Abstract

Chronic metabolic acidosis, a relatively common clinical disorder found in the patients with renal insufficiency and renal tubular acidosis, cause dissolution of bone mineral. This research has the long-term objective of improving our understanding of how protons cause bone mineral dissolution. This will be accomplished by studying acid induced calcium release from cultured mouse calvariae using a high resolution scanning ion microprobe and x-ray diffraction in conjunction with measurements of medium saturation and ion flux. Neonatal mouse calvaria (frontal and parietal bones of the skull) in culture is an appropriate model in which to study the effects of protons on bone since calvariae release calcium an buffer protons during culture in acidic medium, as human bone dose in vivo. We will attempt to attain a better understanding of how changes in pH effect the bone mineral in order to construct a model of proton induced bone mineral dissolution. We propose to test the following hypothesis: 1) That chronic culture of bone in an acidic medium results in similar changes in one surface elements as chronic metabolic acidosis in vivo. We will determine the change in surface elements, using the ion microprobe, of cultured neonatal mouse calvariae in response to a chronic (24-96 hrs) lowering of medium bicarbonate concentration, an in vitro model of chronic metabolic acidosis. We will determine the change in mineral composition in neonatal mice injected with NH4C1, an in vivo model of chronic metabolic acidosis, and compare them to calvariae cultured in acidic medium. 2) That pH induced alterations in bone cell function are instrumental in augmenting calcium release during chronic culture in an acidic medium. This will be tested by treating the calvariae with agents which alter bone cell function, but do not directly affect the bone mineral, and comparing rates of proton induced calcium efflux, differences in the mineral surface elements and differences in the mineral phases. 3) That calcium carbonate is the initial phase of the bone mineral depleted during chronic culture in an acid medium by determining the phase(s) of mineral depleted in chronic culture using x-ray diffraction. 4) That hormonally induced bone resorption has the same effect on the bone mineral surface elements and mineral phases as proton induced bone resorption. This will be tested by culturing calvariae with parathyroid hormone and comparing them to calvariae cultured in and acidic medium. 5) That an elevated partial pressure of carbon dioxide (pC02) will increase bone carbonate content by culturing calvariae in an elevated pC02, a model of chronic respiratory acidosis, and determining the mineral phases by x-ray diffraction.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR039906-03
Application #
3160142
Study Section
Orthopedics and Musculoskeletal Study Section (ORTH)
Project Start
1989-09-30
Project End
1992-08-31
Budget Start
1990-09-01
Budget End
1992-08-31
Support Year
3
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of Rochester
Department
Type
Schools of Dentistry
DUNS #
208469486
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Bushinsky, D A; Grynpas, M D; Asplin, J R (2001) Effect of acidosis on urine supersaturation and stone formation in genetic hypercalciuric stone-forming rats. Kidney Int 59:1415-23
Bushinsky, D A; Parker, W R; Asplin, J R (2000) Calcium phosphate supersaturation regulates stone formation in genetic hypercalciuric stone-forming rats. Kidney Int 57:550-60
Bushinsky, D A (1999) Genetic hypercalciuric stone-forming rats. Curr Opin Nephrol Hypertens 8:479-88
Frick, K K; Bushinsky, D A (1999) In vitro metabolic and respiratory acidosis selectively inhibit osteoblastic matrix gene expression. Am J Physiol 277:F750-5
Bushinsky, D A; Neumann, K J; Asplin, J et al. (1999) Alendronate decreases urine calcium and supersaturation in genetic hypercalciuric rats. Kidney Int 55:234-43
Bushinsky, D A; Chabala, J M; Gavrilov, K L et al. (1999) Effects of in vivo metabolic acidosis on midcortical bone ion composition. Am J Physiol 277:F813-9
Bushinsky, D A; Bashir, M A; Riordon, D R et al. (1999) Increased dietary oxalate does not increase urinary calcium oxalate saturation in hypercalciuric rats. Kidney Int 55:602-12
Frick, K K; Bushinsky, D A (1998) Chronic metabolic acidosis reversibly inhibits extracellular matrix gene expression in mouse osteoblasts. Am J Physiol 275:F840-7
Bushinsky, D A (1998) Nephrolithiasis. J Am Soc Nephrol 9:917-24
Tsuruoka, S; Bushinsky, D A; Schwartz, G J (1997) Defective renal calcium reabsorption in genetic hypercalciuric rats. Kidney Int 51:1540-7

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