Gene/Protein Disease Symptom Drug Enzyme Compound
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Query: UMLS:C0020438 (hypercalciuria)
 2,502 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

Dent's disease, a renal tubular disorder characterized by low-molecular-weight proteinuria (LMWP), hypercalciuria, and nephrolithiasis, is due to inactivating mutations in the x-linked renal specific chloride channel CLC-5. CLC-5 belongs to the family of voltage-gated chloride channels, which function as homodimeric proteins with each subunit consisting of 18 helices and a chloride selectivity filter, i.e. pore. None of the 15 CLC-5 missense mutations reported in patients with dent's disease involves the chloride selectivity filter, but 12 of these are clustered around the interface of the two subunits, thereby emphasising the important role for the interaction between the two subunits at the interface of the homodimeric CLC-5. In the kidney, CLC-5 forms part of the receptor-mediated endocytic pathway, and defects in this pathway due to a loss of CLC-5 function, may help to account for the LMWP, hyperphosphaturia, hypercalciuria and nephrolithiasis. The molecular studies and the generation of mouse models of the disease have increased our understanding of the renal tubular mechanisms that regulate mineral homeostasis.
Bull Mem Acad R Med Belg 2004
PMID:Dent's disease--a nephrolithiasis disorder associated with defective receptor-mediated endocytosis. 1561 94

Dent's disease is an hereditary renal tubular disorder characterized by low-molecular-weight (LMW) proteinuria, hypercalciuria and nephrolithiasis. The disease is due to mutations of CLC-5, a member of the family of voltage-gated CLC chloride channels. CLC-5 is distributed in cells lining the proximal tubule (PT) of the kidney, where it co-localizes with albumin-containing endocytic vesicles that form part of the receptor-mediated endocytic pathway that mediates the reabsorption of low-molecular-weight (LMW) proteins filtered at the glomerular level. Since progression along the endocytic apparatus requires endosomal acidification, it has been suggested that dysfunction of CLC-5 in endosomes may lead to inefficient reabsorption of LMW proteins and dysfunction of PT cells. Investigations conducted in a CLC-5 knockout (KO) mouse model harbouring all the characteristic renal tubular defects of Dent's disease showed a severe impairment of endocytosis by PT cells, such that the endocytic tracer peroxidase was poorly transferred into early endocytic vesicles. These data demonstrated that an impairment of receptor-mediated endocytosis in PT cells is the basis for the defective uptake of LMW proteins in patients with Dent's disease. The endocytosis and processing of LMW proteins involves the multiligand tandem receptors, megalin and cubilin, that are abundantly expressed at the brush border of PT cells. The characterization of the endocytic defect in CLC-5 KO mice revealed that ligands of both megalin and cubilin were affected, whereas a decrease in total kidney content of megalin and cubilin at the protein level was detected. Using analytical subcellular fractionation and quantitative immunogold labelling, we demonstrated a selective disappearance of megalin and cubilin at the brush border of PT cells. These observations allowed us to conclude that defective protein endocytosis linked to CLC-5 inactivation is due to a major and selective loss of megalin and cubilin at the brush border, reflecting a trafficking defect in renal PT cells. These results improve our understanding of Dent's disease, taken as a paradigm for renal Fanconi syndrome and nephrolithiasis, and demonstrate multiple roles for CLC-5 in the kidney. These studies also provided insights in important functions such as apical endocytosis, handling of proteins by renal tubular cells, calcium metabolism, and urinary acidification.
Bull Mem Acad R Med Belg 2004
PMID:Chloride channels and endocytosis: new insights from Dent's disease and CLC-5 knockout mice. 1561 95