developing area of bone–muscle/fat/pancreas/testis cross-talk signaling and the role that these proteins play in those interactions.

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