Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5

Hypercalciuria is a major cause of nephrolithiasis, and is a common and complex disorder involving genetic and environmental factors. Identification of genetic factors for monogenic forms of hypercalciuria is hampered by the limited availability of large families, and to facilitate such studies, we...

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Autores principales: Loh, Nellie Y., Bentley, Liz, Dimke, Henrik, Verkaart, Sjoerd, Tammaro, Paolo, Gorvin, Caroline M., Stechman, Michael J., Ahmad, Bushra N., Hannan, Fadil M., Piret, Sian E., Evans, Holly, Bellantuono, Ilaria, Hough, Tertius A., Fraser, William D., Hoenderop, Joost G. J., Ashcroft, Frances M., Brown, Steve D. M., Bindels, René J. M., Cox, Roger D., Thakker, Rajesh V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3559602/
https://www.ncbi.nlm.nih.gov/pubmed/23383183
http://dx.doi.org/10.1371/journal.pone.0055412
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author Loh, Nellie Y.
Bentley, Liz
Dimke, Henrik
Verkaart, Sjoerd
Tammaro, Paolo
Gorvin, Caroline M.
Stechman, Michael J.
Ahmad, Bushra N.
Hannan, Fadil M.
Piret, Sian E.
Evans, Holly
Bellantuono, Ilaria
Hough, Tertius A.
Fraser, William D.
Hoenderop, Joost G. J.
Ashcroft, Frances M.
Brown, Steve D. M.
Bindels, René J. M.
Cox, Roger D.
Thakker, Rajesh V.
author_facet Loh, Nellie Y.
Bentley, Liz
Dimke, Henrik
Verkaart, Sjoerd
Tammaro, Paolo
Gorvin, Caroline M.
Stechman, Michael J.
Ahmad, Bushra N.
Hannan, Fadil M.
Piret, Sian E.
Evans, Holly
Bellantuono, Ilaria
Hough, Tertius A.
Fraser, William D.
Hoenderop, Joost G. J.
Ashcroft, Frances M.
Brown, Steve D. M.
Bindels, René J. M.
Cox, Roger D.
Thakker, Rajesh V.
author_sort Loh, Nellie Y.
collection PubMed
description Hypercalciuria is a major cause of nephrolithiasis, and is a common and complex disorder involving genetic and environmental factors. Identification of genetic factors for monogenic forms of hypercalciuria is hampered by the limited availability of large families, and to facilitate such studies, we screened for hypercalciuria in mice from an N-ethyl-N-nitrosourea mutagenesis programme. We identified a mouse with autosomal dominant hypercalciuria (HCALC1). Linkage studies mapped the Hcalc1 locus to a 11.94 Mb region on chromosome 6 containing the transient receptor potential cation channel, subfamily V, members 5 (Trpv5) and 6 (Trpv6) genes. DNA sequence analysis of coding regions, intron-exon boundaries and promoters of Trpv5 and Trpv6 identified a novel T to C transition in codon 682 of TRPV5, mutating a conserved serine to a proline (S682P). Compared to wild-type littermates, heterozygous (Trpv5 (682P/+)) and homozygous (Trpv5 (682P/682P)) mutant mice had hypercalciuria, polyuria, hyperphosphaturia and a more acidic urine, and ∼10% of males developed tubulointerstitial nephritis. Trpv5 (682P/682P) mice also had normal plasma parathyroid hormone but increased 1,25-dihydroxyvitamin D(3) concentrations without increased bone resorption, consistent with a renal defect for the hypercalciuria. Expression of the S682P mutation in human embryonic kidney cells revealed that TRPV5-S682P-expressing cells had a lower baseline intracellular calcium concentration than wild-type TRPV5-expressing cells, suggesting an altered calcium permeability. Immunohistological studies revealed a selective decrease in TRPV5-expression from the renal distal convoluted tubules of Trpv5 (682P/+) and Trpv5 (682P/682P) mice consistent with a trafficking defect. In addition, Trpv5(682P/682P) mice had a reduction in renal expression of the intracellular calcium-binding protein, calbindin-D(28K), consistent with a specific defect in TRPV5-mediated renal calcium reabsorption. Thus, our findings indicate that the TRPV5 S682P mutant is functionally significant and study of HCALC1, a novel model for autosomal dominant hypercalciuria, may help further our understanding of renal calcium reabsorption and hypercalciuria.
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spelling pubmed-35596022013-02-04 Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5 Loh, Nellie Y. Bentley, Liz Dimke, Henrik Verkaart, Sjoerd Tammaro, Paolo Gorvin, Caroline M. Stechman, Michael J. Ahmad, Bushra N. Hannan, Fadil M. Piret, Sian E. Evans, Holly Bellantuono, Ilaria Hough, Tertius A. Fraser, William D. Hoenderop, Joost G. J. Ashcroft, Frances M. Brown, Steve D. M. Bindels, René J. M. Cox, Roger D. Thakker, Rajesh V. PLoS One Research Article Hypercalciuria is a major cause of nephrolithiasis, and is a common and complex disorder involving genetic and environmental factors. Identification of genetic factors for monogenic forms of hypercalciuria is hampered by the limited availability of large families, and to facilitate such studies, we screened for hypercalciuria in mice from an N-ethyl-N-nitrosourea mutagenesis programme. We identified a mouse with autosomal dominant hypercalciuria (HCALC1). Linkage studies mapped the Hcalc1 locus to a 11.94 Mb region on chromosome 6 containing the transient receptor potential cation channel, subfamily V, members 5 (Trpv5) and 6 (Trpv6) genes. DNA sequence analysis of coding regions, intron-exon boundaries and promoters of Trpv5 and Trpv6 identified a novel T to C transition in codon 682 of TRPV5, mutating a conserved serine to a proline (S682P). Compared to wild-type littermates, heterozygous (Trpv5 (682P/+)) and homozygous (Trpv5 (682P/682P)) mutant mice had hypercalciuria, polyuria, hyperphosphaturia and a more acidic urine, and ∼10% of males developed tubulointerstitial nephritis. Trpv5 (682P/682P) mice also had normal plasma parathyroid hormone but increased 1,25-dihydroxyvitamin D(3) concentrations without increased bone resorption, consistent with a renal defect for the hypercalciuria. Expression of the S682P mutation in human embryonic kidney cells revealed that TRPV5-S682P-expressing cells had a lower baseline intracellular calcium concentration than wild-type TRPV5-expressing cells, suggesting an altered calcium permeability. Immunohistological studies revealed a selective decrease in TRPV5-expression from the renal distal convoluted tubules of Trpv5 (682P/+) and Trpv5 (682P/682P) mice consistent with a trafficking defect. In addition, Trpv5(682P/682P) mice had a reduction in renal expression of the intracellular calcium-binding protein, calbindin-D(28K), consistent with a specific defect in TRPV5-mediated renal calcium reabsorption. Thus, our findings indicate that the TRPV5 S682P mutant is functionally significant and study of HCALC1, a novel model for autosomal dominant hypercalciuria, may help further our understanding of renal calcium reabsorption and hypercalciuria. Public Library of Science 2013-01-30 /pmc/articles/PMC3559602/ /pubmed/23383183 http://dx.doi.org/10.1371/journal.pone.0055412 Text en © 2013 Loh et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Loh, Nellie Y.
Bentley, Liz
Dimke, Henrik
Verkaart, Sjoerd
Tammaro, Paolo
Gorvin, Caroline M.
Stechman, Michael J.
Ahmad, Bushra N.
Hannan, Fadil M.
Piret, Sian E.
Evans, Holly
Bellantuono, Ilaria
Hough, Tertius A.
Fraser, William D.
Hoenderop, Joost G. J.
Ashcroft, Frances M.
Brown, Steve D. M.
Bindels, René J. M.
Cox, Roger D.
Thakker, Rajesh V.
Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title_full Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title_fullStr Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title_full_unstemmed Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title_short Autosomal Dominant Hypercalciuria in a Mouse Model Due to a Mutation of the Epithelial Calcium Channel, TRPV5
title_sort autosomal dominant hypercalciuria in a mouse model due to a mutation of the epithelial calcium channel, trpv5
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3559602/
https://www.ncbi.nlm.nih.gov/pubmed/23383183
http://dx.doi.org/10.1371/journal.pone.0055412
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