| Literature DB >> 32149733 |
Joshua N Curry1,2, Matthew Saurette3,4, Masomeh Askari5, Lei Pei6, Michael B Filla2,6, Megan R Beggs3,4, Peter Sn Rowe2,6, Timothy Fields7, Andre J Sommer8, Chizu Tanikawa9, Yoichiro Kamatani10, Andrew P Evan11, Mehdi Totonchi5,12, R Todd Alexander4,13, Koichi Matsuda9,14, Alan Sl Yu1,2,6.
Abstract
The major risk factor for kidney stone disease is idiopathic hypercalciuria. Recent evidence implicates a role for defective calcium reabsorption in the renal proximal tubule. We hypothesized that claudin-2, a paracellular cation channel protein, mediates proximal tubule calcium reabsorption. We found that claudin-2-null mice have hypercalciuria due to a primary defect in renal tubule calcium transport and papillary nephrocalcinosis that resembles the intratubular plugs in kidney stone formers. Our findings suggest that a proximal tubule defect in calcium reabsorption predisposes to papillary calcification, providing support for the vas washdown hypothesis. Claudin-2-null mice were also found to have increased net intestinal calcium absorption, but reduced paracellular calcium permeability in the colon, suggesting that this was due to reduced intestinal calcium secretion. Common genetic variants in the claudin-2 gene were associated with decreased tissue expression of claudin-2 and increased risk of kidney stones in 2 large population-based studies. Finally, we describe a family in which males with a rare missense variant in claudin-2 have marked hypercalciuria and kidney stone disease. Our findings indicate that claudin-2 is a key regulator of calcium excretion and a potential target for therapies to prevent kidney stones.Entities:
Keywords: Calcium; Cell Biology; Epithelial transport of ions and water; Nephrology; Transport
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Year: 2020 PMID: 32149733 PMCID: PMC7108907 DOI: 10.1172/JCI127750
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808