Abstract

The unique strength and rigidity of bone arises from a combination of organic components (primarily collagen) and inorganic (mineral) components. Over a lifetime, bone is continuously remodeling itself. Old bone is eroded away in a tunnel-like fashion by osteoclasts and new bone is deposited layer-by-layer in the ?tunnel? by osteoblasts. From a cross-sectional view, these new layers of bone, collectively termed an osteon, appear as series of concentric circles through a microscope. A typical osteon measures ~200 ?m in diameter, where the youngest bone is at the center. In many diseased states of bone, there is an imbalance between bone production and resorption, resulting in overgrowth (osteopetrosis) or undergrowth (osteoporosis) of bone. To date, it is unclear whether the chemical composition of the bone in a diseased state is the same as normal bone. Using infrared micro-spectroscopy, we are able to visibly and chemically image individual osteons in terms of growth-, site-, and age-dependent variations in mineral content (i.e. carbonate, phosphate, acid phosphate), mineral crystallinity, and the content/nature of the organic matrix. A significant advantage of this technique over other chemical methods is that the bone does not need to be homogenized before testing; we are able to study cross-sectional samples of bone in situ at a resolution of 3-5 ?m. In this study, we present a comparison of human osteoporotic bone to osteopetrotic bone. Early results show some similarities and also significant differences between osteopetrotic and osteoporotic bone. For both diseased states Hof bone, the ratios of phosphate-to-collagen and carbonate-to-collagen Hconcentrations are similar and these ratios increases as bone matures H(from the center to the periphery of the osteon). Also for both, the Hphosphate ions (PO43-) are replaced by other anions such as carbonate H(CO32-) as bone ages, i.e. the hydroxyapatite becomes Hnon-stoichiometric. However in contrast, we observe significantly Hmore CO32- substitution in osteoporotic bone than osteopetrotic bone Has the bone matures.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Biotechnology Resource Grants (P41)
Project #
5P41RR001633-17
Application #
6205728
Study Section
Project Start
1999-09-01
Project End
2000-08-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
17
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Type
DUNS #
009095365
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Vongsvivut, Jitraporn; Fernandez, Jason; Ekgasit, Sanong et al. (2004) Characterization of supported cylinder-planar germanium waveguide sensors with synchrotron infrared radiation. Appl Spectrosc 58:143-51
Masip, Lluis; Pan, Jonathan L; Haldar, Suranjana et al. (2004) An engineered pathway for the formation of protein disulfide bonds. Science 303:1185-9
Huang, Raymond Y; Miller, Lisa M; Carlson, Cathy S et al. (2003) In situ chemistry of osteoporosis revealed by synchrotron infrared microspectroscopy. Bone 33:514-21
Rashidzadeh, Hassan; Khrapunov, Sergei; Chance, Mark R et al. (2003) Solution structure and interdomain interactions of the Saccharomyces cerevisiae ""TATA binding protein"" (TBP) probed by radiolytic protein footprinting. Biochemistry 42:3655-65
Uchida, Takeshi; Takamoto, Keiji; He, Qin et al. (2003) Multiple monovalent ion-dependent pathways for the folding of the L-21 Tetrahymena thermophila ribozyme. J Mol Biol 328:463-78
Taylor, Colleen M; Watton, Stephen P; Bryngelson, Peter A et al. (2003) Inner-sphere complexation of cobalt(II) 2,9-dimethyl-1,10-phenanthroline ([Co(neo)]2+) with commercial and sol-gel derived silica gel surfaces. Inorg Chem 42:312-20
Tang, Qun; Carrington, Paul E; Horng, Yih-Chern et al. (2002) X-ray absorption and resonance Raman studies of methyl-coenzyme M reductase indicating that ligand exchange and macrocycle reduction accompany reductive activation. J Am Chem Soc 124:13242-56
Guan, Jing-Qu; Vorobiev, Sergeui; Almo, Steven C et al. (2002) Mapping the G-actin binding surface of cofilin using synchrotron protein footprinting. Biochemistry 41:5765-75
Chance, Mark R; Bresnick, Anne R; Burley, Stephen K et al. (2002) Structural genomics: a pipeline for providing structures for the biologist. Protein Sci 11:723-38
Maleknia, Simin D; Kiselar, Janna G; Downard, Kevin M (2002) Hydroxyl radical probe of the surface of lysozyme by synchrotron radiolysis and mass spectrometry. Rapid Commun Mass Spectrom 16:53-61

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