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Title: Calcium and phosphate homeostasis: concerted interplay of new regulators.
Author(s): Renkema, K.Y.R. (298980150)
Alexander, R.T. (314445641)
Bindels, R.J.M. (07205378X)
Hoenderop, J.G.J. (195017544)
Publication year: 2008
Document type: Article / Letter to editor
Journal: Annals of Medicine
ISSN: 0785-3890
Volume: vol. 40
Issue: iss. 2
Start page: p. 82
End page: p. 91
Abstract: Calcium (Ca(2+)) and phosphate (P(i)) are essential to many vital physiological processes. Consequently the maintenance of Ca(2+) and P(i) homeostasis is essential to a healthy existence. This occurs through the concerted action of intestinal, renal, and skeletal regulatory mechanisms. Ca(2+) and P(i) handling by these organs is under tight hormonal control. Disturbances in their homeostasis have been linked to pathophysiological disorders including chronic renal insufficiency, kidney stone formation, and bone abnormalities. Importantly, the kidneys fine-tune the amount of Ca(2+) and P(i) retained in the body by altering their (re)absorption from the glomerular filtrate. The ion transport proteins involved in this process have been studied extensively. Recently, new key players have been identified in the regulation of the Ca(2+) and P(i) balance. Novel regulatory mechanisms and their implications were introduced for the antiaging hormone klotho and fibroblast growth factor member 23 (FGF23). Importantly, transgenic mouse models, exhibiting disturbances in Ca(2+) and P(i) balance, have been of great value in the elucidation of klotho and FGF23 functioning. This review highlights the current knowledge and ongoing research into Ca(2+) and P(i) homeostasis, emphasizing findings from several relevant knockout mouse models.
Subject: NCMLS 1: Immunity, infection and tissue repair
NCMLS 2: Metabolism, transport and motion
UMCN 5.4: Renal disorders
Organization: Physiology
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/70107

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