Literature DB >> 18337544

Calcium oxalate crystal deposition in kidneys of hypercalciuric mice with disrupted type IIa sodium-phosphate cotransporter.

Saeed R Khan1, Patricia A Glenton.   

Abstract

The most common theories about the pathogenesis of idiopathic kidney stones consider precipitation of calcium phosphate (CaP) within the kidneys critical for the development of the disease. We decided to test the hypothesis that a CaP substrate can promote the deposition of calcium oxalate (CaOx) in the kidneys. Experimental hyperoxaluria was induced by feeding glyoxylate to male mice with knockout (KO) of NaP(i) IIa (Npt2a), a sodium-phosphate cotransporter. Npt2a KO mice are hypercalciuric and produce CaP deposits in their renal tubules. Experimental hyperoxaluria led to CaOx crystalluria in both the hypercalciuric KO mice and the normocalciuric control B6 mice. Only the KO mice produced CaOx crystal deposits in their kidneys, but the CaOx crystals deposited separately from the CaP deposits. Perhaps CaP deposits were not available for a CaOx overgrowth. These results also validate earlier animal model observations that showed that CaP substrate is not required for renal deposition of CaOx and that other factors, such as local supersaturation, may be involved. The absence of CaOx deposition in the B6 mice despite extreme hyperoxaluria also signifies the importance of both calcium and oxalate in the development of CaOx nephrolithiasis.

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Year:  2008        PMID: 18337544      PMCID: PMC3625965          DOI: 10.1152/ajprenal.00620.2007

Source DB:  PubMed          Journal:  Am J Physiol Renal Physiol        ISSN: 1522-1466


  25 in total

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6.  Calcium oxalate crystal localization and osteopontin immunostaining in genetic hypercalciuric stone-forming rats.

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10.  Deposition of calcium phosphate and calcium oxalate crystals in the kidneys.

Authors:  S R Khan; P A Glenton
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  21 in total

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Review 4.  Histological aspects of the "fixed-particle" model of stone formation: animal studies.

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5.  Simplified estimates of ion-activity products of calcium oxalate and calcium phosphate in mouse urine.

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7.  Unified theory on the pathogenesis of Randall's plaques and plugs.

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Authors:  Saeed R Khan; Benjamin K Canales
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Review 9.  Interstitial calcinosis in renal papillae of genetically engineered mouse models: relation to Randall's plaques.

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Journal:  Urolithiasis       Date:  2014-08-06       Impact factor: 3.436

10.  The kidney sodium-phosphate co-transporter alters bone quality in an age and gender specific manner.

Authors:  Adele L Boskey; Lyudmilla Lukashova; Lyudmila Spevak; Yan Ma; Saeed R Khan
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