Your search keyword '"Hypercalciuria genetics"' showing total 30 results

1. Clinical and genetic characteristics of Dent's disease type 1 in Europe.

Author

Burballa C, Cantero-Recasens G, Prikhodina L, Lugani F, Schlingmann K, Ananin PV, Besouw M, Bockenhauer D, Madariaga L, Bertholet-Thomas A, Taroni F, Parolin M, Conlon P, Emma F, Del Prete D, Chauveau D, Koster-Kamphuis L, Fila M, Pasini A, Castro I, Colussi G, Gil M, Mohidin B, Wlodkowski T, Schaefer F, and Ariceta G

Subjects

Male, Humans, Hypercalciuria epidemiology, Hypercalciuria genetics, Mutation, Europe epidemiology, Proteinuria genetics, Chloride Channels genetics, Nephrocalcinosis etiology, Nephrocalcinosis genetics, Dent Disease diagnosis, Dent Disease genetics, Kidney Calculi, Renal Insufficiency, Renal Insufficiency, Chronic etiology, Renal Insufficiency, Chronic genetics

Abstract

Background: Dent's disease type 1 (DD1) is a rare X-linked nephropathy caused by CLCN5 mutations, characterized by proximal tubule dysfunction, including low molecular weight proteinuria (LMWP), hypercalciuria, nephrolithiasis-nephrocalcinosis, progressive chronic kidney disease (CKD) and kidney failure (KF). Current management is symptomatic and does not prevent disease progression. Here we describe the contemporary DD1 picture across Europe to highlight its unmet needs., Methods: A physician-based anonymous international e-survey supported by several European nephrology networks/societies was conducted. Questions focused on DD1 clinical features, diagnostic procedure and mutation spectra., Results: A total of 207 DD1 male patients were reported; clinical data were available for 163 with confirmed CLCN5 mutations. Proteinuria was the most common manifestation (49.1%). During follow-up, all patients showed LMWP, 66.4% nephrocalcinosis, 44.4% hypercalciuria and 26.4% nephrolithiasis. After 5.5 years, ≈50% of patients presented with renal dysfunction, 20.7% developed CKD stage ≥3 and 11.1% developed KF. At the last visit, hypercalciuria was more frequent in paediatric patients than in adults (73.4% versus 19.0%). Conversely, nephrolithiasis, nephrocalcinosis and renal dysfunction were more prominent in adults. Furthermore, CKD progressed with age. Despite no clear phenotype/genotype correlation, decreased glomerular filtration rate was more frequent in subjects with CLCN5 mutations affecting the pore or CBS domains compared with those with early-stop mutations., Conclusions: Results from this large DD1 cohort confirm previous findings and provide new insights regarding age and genotype impact on CKD progression. Our data strongly support that DD1 should be considered in male patients with CKD, nephrocalcinosis/hypercalciuria and non-nephrotic proteinuria and provide additional support for new research opportunities., (© The Author(s) 2022. Published by Oxford University Press on behalf of the ERA.)

Published

2023

2. Hypocalcemia as the Initial Presentation of Type 2 Bartter Syndrome: A Family Report.

Author

London S, Levine MA, Li D, Spiegel R, Lebel A, Halevy R, and Tenenbaum-Rakover Y

Subjects

Child, Child, Preschool, Female, Humans, Hypercalciuria diagnosis, Hypercalciuria genetics, Male, Phosphates, Pregnancy, Alkalosis complications, Bartter Syndrome complications, Bartter Syndrome diagnosis, Bartter Syndrome genetics, Hypocalcemia etiology, Hypocalcemia genetics, Vitamin D Deficiency complications

Abstract

Context: Bartter syndrome (BS) is a group of rare autosomal-recessive tubulopathies characterized by hypokalemic, hypochloremic metabolic alkalosis in which the primary defect is a deficiency of transporters involved in sodium chloride reabsorption. Type 2 BS results from a defect in the renal outer medullary potassium channel encoded by the KCNJ1 gene. Type 2 BS presents with polyhydramnios, intrauterine growth retardation, prematurity, failure to thrive, polyuria, hypercalciuria, and life-threatening episodes of dehydration. Hypocalcemia is a very rare presenting symptom of BS, with only a few published cases reporting it as the initial manifestation of type 2 BS., Objective: To describe a child who presented with hypocalcemic seizure at the age of 2.3 years that was first related to vitamin D deficiency and high-phosphate soft drink consumption., Methods: Whole exome sequencing (WES) was used to evaluate the biochemical abnormalities of the proband., Results: We identified a previously described homozygous missense mutation c.212C>T, p.T71M in the KCNJ1 gene associated with type 2 BS. Six additional family members with the same mutation and diagnosed clinically with BS are also reported, 2 presenting with hypocalcemia associated with vitamin D deficiency., Conclusion: This report expands the clinical spectrum associated with KCNJ1 mutations and emphasizes the role of WES in unsolved cases of hypocalcemia when genetic disease is suspected. It also highlights the hazardous effects of phosphate-containing soft drinks on calcium metabolism., (© The Author(s) 2021. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2022

3. The Calcium-Sensing Receptor Is Essential for Calcium and Bicarbonate Sensitivity in Human Spermatozoa.

Author

Boisen IM, Rehfeld A, Mos I, Poulsen NN, Nielsen JE, Schwarz P, Rejnmark L, Dissing S, Bach-Mortensen P, Juul A, Bräuner-Osborne H, Lanske B, and Blomberg Jensen M

Subjects

Acrosome Reaction drug effects, Acrosome Reaction genetics, Adult, Bicarbonates pharmacology, Calcium pharmacology, Calcium Signaling drug effects, Calcium Signaling genetics, Case-Control Studies, Female, Humans, Hypercalcemia congenital, Hypercalcemia genetics, Hypercalcemia metabolism, Hypercalcemia pathology, Hypercalciuria genetics, Hypercalciuria metabolism, Hypercalciuria pathology, Hypocalcemia genetics, Hypocalcemia metabolism, Hypocalcemia pathology, Hypoparathyroidism congenital, Hypoparathyroidism genetics, Hypoparathyroidism metabolism, Hypoparathyroidism pathology, Kidney metabolism, Kidney pathology, Magnesium metabolism, Magnesium pharmacology, Male, Mutation, Receptors, Calcium-Sensing genetics, Sperm Motility drug effects, Sperm Motility genetics, Spermatozoa drug effects, Spermatozoa physiology, Testicular Neoplasms genetics, Testicular Neoplasms metabolism, Testicular Neoplasms pathology, Bicarbonates metabolism, Calcium metabolism, Receptors, Calcium-Sensing physiology, Spermatozoa metabolism

Abstract

Context: The calcium-sensing receptor (CaSR) is essential to maintain a stable calcium concentration in serum. Spermatozoa are exposed to immense changes in concentrations of CaSR ligands such as calcium, magnesium, and spermine during epididymal maturation, in the ejaculate, and in the female reproductive environment. However, the role of CaSR in human spermatozoa is unknown., Objective: This work aimed to investigate the role of CaSR in human spermatozoa., Methods: We identified CaSR in human spermatozoa and characterized the response to CaSR agonists on intracellular calcium, acrosome reaction, and 3',5'-cyclic adenosine 5'-monophosphate (cAMP) in spermatozoa from men with either loss-of-function or gain-of-function mutations in CASR and healthy donors., Results: CaSR is expressed in human spermatozoa and is essential for sensing extracellular free ionized calcium (Ca2+) and Mg2+. Activators of CaSR augmented the effect of sperm-activating signals such as the response to HCO3- and the acrosome reaction, whereas spermatozoa from men with a loss-of-function mutation in CASR had a diminished response to HCO3-, lower progesterone-mediated calcium influx, and were less likely to undergo the acrosome reaction in response to progesterone or Ca2+. CaSR activation increased cAMP through soluble adenylyl cyclase (sAC) activity and increased calcium influx through CatSper. Moreover, external Ca2+ or Mg2+ was indispensable for HCO3- activation of sAC. Two male patients with a CASR loss-of-function mutation in exon 3 presented with normal sperm counts and motility, whereas a patient with a loss-of-function mutation in exon 7 had low sperm count, motility, and morphology., Conclusion: CaSR is important for the sensing of Ca2+, Mg2+, and HCO3- in spermatozoa, and loss-of-function may impair male sperm function., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2021

4. Do the Heterozygous Carriers of a CYP24A1 Mutation Display a Different Biochemical Phenotype Than Wild Types?

Author

Brancatella A, Cappellani D, Kaufmann M, Borsari S, Piaggi P, Baldinotti F, Caligo MA, Jones G, Marcocci C, and Cetani F

Subjects

Adult, Biological Variation, Population, Biomarkers blood, Case-Control Studies, Codon, Nonsense, Family, Fibroblast Growth Factor-23, Fibroblast Growth Factors blood, Genotype, Heterozygote, Homozygote, Humans, Hypercalcemia pathology, Hypercalciuria blood, Hypercalciuria genetics, Hypercalciuria pathology, Male, Nephrocalcinosis blood, Nephrocalcinosis genetics, Nephrocalcinosis pathology, Pedigree, Phenotype, Vitamin D blood, Hypercalcemia blood, Hypercalcemia genetics, Vitamin D3 24-Hydroxylase genetics

Abstract

Context: Human cytochrome P450 24 subfamily A member 1 (CYP24A1) loss-of-function mutations result in impaired activity of the 24-hydroxylase involved in vitamin D catabolism, thus inducing a vitamin D-dependent hypercalcemia. Homozygotes often present an overt clinical phenotype named idiopathic infantile hypercalcemia (IIH), whereas it is debated whether heterozygotes display an abnormal phenotype., Objective: To compare the clinical and biochemical features of heterozygous carriers of CYP24A1 variant and healthy wild-type controls sharing the same genetic and environmental exposure., Methods: A large family harboring the nonsense c.667A>T, p.Arg223* pathogenic variant in the CYP24A1 gene was evaluated. All subjects underwent clinical and biochemical evaluation and complete analysis of vitamin D metabolites using mass spectroscopy including 1,24,25(OH)3D3. Subjects were divided into 2 groups according to their genotype: heterozygotes and wild-type for the CYP24A1 variant., Results: The proband, a 40-year-old man, homozygous for p.Arg223* pathogenic variant, had a history of mild hypercalcemia with a seasonal trend, recurrent nephrolithiasis, and no episodes of acute hypercalcemia. He showed the highest serum levels of fibroblast growth factor 23, the highest 25(OH)D3/24,25(OH)2D3 ratio and undetectable levels of 1,24,25(OH)3D3, which represent indicators of a loss-of-function CYP24A1. Compared with the wild-types, heterozygotes had higher serum calcium and 25(OH)D3 concentrations (P = .017 and P = .025, respectively), without any difference in the other biochemical parameters and in the rate of nephrolithiasis., Conclusion: Heterozygotes exhibit a biochemical phenotype different from that of wild-type subjects. In clinical practice, these individuals might require surveillance because of the potential risk of developing hypercalcemia and related clinical manifestations if exposed to triggering factors., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2021

5. Digenic Heterozygous Mutations in SLC34A3 and SLC34A1 Cause Dominant Hypophosphatemic Rickets with Hypercalciuria.

Author

Gordon RJ, Li D, Doyle D, Zaritsky J, and Levine MA

Subjects

Adolescent, Adult, Aged, Female, Heterozygote, Humans, Male, Middle Aged, Mutation, Pedigree, Prospective Studies, Retrospective Studies, Young Adult, Hypercalciuria genetics, Rickets, Hypophosphatemic genetics, Sodium-Phosphate Cotransporter Proteins, Type IIa genetics, Sodium-Phosphate Cotransporter Proteins, Type IIc genetics

Abstract

Context: Hypophosphatemia and metabolic bone disease are associated with hereditary hypophosphatemic rickets with hypercalciuria (HHRH) due to biallelic mutations of SLC34A3 encoding the NPT2C sodium-phosphate cotransporter and nephrolithiasis/osteoporosis, hypophosphatemic 1 (NPHLOP1) due to monoallelic mutations in SLC34A1 encoding the NPT2A sodium-phosphate cotransporter., Objective: To identify a genetic cause of apparent dominant transmission of HHRH., Design and Setting: Retrospective and prospective analysis of clinical and molecular characteristics of patients studied in 2 academic medical centers., Methods: We recruited 4 affected and 3 unaffected members of a 4-generation family in which the proband presented with apparent HHRH. We performed clinical examinations, biochemical and radiological analyses, and molecular studies of genomic DNA., Results: The proband and her affected sister and mother carried pathogenic heterozygous mutations in 2 related genes, SLC34A1 (exon 13, c.1535G>A; p.R512H) and SLC34A3 (exon 13, c.1561dupC; L521Pfs*72). The proband and her affected sister inherited both gene mutations from their mother, while their clinically less affected brother, father, and paternal grandmother carried only the SLC34A3 mutation. Renal phosphate-wasting exhibited both a gene dosage-effect and an age-dependent attenuation of severity., Conclusions: We describe a kindred with autosomal dominant hypophosphatemic rickets in which whole exome analysis identified digenic heterozygous mutations in SLC34A1 and SLC34A3. Subjects with both mutations were more severely affected than subjects carrying only one mutation. These findings highlight the challenges of assigning causality to plausible genetic variants in the next generation sequencing era., (© Endocrine Society 2020. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2020

6. Activating Mutations of the G-protein Subunit α 11 Interdomain Interface Cause Autosomal Dominant Hypocalcemia Type 2.

Author

Gorvin CM, Stokes VJ, Boon H, Cranston T, Glück AK, Bahl S, Homfray T, Aung T, Shine B, Lines KE, Hannan FM, and Thakker RV

Subjects

Adult, Child, Female, HEK293 Cells, Humans, Hypoparathyroidism genetics, Male, Pedigree, GTP-Binding Protein alpha Subunits, Gq-G11 genetics, Gain of Function Mutation genetics, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital, Receptors, Calcium-Sensing genetics

Abstract

Context: Autosomal dominant hypocalcemia types 1 and 2 (ADH1 and ADH2) are caused by germline gain-of-function mutations of the calcium-sensing receptor (CaSR) and its signaling partner, the G-protein subunit α 11 (Gα 11), respectively. More than 70 different gain-of-function CaSR mutations, but only 6 different gain-of-function Gα 11 mutations are reported to date., Methods: We ascertained 2 additional ADH families and investigated them for CaSR and Gα 11 mutations. The effects of identified variants on CaSR signaling were evaluated by transiently transfecting wild-type (WT) and variant expression constructs into HEK293 cells stably expressing CaSR (HEK-CaSR), and measuring intracellular calcium (Ca2+i) and MAPK responses following stimulation with extracellular calcium (Ca2+e)., Results: CaSR variants were not found, but 2 novel heterozygous germline Gα 11 variants, p.Gly66Ser and p.Arg149His, were identified. Homology modeling of these revealed that the Gly66 and Arg149 residues are located at the interface between the Gα 11 helical and GTPase domains, which is involved in guanine nucleotide binding, and this is the site of 3 other reported ADH2 mutations. The Ca2+i and MAPK responses of cells expressing the variant Ser66 or His149 Gα 11 proteins were similar to WT cells at low Ca2+e, but significantly increased in a dose-dependent manner following Ca2+e stimulation, thereby indicating that the p.Gly66Ser and p.Arg149His variants represent pathogenic gain-of-function Gα 11 mutations. Treatment of Ser66- and His149-Gα 11 expressing cells with the CaSR negative allosteric modulator NPS 2143 normalized Ca2+i and MAPK responses., Conclusion: Two novel ADH2-causing mutations that highlight the Gα 11 interdomain interface as a hotspot for gain-of-function Gα 11 mutations have been identified., (© Endocrine Society 2019.)

Published

2020

7. ADCY10 frameshift variant leading to severe recessive asthenozoospermia and segregating with absorptive hypercalciuria.

Author

Akbari A, Pipitone GB, Anvar Z, Jaafarinia M, Ferrari M, Carrera P, and Totonchi M

Subjects

Adult, Asthenozoospermia diagnosis, Calcium urine, Consanguinity, Cyclic CMP analogs & derivatives, Cyclic CMP pharmacology, DNA Mutational Analysis, Frameshift Mutation, Homozygote, Humans, Hypercalciuria diagnosis, Hypercalciuria urine, Iran, Karyotyping, Kidney Calculi diagnosis, Kidney Calculi urine, Male, Pedigree, Sperm Motility drug effects, Sperm Motility genetics, Treatment Outcome, Adenylyl Cyclases genetics, Asthenozoospermia genetics, Hypercalciuria genetics, Kidney Calculi genetics

Abstract

Study Question: Can whole exome sequencing (WES) reveal a novel pathogenic variant in asthenozoospermia in a multiplex family including multiple patients?, Summary Answer: Patients were discovered to be homozygous for a rare 2-bp deletion in the ADCY10 coding region (c.1205_1206del, rs779944215)., What Is Known Already: ADCY10 encodes for soluble adenylyl cyclase (sAC), which is the predominant adenylate cyclase in sperm. It is already established that proper sAC activity and a constant supply of cAMP are crucial to sperm motility regulation, and knockout mouse models have been reported as severely asthenozoospermic. ADCY10 is a susceptibility gene for dominant absorptive hypercalciuria (OMIM#143870); however, no ADCY10 variations have been confirmed to cause human asthenozoospermia to date., Study Design, Size, Duration: This was a retrospective genetics study of a highly consanguineous pedigree of asthenozoospermia. The subject family was recruited in Iran in 2016., Participants/materials, Setting, Methods: The two patients were diagnosed as asthenozoospermic through careful clinical investigations. Both patients, respective parents, and an unaffected brother were subjected to WES. The discovered variant was validated by Sanger sequencing and segregated with the phenotype. To confirm the pathogenicity of the variant, sperm samples from both patients, 10 normozoospermic men and 10 asthenozoospermic patients not representing the variation, were treated with a cAMP analogue dissolved in human tubal fluid medium, followed by computer-assisted sperm analysis and statistical analyses., Main Results and the Role of Chance: The discovered homozygous variant occurs at 10 amino acids upstream of the ADCY10 nucleotide binding site leading to a premature termination (p.His402Argfs*41). Treatment of the patients' sperm samples with a cell-permeable cAMP analogue resulted in a significant increase in sperm motility, indicating the pathogenic role of the variant. Moreover, absorptive hypercalciuria, segregating within the family, was also associated with the same variant following a dominant inheritance., Limitations, Reasons for Caution: Though nonsense-mediated decay is highly likely to occur in the mutated transcripts, we were not able to confirm this due to low RNA levels in mature sperm., Wider Implications of the Findings: Our finding enlarges the phenotypic spectrum associated with the ADCY10 gene, previously described as a susceptibility gene for dominant absorptive hypercalciuria., Study Funding/competing Interest(s): This study was supported by grants from the Royan Institute, Tehran, Iran, and San Raffaele Hospital, Milan, Italy. The authors have no conflict of interest., Trial Registration Number: N/A., (© The Author(s) 2019. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2019

8. Novel mutations associated with inherited human calcium-sensing receptor disorders: A clinical genetic study.

Author

García-Castaño A, Madariaga L, Pérez de Nanclares G, Ariceta G, Gaztambide S, and Castaño L

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, DNA Mutational Analysis, Female, Humans, Infant, Newborn, Male, Middle Aged, Plant Extracts, Hypercalcemia genetics, Hypercalciuria genetics, Hypocalcemia genetics, Mutation, Polymorphism, Genetic, Receptors, Calcium-Sensing genetics

Abstract

Objective Molecular diagnosis is a useful diagnostic tool in calcium metabolism disorders. The calcium-sensing receptor (CaSR) is known to play a central role in the regulation of extracellular calcium homeostasis. We performed clinical, biochemical and genetic characterization of sequence anomalies in this receptor in a cohort of 130 individuals from 82 families with suspected alterations in the CASR gene, one of the largest series described. Methods The CASR gene was screened for mutations by polymerase chain reaction followed by direct Sanger sequencing. Results Presumed CaSR-inactivating mutations were found in 65 patients from 26 families. These patients had hypercalcemia (median: 11.3 mg/dL) but normal or abnormally high parathyroid hormone (PTH) levels (median: 52 pg/mL). On the other hand, presumed CaSR-activating mutations were detected in 17 patients from eight families. These patients had a median serum calcium level of 7.4 mg/dL and hypoparathyroidism (median: PTH 13 pg/mL). Further, common polymorphisms previously associated with high blood ionized calcium levels were found in 27 patients (median calcium: 10.6 mg/dL; median PTH: 65 pg/mL) with no other alterations in CASR. Overall, we found 30 different mutations, of which, 14 have not been previously reported (p.Ala26Ser, p.Cys60Arg, p.Lys119Ile, p.Leu123Met, p.Glu133Val, p.Gly222Glu, p.Phe351Ile, p.Cys542Tyr, p.Cys546Gly, p.Cys677Tyr, p.Ile816Val, p.Ala887Asp, p.Glu934*, p.Pro935_Gln945dup). Conclusions Patients with CASR mutations may not fit the classic clinical pictures of hypercalcemia with hypocalciuria or hypocalcemia with hypercalciuria. Molecular studies are important for confirming the diagnosis and distinguishing it from other entities. Our genetic analysis confirmed CaSR disorders in 82 patients in the study cohort.

Published

2019

9. Heterozygous Mutations in TBX1 as a Cause of Isolated Hypoparathyroidism.

Author

Li D, Gordon CT, Oufadem M, Amiel J, Kanwar HS, Bakay M, Wang T, Hakonarson H, and Levine MA

Subjects

Aged, DiGeorge Syndrome blood, DiGeorge Syndrome diagnosis, Exons genetics, Female, Heterozygote, Humans, Hypercalciuria blood, Hypercalciuria diagnosis, Hypocalcemia blood, Hypocalcemia diagnosis, Hypoparathyroidism blood, Hypoparathyroidism diagnosis, Hypoparathyroidism genetics, Infant, Male, Mutation, Pedigree, Penetrance, RNA Splice Sites genetics, Exome Sequencing, DiGeorge Syndrome genetics, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital, T-Box Domain Proteins genetics

Abstract

Context: Most cases of autosomal dominant isolated hypoparathyroidism are caused by gain-of-function mutations in CASR or GNA11 or dominant negative mutations in GCM2 or PTH., Objective: To identify the genetic etiology for dominantly transmitted isolated hypoparathyroidism in two multigenerational families with 14 affected family members., Methods: We performed whole exome sequencing of DNA from two families and examined the consequences of mutations by minigene splicing assay., Results: We discovered disease-causing mutations in both families. A splice-altering mutation in TBX1 (c.1009+1G>C) leading to skipping of exon 8 (101 bp) was identified in 10 affected family members and five unaffected subjects of family A, indicating reduced penetrance for this point mutation. In a second family from France (family B), we identified another splice-altering mutation (c.1009+2T>C) adjacent to the mutation identified in family A that results in skipping of the same exon; two subjects in family B had isolated hypoparathyroidism, whereas a third subject manifested the clinical triad of the 22q11.2 deletion syndrome, indicative of variable expressivity., Conclusions: We report evidence that heterozygous TBX1 mutations can cause isolated hypoparathyroidism. This study adds knowledge to the increasingly expanding list of causative and candidate genes in isolated hypoparathyroidism.

Published

2018

10. Long-term renal outcome in children with OCRL mutations: retrospective analysis of a large international cohort.

Author

Zaniew M, Bökenkamp A, Kolbuc M, La Scola C, Baronio F, Niemirska A, Szczepanska M, Bürger J, La Manna A, Miklaszewska M, Rogowska-Kalisz A, Gellermann J, Zampetoglou A, Wasilewska A, Roszak M, Moczko J, Krzemien A, Runowski D, Siten G, Zaluska-Lesniewska I, Fonduli P, Zurrida F, Paglialonga F, Gucev Z, Paripovic D, Rus R, Said-Conti V, Sartz L, Chung WY, Park SJ, Lee JW, Park YH, Ahn YH, Sikora P, Stefanidis CJ, Tasic V, Konrad M, Anglani F, Addis M, Cheong HI, Ludwig M, and Bockenhauer D

Subjects

Adolescent, Child, Child, Preschool, Disease Progression, Female, Genotype, Glomerular Filtration Rate, Humans, Hypercalciuria genetics, Male, Nephrocalcinosis genetics, Phenotype, Proteinuria genetics, Renal Insufficiency, Chronic physiopathology, Renal Insufficiency, Chronic therapy, Retrospective Studies, Treatment Outcome, Hypercalciuria epidemiology, Mutation, Nephrocalcinosis epidemiology, Phosphoric Monoester Hydrolases genetics, Proteinuria epidemiology, Renal Insufficiency, Chronic genetics

Abstract

Background: Lowe syndrome (LS) and Dent-2 disease (DD2) are disorders associated with mutations in the OCRL gene and characterized by progressive chronic kidney disease (CKD). Here, we aimed to investigate the long-term renal outcome and identify potential determinants of CKD and its progression in children with these tubulopathies., Methods: Retrospective analyses were conducted of clinical and genetic data in a cohort of 106 boys (LS: 88 and DD2: 18). For genotype-phenotype analysis, we grouped mutations according to their type and localization. To investigate progression of CKD we used survival analysis by Kaplan-Meier method using stage 3 CKD as the end-point., Results: Median estimated glomerular filtration rate (eGFR) was lower in the LS group compared with DD2 (58.8 versus 87.4 mL/min/1.73 m2, P < 0.01). CKD stage II-V was found in 82% of patients, of these 58% and 28% had moderate-to-severe CKD in LS and DD2, respectively. Three patients (3%), all with LS, developed stage 5 of CKD. Survival analysis showed that LS was also associated with a faster CKD progression than DD2 (P < 0.01). On multivariate analysis, eGFR was dependent only on age (b = -0.46, P < 0.001). Localization, but not type of mutations, tended to correlate with eGFR. There was also no significant association between presence of nephrocalcinosis, hypercalciuria, proteinuria and number of adverse clinical events and CKD., Conclusions: CKD is commonly found in children with OCRL mutations. CKD progression was strongly related to the underlying diagnosis but did not associate with clinical parameters, such as nephrocalcinosis or proteinuria., (© The Author 2016. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2018

11. Impaired growth and intracranial calcifications in autosomal dominant hypocalcemia caused by a GNA11 mutation.

Author

Tenhola S, Voutilainen R, Reyes M, Toiviainen-Salo S, Jüppner H, and Mäkitie O

Subjects

Adult, Calcinosis blood, Calcinosis diagnostic imaging, Calcium blood, Child, Female, Humans, Hypercalciuria blood, Hypercalciuria diagnostic imaging, Hypocalcemia blood, Hypocalcemia diagnostic imaging, Hypoparathyroidism blood, Hypoparathyroidism diagnostic imaging, Hypoparathyroidism genetics, Magnetic Resonance Imaging, Male, Middle Aged, Mutation, Missense, Pedigree, Tomography, X-Ray Computed, Calcinosis genetics, GTP-Binding Protein alpha Subunits genetics, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital

Abstract

Objective: Autosomal dominant hypocalcemia (ADH) is characterized by hypocalcemia and inappropriately low PTH concentrations. ADH type 1 is caused by activating mutations in the calcium-sensing receptor (CASR), a G-protein-coupled receptor signaling through α11 (Gα11) and αq (Gαq) subunits. Heterozygous activating mutations in GNA11, the gene encoding Gα11, underlie ADH type 2. This study describes disease characteristics in a family with ADH caused by a gain-of-function mutation in GNA11., Design: A three-generation family with seven members (3 adults, 4 children) presenting with ADH., Methods: Biochemical parameters of calcium metabolism, clinical, genetic and brain imaging findings were analyzed., Results: Sanger sequencing revealed a heterozygous GNA11 missense mutation (c.1018G>A, p.V340M) in all seven hypocalcemic subjects, but not in the healthy family members (n=4). The adult patients showed clinical symptoms of hypocalcemia, while the children were asymptomatic. Plasma ionized calcium ranged from 0.95 to 1.14mmol/L, yet plasma PTH was inappropriately low for the degree of hypocalcemia. Serum 25OHD was normal. Despite hypocalcemia 1,25(OH)2D and urinary calcium excretion were inappropriately in the reference range. None of the patients had nephrocalcinosis. Two adults and one child (of the two MRI scanned children) had distinct intracranial calcifications. All affected subjects had short stature (height s.d. scores ranging from -3.4 to -2.3 vs -0.5 in the unaffected children)., Conclusions: The identified GNA11 mutation results in biochemical abnormalities typical for ADH. Additional features, including short stature and early intracranial calcifications, cosegregated with the mutation. These findings may indicate a wider role for Gα11 signaling besides calcium regulation., Competing Interests: Declaration of interest The authors declare that there is no conflict of interest that could be perceived as prejudicing the impartiality of the research reported., (© 2016 European Society of Endocrinology.)

Published

2016

12. Novel calcium-sensing receptor cytoplasmic tail deletion mutation causing autosomal dominant hypocalcemia: molecular and clinical study.

Author

Obermannova B, Sumnik Z, Dusatkova P, Cinek O, Grant M, Lebl J, and Hendy GN

Subjects

Adult, Base Sequence, Child, Preschool, Codon, Nonsense genetics, Cytoplasm, Family, Female, HEK293 Cells, Heterozygote, Humans, Hypercalciuria pathology, Hypocalcemia pathology, Hypoparathyroidism genetics, Hypoparathyroidism pathology, Male, Pedigree, Protein Structure, Tertiary genetics, Receptors, Calcium-Sensing chemistry, Genes, Dominant, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital, Receptors, Calcium-Sensing genetics, Sequence Deletion

Abstract

Objective: Autosomal dominant hypocalcemia (ADH) is a rare disorder caused by activating mutations of the calcium-sensing receptor (CASR). The treatment of ADH patients with 1α-hydroxylated vitamin D derivatives can cause hypercalciuria leading to nephrocalcinosis., Design and Methods: We studied a girl who presented with hypoparathyroidism and asymptomatic hypocalcemia at age 2.5 years. Mutations of CASR were investigated by DNA sequencing. Functional analyses of mutant and WT CASRs were done in transiently transfected human embryonic kidney (HEK293) cells., Results: The proband and her father are heterozygous for an eight-nucleotide deletion c.2703&#95;2710delCCTTGGAG in the CASR encoding the intracellular domain of the protein. Transient expression of CASR constructs in kidney cells in vitro suggested greater cell surface expression of the mutant receptor with a left-shifted extracellular calcium dose-response curve relative to that of the WT receptor consistent with gain of function. Initial treatment of the patient with calcitriol led to increased urinary calcium excretion. Evaluation for mosaicism in the paternal grandparents of the proband was negative., Conclusions: We describe a novel naturally occurring deletion mutation within the CASR that apparently arose de novo in the father of the ADH proband. Functional analysis suggests that the cytoplasmic tail of the CASR contains determinants that regulate the attenuation of signal transduction. Early molecular analysis of the CASR gene in patients with isolated idiopathic hypoparathyroidism is recommended because of its relevance to clinical outcome and treatment choice. In ADH patients, calcium supplementation and low-dose cholecalciferol avoids hypocalcemic symptoms without compromising renal function., (© 2016 European Society of Endocrinology.)

Published

2016

13. Recurrent FXYD2 p.Gly41Arg mutation in patients with isolated dominant hypomagnesaemia.

Author

de Baaij JH, Dorresteijn EM, Hennekam EA, Kamsteeg EJ, Meijer R, Dahan K, Muller M, van den Dorpel MA, Bindels RJ, Hoenderop JG, Devuyst O, and Knoers NV

Subjects

Adult, Female, Genes, Dominant, Homeostasis genetics, Humans, Hypercalciuria metabolism, Male, Nephrocalcinosis metabolism, Pedigree, Renal Tubular Transport, Inborn Errors metabolism, Sodium-Potassium-Exchanging ATPase metabolism, Hypercalciuria genetics, Magnesium blood, Mutation genetics, Nephrocalcinosis genetics, Renal Tubular Transport, Inborn Errors genetics, Sodium-Potassium-Exchanging ATPase genetics

Abstract

Background: Magnesium (Mg(2+)) is an essential ion for cell growth, neuroplasticity and muscle contraction. Blood Mg(2+) levels <0.7 mmol/L may cause a heterogeneous clinical phenotype, including muscle cramps and epilepsy and disturbances in K(+) and Ca(2+) homeostasis. Over the last decade, the genetic origin of several familial forms of hypomagnesaemia has been found. In 2000, mutations in FXYD2, encoding the γ-subunit of the Na(+)-K(+)-ATPase, were identified to cause isolated dominant hypomagnesaemia (IDH) in a large Dutch family suffering from hypomagnesaemia, hypocalciuria and chondrocalcinosis. However, no additional patients have been identified since then., Methods: Here, two families with hypomagnesaemia and hypocalciuria were screened for mutations in the FXYD2 gene. Moreover, the patients were clinically and genetically characterized., Results: We report a p.Gly41Arg FXYD2 mutation in two families with hypomagnesaemia and hypocalciuria. Interestingly, this is the same mutation as was described in the original study. As in the initial family, several patients suffered from muscle cramps, chondrocalcinosis and epilepsy. Haplotype analysis revealed an overlapping haplotype in all families, suggesting a founder effect., Conclusions: The recurrent p.Gly41Arg FXYD2 mutation in two new families with IDH confirms that FXYD2 mutation causes hypomagnesaemia. Until now, no other FXYD2 mutations have been reported which could indicate that other FXYD2 mutations will not cause hypomagnesaemia or are embryonically lethal., (© The Author 2015. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2015

14. Retrospective cohort study of familial hypomagnesaemia with hypercalciuria and nephrocalcinosis due to CLDN16 mutations.

Author

Sikora P, Zaniew M, Haisch L, Pulcer B, Szczepańska M, Moczulska A, Rogowska-Kalisz A, Bieniaś B, Tkaczyk M, Ostalska-Nowicka D, Zachwieja K, Hyla-Klekot L, Schlingmann KP, and Konrad M

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Heterozygote, Homozygote, Humans, Hypercalciuria epidemiology, Infant, Male, Nephrocalcinosis epidemiology, Poland epidemiology, Prevalence, Renal Tubular Transport, Inborn Errors epidemiology, Retrospective Studies, Young Adult, Claudins genetics, Hypercalciuria genetics, Mutation genetics, Nephrocalcinosis genetics, Renal Tubular Transport, Inborn Errors genetics

Abstract

Background: Familial hypomagnesaemia with hypercalciuria and nephrocalcinosis (FHHNC) is a rare autosomal recessive tubular disorder exhibiting a high risk for progressive chronic kidney disease (CKD)., Methods: This is a retrospective multicentre study of 25 paediatric cases with FHHNC in Poland. Median age at diagnosis was 4 years and median follow-up time was 4.8 years., Results: All cases of FHHNC carried recessive mutations in CLDN16. The founder mutation in CLDN16, Leu151Phe, was the most frequent cause of FHHNC in Polish patients, with 13 (52%) cases being homozygous and 5 (20%) carrying Leu151Phe allele in compound heterozygosity. All cases showed nephrocalcinosis, increased urinary fractional excretion of magnesium and hypercalciuria. Other disease features included hypomagnesaemia (76%), hyperparathyroidism (76%), hyperuricaemia (56%) and hypocitraturia (60%). Treatment with thiazides effectively reduced hypercalciuria in most cases. During follow-up, renal function declined in 60% of patients; 12% of patients reached CKD stage 3 or 4 and one patient developed end-stage renal failure., Conclusions: We report one of the largest cohorts of FHHNC cases caused by CLDN16 mutations. A missense variant of CLDN16, Leu151Phe, is the most common mutation responsible for FHHNC in Poland. Additionally, we found that normomagnesaemia does not exclude FHHNC and the calculation of fractional excretion of Mg can be diagnostic in the setting of normomagnesaemia. We also demonstrate the efficacy of a treatment with thiazides in terms of hypercalciuria in the majority of patients., (© The Author 2014. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2015

15. Exome sequencing identifies a novel homozygous mutation in the phosphate transporter SLC34A1 in hypophosphatemia and nephrocalcinosis.

Author

Rajagopal A, Braslavsky D, Lu JT, Kleppe S, Clément F, Cassinelli H, Liu DS, Liern JM, Vallejo G, Bergadá I, Gibbs RA, Campeau PM, and Lee BH

Subjects

Child, Child, Preschool, DNA Mutational Analysis, Female, Humans, Hypercalcemia genetics, Hypercalciuria genetics, Male, Parathyroid Hormone blood, Pedigree, Phenotype, Exome, Hypophosphatemia genetics, Mutation, Nephrocalcinosis genetics, Sodium-Phosphate Cotransporter Proteins, Type IIa genetics

Abstract

Context: Two Argentinean siblings (a boy and a girl) from a nonconsanguineous family presented with hypercalcemia, hypercalciuria, hypophosphatemia, low parathyroid hormone (PTH), and nephrocalcinosis., Objective: The goal of this study was to identify genetic causes of the clinical findings in the two siblings., Design: Whole exome sequencing was performed to identify disease-causing mutations in the youngest sibling, and a candidate variant was screened in other family members by Sanger sequencing. In vitro experiments were conducted to determine the effects of the mutation that was identified., Patients and Other Participants: Affected siblings (2 y.o. female and 10 y.o male) and their parents were included in the study. Informed consent was obtained for genetic studies., Results: A novel homozygous mutation in the gene encoding the renal sodium-dependent phosphate transporter SLC34A1 was identified in both siblings (c.1484G>A, p.Arg495His). In vitro studies showed that the p.Arg495His mutation resulted in decreased phosphate uptake when compared to wild-type SLC34A1., Conclusions: The homozygous G>A transition that results in the substitution of histidine for arginine at position 495 of the renal sodium-dependent phosphate transporter, SLC34A1, is involved in disease pathogenesis in these patients. Our report of the second family with two mutated SLC34A1 alleles expands the known phenotype of this rare condition.

Published

2014

16. Inherited disorders of renal hypomagnesaemia.

Author

Konrad M and Schlingmann KP

Subjects

Humans, Magnesium Deficiency blood, Metal Metabolism, Inborn Errors blood, Hypercalciuria genetics, Magnesium blood, Magnesium Deficiency genetics, Metal Metabolism, Inborn Errors genetics, Nephrocalcinosis genetics, Renal Tubular Transport, Inborn Errors genetics

Abstract

The kidney plays a key role in the maintenance of normal magnesium balance. The distal tubule of the kidney, namely the thick ascending limb of the loop of Henle and the distal convoluted tubule, is crucial for the regulation of serum magnesium levels and body magnesium content. The identification of molecular defects related to rare inherited magnesium losing disorders has contributed greatly to a better understanding of the process of renal magnesium handling. Since the number of genetic defects related to magnesium metabolism is still increasing, it might be expected that our knowledge on magnesium physiology will further improve. This knowledge will hopefully lead to therapeutic strategies that enable specific therapies for patients suffering from the symptoms and possible sequelae of chronic magnesium depletion., (© The Author 2014. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2014

17. Autosomal dominant hypoparathyroidism caused by germline mutation in GNA11: phenotypic and molecular characterization.

Author

Li D, Opas EE, Tuluc F, Metzger DL, Hou C, Hakonarson H, and Levine MA

Subjects

Adolescent, Adult, Bone Development genetics, Child, Child, Preschool, Family Health, Female, Genome-Wide Association Study, Heterozygote, Humans, Hypoparathyroidism genetics, Male, Middle Aged, Pedigree, Phenotype, Young Adult, GTP-Binding Protein alpha Subunits genetics, Germ-Line Mutation genetics, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital

Abstract

Context: Most cases of autosomal dominant hypoparathyroidism (ADH) are caused by gain-of-function mutations in CASR or dominant inhibitor mutations in GCM2 or PTH., Objective: Our objectives were to identify the genetic basis for ADH in a multigenerational family and define the underlying disease mechanism., Subjects: Here we evaluated a multigenerational family with ADH in which affected subjects had normal sequences in these genes and were shorter than unaffected family members., Methods: We collected clinical and biochemical data from 6 of 11 affected subjects and performed whole-exome sequence analysis on DNA from two affected sisters and their affected father. Functional studies were performed after expression of wild-type and mutant Gα11 proteins in human embryonic kidney-293-CaR cells that stably express calcium-sensing receptors., Results: Whole-exome-sequencing followed by Sanger sequencing revealed a heterozygous mutation, c.179G>T; p.R60L, in GNA11, which encodes the α-subunit of G11, the principal heterotrimeric G protein that couples calcium-sensing receptors to signal activation in parathyroid cells. Functional studies of Gα11 R60L showed increased accumulation of intracellular concentration of free calcium in response to extracellular concentration of free calcium with a significantly decreased EC50 compared with wild-type Gα11. By contrast, R60L was significantly less effective than the oncogenic Q209L form of Gα11 as an activator of the MAPK pathway. Compared to subjects with CASR mutations, patients with GNA11 mutations lacked hypercalciuria and had normal serum magnesium levels., Conclusions: Our findings indicate that the germline gain-of-function mutation of GNA11 is a cause of ADH and implicate a novel role for GNA11 in skeletal growth.

Published

2014

18. Mutational analysis of the adaptor protein 2 sigma subunit (AP2S1) gene: search for autosomal dominant hypocalcemia type 3 (ADH3).

Author

Rogers A, Nesbit MA, Hannan FM, Howles SA, Gorvin CM, Cranston T, Allgrove J, Bevan JS, Bano G, Brain C, Datta V, Grossman AB, Hodgson SV, Izatt L, Millar-Jones L, Pearce SH, Robertson L, Selby PL, Shine B, Snape K, Warner J, and Thakker RV

Subjects

Adult, Child, Child, Preschool, DNA Mutational Analysis, Female, Gene Frequency, Humans, Hypoparathyroidism genetics, Infant, Infant, Newborn, Male, Middle Aged, Polymorphism, Single Nucleotide, Adaptor Protein Complex 2 genetics, Adaptor Protein Complex sigma Subunits genetics, Hypercalciuria genetics, Hypocalcemia genetics, Hypoparathyroidism congenital

Abstract

Context: Autosomal dominant hypocalcemia (ADH) types 1 and 2 are due to calcium-sensing receptor (CASR) and G-protein subunit-α11 (GNA11) gain-of-function mutations, respectively, whereas CASR and GNA11 loss-of-function mutations result in familial hypocalciuric hypercalcemia (FHH) types 1 and 2, respectively. Loss-of-function mutations of adaptor protein-2 sigma subunit (AP2σ 2), encoded by AP2S1, cause FHH3, and we therefore sought for gain-of-function AP2S1 mutations that may cause an additional form of ADH, which we designated ADH3., Objective: The objective of the study was to investigate the hypothesis that gain-of-function AP2S1 mutations may cause ADH3., Design: The sample size required for the detection of at least one mutation with a greater than 95% likelihood was determined by binomial probability analysis. Nineteen patients (including six familial cases) with hypocalcemia in association with low or normal serum PTH concentrations, consistent with ADH, but who did not have CASR or GNA11 mutations, were ascertained. Leukocyte DNA was used for sequence and copy number variation analysis of AP2S1., Results: Binomial probability analysis, using the assumption that AP2S1 mutations would occur in hypocalcemic patients at a prevalence of 20%, which is observed in FHH patients without CASR or GNA11 mutations, indicated that the likelihood of detecting at least one AP2S1 mutation was greater than 95% and greater than 98% in sample sizes of 14 and 19 hypocalcemic patients, respectively. AP2S1 mutations and copy number variations were not detected in the 19 hypocalcemic patients., Conclusion: The absence of AP2S1 abnormalities in hypocalcemic patients, suggests that ADH3 may not occur or otherwise represents a rare hypocalcemic disorder.

Published

2014

19. A lifetime of hypercalcemia and hypercalciuria, finally explained.

Author

Jacobs TP, Kaufman M, Jones G, Kumar R, Schlingmann KP, Shapses S, and Bilezikian JP

Subjects

Aged, Confusion blood, Confusion diagnosis, Confusion genetics, Fatigue blood, Fatigue diagnosis, Fatigue genetics, Humans, Hypercalcemia blood, Hypercalciuria blood, Hypertension blood, Hypertension diagnosis, Hypertension genetics, Male, Nephrolithiasis blood, Nephrolithiasis diagnosis, Nephrolithiasis genetics, Recurrence, Steroid Hydroxylases genetics, Vitamin D analogs & derivatives, Vitamin D blood, Vitamin D3 24-Hydroxylase, Delayed Diagnosis, Hypercalcemia diagnosis, Hypercalcemia genetics, Hypercalciuria diagnosis, Hypercalciuria genetics

Abstract

Context: Hypercalcemia, hypercalciuria, and recurrent nephrolithiasis are all common clinical problems. This case report illustrates a newly described but possibly not uncommon cause of this presenting complex., Objective: We report on a patient studied for over 30 years, with the diagnosis finally made with modern biochemical and genetic tools., Design and Setting: This study consists of a case report and review of literature conducted in a University Referral Center., Patient and Intervention: A single patient with hypercalcemia, hypercalciuria, and recurrent nephrolithiasis was treated with low-calcium diet, low vitamin D intake, prednisone, and ketoconazole., Main Outcome Measure: We measured the patient's clinical and biochemical response to interventions above., Results: Calcium absorption measured by dual isotope absorptiometry was elevated at 37.4%. Serum levels of 24,25-dihydroxyvitamin D were very low, as measured in two laboratories (0.62 ng/mL [normal, 3.49 ± 1.57], and 0.18 mg/mL). Genetic analysis of CYP24A1 revealed homozygous mutation E143del previously described. The patient's serum calcium and renal function improved markedly on treatment with ketoconazole but not with prednisone., Conclusions: Chronic hypercalcemia, hypercalciuria, and/or nephrolithiasis may be caused by mutations in CYP24A1 causing failure to metabolize 1,25-dihydroxyvitamin D.

Published

2014

20. Functional activities of mutant calcium-sensing receptors determine clinical presentations in patients with autosomal dominant hypocalcemia.

Author

Kinoshita Y, Hori M, Taguchi M, Watanabe S, and Fukumoto S

Subjects

Adult, Calcium blood, Child, Female, Humans, Hypercalciuria genetics, Hypercalciuria metabolism, Hypocalcemia genetics, Hypocalcemia metabolism, Hypoparathyroidism diagnosis, Hypoparathyroidism genetics, Hypoparathyroidism metabolism, Magnesium blood, Male, Middle Aged, Parathyroid Hormone blood, Phenotype, Receptors, Calcium-Sensing metabolism, Hypercalciuria diagnosis, Hypocalcemia diagnosis, Hypoparathyroidism congenital, Mutation, Receptors, Calcium-Sensing genetics

Abstract

Objective: Autosomal dominant hypocalcemia (ADH) is a congenital isolated hypoparathyroidism caused by activating mutations in the calcium-sensing receptor (CASR) gene. The clinical features of ADH are heterogeneous; some patients are asymptomatic, and others show severe hypocalcemia with Bartter's syndrome. We therefore recruited 12 patients with ADH to clarify the determinants of their clinical presentation., Design and Methods: We studied two sporadic and 10 familial cases of ADH. Serum concentrations of calcium, intact PTH, and magnesium (Mg(2+)) were measured in each patient. Fractional excretion of Mg (FE(Mg)) was calculated in spot urine samples. A nuclear factor of activated T cells luciferase assay was used to analyze the responsiveness of each mutant CaSR to extracellular Ca(2+)., Results: Genomic analysis revealed five known activating mutations and a novel mutation, E481K, in the CASR. Patients with the A843E, C131W, or F788C mutation showed hypomagnesemia with elevated FE(Mg). Intact PTH in these patients was consistently near the detection limit. In contrast, patients with the P221L, K47N, or E481K mutation exhibited normal Mg(2+) levels. In these patients, intact PTH increased in response to low calcium, and their maximum intact PTH exceeded the lower limit of the reference range. Functional analysis showed an association between the disease severity and the in vitro activity of the mutant CaSR., Conclusions: The functional activity of mutant CaSR determines the serum Mg(2+) level, renal Mg(2+) handling, and intact PTH in patients with ADH. The presence of hypomagnesemia with elevated FE(Mg) may indicate the diagnosis of ADH among patients with PTH-deficient hypoparathyroidism.

Published

2014

21. Decreased transcriptional activity of calcium-sensing receptor gene promoter 1 is associated with calcium nephrolithiasis.

Author

Vezzoli G, Terranegra A, Aloia A, Arcidiacono T, Milanesi L, Mosca E, Mingione A, Spotti D, Cusi D, Hou J, Hendy GN, Soldati L, Paloschi V, Dogliotti E, Brasacchio C, Dell'Antonio G, Montorsi F, Bertini R, Bellinzoni P, Guazzoni G, Borghi L, Guerra A, Allegri F, Ticinesi A, Meschi T, Nouvenne A, Lupo A, Fabris A, Gambaro G, Strazzullo P, Rendina D, De Filippo G, Brandi ML, Croppi E, Cianferotti L, Trinchieri A, Caudarella R, Cupisti A, Anglani F, and Del Prete D

Subjects

Adult, Alleles, Case-Control Studies, Female, Genotype, HEK293 Cells, Humans, Hypercalciuria genetics, Hypercalciuria metabolism, Male, Middle Aged, Mutagenesis, Site-Directed, Nephrolithiasis metabolism, Polymorphism, Single Nucleotide, Receptors, Calcium-Sensing metabolism, Kidney metabolism, Nephrolithiasis genetics, Promoter Regions, Genetic genetics, Receptors, Calcium-Sensing genetics, Transcription, Genetic

Abstract

Background: CaSR gene is a candidate for calcium nephrolithiasis. Single-nucleotide polymorphisms (SNPs) encompassing its regulatory region were associated with calcium nephrolithiasis., Aims: We tested SNPs in the CaSR gene regulatory region associated with calcium nephrolithiasis and their effects in kidney., Subjects and Methods: One hundred sixty-seven idiopathic calcium stone formers and 214 healthy controls were genotyped for four CaSR gene SNPs identified by bioinformatics analysis as modifying transcription factor binding sites. Strontium excretion after an oral load was tested in 55 stone formers. Transcriptional activity induced by variant alleles at CaSR gene promoters was compared by luciferase reporter gene assay in HEK-293 and HKC-8 cells. CaSR and claudin-14 mRNA levels were measured by real-time PCR in 107 normal kidney medulla samples and compared in patients with different CaSR genotype., Results: Only rs6776158 (A>G), located in the promoter 1, was associated with nephrolithiasis. Its minor G allele was more frequent in stone formers than controls (37.8% vs 26.4%, P = .001). A reduced strontium excretion was observed in GG homozygous stone formers. Luciferase fluorescent activity was lower in cells transfected with the promoter 1 including G allele at rs6776158 than cells transfected with the A allele. CaSR mRNA levels were lower in kidney medulla samples from homozygous carriers for the G allele at rs6776158 than carriers for the A allele. Claudin-14 mRNA levels were also lower in GG homozygous subjects., Conclusions: Minor allele at rs6776158 may predispose to calcium stones by decreasing transcriptional activity of the CaSR gene promoter 1 and CaSR expression in kidney tubules.

Published

2013

22. Fanconi-Bickel syndrome and autosomal recessive proximal tubulopathy with hypercalciuria (ARPTH) are allelic variants caused by GLUT2 mutations.

Author

Mannstadt M, Magen D, Segawa H, Stanley T, Sharma A, Sasaki S, Bergwitz C, Mounien L, Boepple P, Thorens B, Zelikovic I, and Jüppner H

Subjects

Adolescent, Amino Acid Sequence, Animals, Familial Hypophosphatemic Rickets, Family Health, Fanconi Syndrome metabolism, Female, Genes, Recessive genetics, Genetic Variation, Genome-Wide Association Study, Glucose Transporter Type 1 genetics, Glucose Transporter Type 2 metabolism, Humans, Hypercalciuria metabolism, Hypophosphatemia, Familial metabolism, Kidney Tubules, Proximal metabolism, Male, Mice, Mice, Transgenic, Molecular Sequence Data, Oocytes physiology, Pedigree, Rickets metabolism, Sodium-Phosphate Cotransporter Proteins, Type IIa genetics, Sodium-Phosphate Cotransporter Proteins, Type IIc genetics, Xenopus laevis, Fanconi Syndrome genetics, Glucose Transporter Type 2 genetics, Hypercalciuria genetics, Hypophosphatemia, Familial genetics, Rickets genetics

Abstract

Context: Many inherited disorders of calcium and phosphate homeostasis are unexplained at the molecular level., Objective: The objective of the study was to identify the molecular basis of phosphate and calcium abnormalities in two unrelated, consanguineous families., Patients: The affected members in family 1 presented with rickets due to profound urinary phosphate-wasting and hypophosphatemic rickets. In the previously reported family 2, patients presented with proximal renal tubulopathy and hypercalciuria yet normal or only mildly increased urinary phosphate excretion., Methods: Genome-wide linkage scans and direct nucleotide sequence analyses of candidate genes were performed. Transport of glucose and phosphate by glucose transporter 2 (GLUT2) was assessed using Xenopus oocytes. Renal sodium-phosphate cotransporter 2a and 2c (Npt2a and Npt2c) expressions were evaluated in transgenically rescued Glut2-null mice (tgGlut2-/-)., Results: In both families, genetic mapping and sequence analysis of candidate genes led to the identification of two novel homozygous mutations (IVS4-2A>G and R124S, respectively) in GLUT2, the gene mutated in Fanconi-Bickel syndrome, a rare disease usually characterized by renal tubulopathy, impaired glucose homeostasis, and hepatomegaly. Xenopus oocytes expressing the [R124S]GLUT2 mutant showed a significant reduction in glucose transport, but neither wild-type nor mutant GLUT2 facilitated phosphate import or export; tgGlut2-/- mice demonstrated a profound reduction of Npt2c expression in the proximal renal tubules., Conclusions: Homozygous mutations in the facilitative glucose transporter GLUT2, which cause Fanconi-Bickel syndrome, can lead to very different clinical and biochemical findings that are not limited to mild proximal renal tubulopathy but can include significant hypercalciuria and highly variable degrees of urinary phosphate-wasting and hypophosphatemia, possibly because of the impaired proximal tubular expression of Npt2c.

Published

2012

23. Hypercalcemia, hypercalciuria, and elevated calcitriol concentrations with autosomal dominant transmission due to CYP24A1 mutations: effects of ketoconazole therapy.

Author

Tebben PJ, Milliner DS, Horst RL, Harris PC, Singh RJ, Wu Y, Foreman JW, Chelminski PR, and Kumar R

Subjects

Adult, Genotype, Humans, Hypercalcemia blood, Hypercalcemia genetics, Hypercalciuria blood, Hypercalciuria genetics, Male, Mutation, Syndrome, Treatment Outcome, Vitamin D3 24-Hydroxylase, 14-alpha Demethylase Inhibitors therapeutic use, Calcitriol blood, Hypercalcemia drug therapy, Hypercalciuria drug therapy, Ketoconazole therapeutic use, Steroid Hydroxylases genetics

Abstract

Background: Mutations of the CYP24A1 gene, which encodes the 1,25-dihydroxyvitamin D-24-hydroxylase cytochrome P450, Cyp24A1, are predicted to result in elevated 1,25-dihydroxyvitamin D concentrations, hypercalcemia, hypercalciuria, nephrolithiasis, and bone disease. Treatment of hypercalcemia associated with CYP24A1 gene mutations has not been described., Methods: The genetic basis of a syndrome in a 44-yr-old Caucasian male characterized by intermittent hypercalcemia, hypercalciuria, elevated serum 1,25-dihydroxyvitamin D, undetectable serum 24,25-dihydroxyvitamin D, metabolically active nephrolithiasis, and reduced bone mineral density of the lumbar spine was examined. Sequencing of the CYP24A1 gene and biochemical and genetic analysis of seven family members in three generations was carried out. Because of hypercalcemia, hypercalciuria, and metabolically active nephrolithiasis, the patient was treated with a cytochrome 3A inhibitor, ketoconazole, 200 mg orally every 8 h, for 2 months., Results: The sequence of the CYP24A1 gene showed two canonical splice junction mutations in the proband. Analysis of family members showed a phenotype associated one or both mutations, suggesting autosomal dominant transmission with partial penetrance of the trait. After therapy with ketoconazole, statistically significant reductions in previously elevated urinary calcium into the normal range were noted. Previously elevated serum 1,25-dihydroxyvitamin D and calcium concentrations decreased, and previously decreased PTH concentrations increased into the normal range, but the differences were not statistically significant., Conclusions: In a syndrome characterized by intermittent hypercalcemia, hypercalciuria, elevated 1,25-dihydroxyvitamin D, undetectable 24,25-dihydroxyvitamin D concentrations, splice junction mutations of the CYP24A1 gene, and autosomal dominant transmission of the trait, treatment with ketoconazole is useful in reducing urinary calcium.

Published

2012

24. Clinical and molecular characterization of Turkish patients with familial hypomagnesaemia: novel mutations in TRPM6 and CLDN16 genes.

Author

Guran T, Akcay T, Bereket A, Atay Z, Turan S, Haisch L, Konrad M, and Schlingmann KP

Subjects

Adolescent, Age Distribution, Child, Child, Preschool, Cohort Studies, DNA Mutational Analysis, Female, Humans, Hypercalciuria diagnosis, Incidence, Infant, Infant, Newborn, Male, Mutation, Nephrocalcinosis diagnosis, Pedigree, Phenotype, Renal Tubular Transport, Inborn Errors diagnosis, Risk Assessment, Severity of Illness Index, Sex Distribution, Turkey epidemiology, Claudins genetics, Genetic Predisposition to Disease, Hypercalciuria epidemiology, Hypercalciuria genetics, Nephrocalcinosis epidemiology, Nephrocalcinosis genetics, Renal Tubular Transport, Inborn Errors epidemiology, Renal Tubular Transport, Inborn Errors genetics, TRPM Cation Channels genetics

Abstract

Background: Recent identification and characterization of novel renal Mg(2+) transporters and ion channels have greatly increased our understanding of the normal physiology of renal magnesium handling., Methods: The present study deals with the clinical and molecular characterization of eight Turkish children (median age 10.6 years, range 3-16.2 years, five boys and three girls) with primary hypomagnesaemia from six families., Results: All patients initially presented with tetany and convulsions. Laboratory evaluation yielded severely low serum magnesium levels and low serum calcium levels in all patients. While six patients exhibited inadequately low parathyroid hormone levels, the two remaining patients showed hyperparathyroidism, hypercalciuria and nephrocalcinosis. Genetic studies revealed familial hypomagnesaemia with secondary hypocalcaemia (HSH) due to a TRPM6 mutation in six patients and familial hypomagnesaemia with hypercalciuria and nephrocalcinosis (FHHNC) due to a CLDN16 mutation in one patient., Conclusions: Among recently identified magnesium-wasting disorders, HSH and FHHNC represent two major entities also in the Turkish population. Besides clinical course and laboratory diagnosis of hypomagnesaemia, the detection of renal calcium wasting and parathyroid function are crucial to differentiate between these most prevalent forms of hereditary magnesium deficiency. While TRPM6 mutations underlying HSH almost uniformly lead to a complete loss of function of the TRPM6 protein, the severity of FHHNC phenotype depends on the residual function of the mutated claudin-16 protein.

Published

2012

25. Mechanisms for hypercalciuria in pseudohypoaldosteronism type II-causing WNK4 knock-in mice.

Author

Yang SS, Hsu YJ, Chiga M, Rai T, Sasaki S, Uchida S, and Lin SH

Subjects

Animals, Blotting, Western, Calbindin 1, Calbindins, Calcifediol blood, Calcium Channels genetics, Calcium Channels metabolism, Creatinine blood, Fluorescent Antibody Technique, Hypercalciuria genetics, Hypercalciuria metabolism, Ion Transport genetics, Mice, Mice, Transgenic, Parathyroid Hormone blood, Pseudohypoaldosteronism genetics, Pseudohypoaldosteronism metabolism, Reverse Transcriptase Polymerase Chain Reaction, S100 Calcium Binding Protein G genetics, S100 Calcium Binding Protein G metabolism, Sodium-Hydrogen Exchanger 3, Sodium-Hydrogen Exchangers genetics, Sodium-Hydrogen Exchangers metabolism, Sodium-Potassium-Chloride Symporters genetics, Sodium-Potassium-Chloride Symporters metabolism, Solute Carrier Family 12, Member 1, TRPV Cation Channels genetics, TRPV Cation Channels metabolism, Hypercalciuria etiology, Nephrons metabolism, Protein Serine-Threonine Kinases genetics, Pseudohypoaldosteronism complications

Abstract

The mechanisms underlying hypercalciuria in pseudohypoaldosteronism type II (PHAII) caused by WNK4 mutations remain unclear. In this study, we used Wnk4(D561A/+) knock-in mice as a model of human PHAII for investigating the pathogenesis of hypercalciuria in PHAII. Serum and urine biochemistries were obtained from Wnk4(+/+) and Wnk4(D561A/+) littermates. Expression of the epithelial Ca(2+) channels [transient receptor potential channel vanilloid subtype 5 (TRPV5) and TRPV6] and calbindin-D28k (CBP-D28k) in the distal nephron and two upstream Na(+) transporters, Na(+)/H(+) exchanger 3 and Na(+)-K(+)-2Cl(-) cotransporter 2 involved in paracellular Ca(2+) reabsorption, were examined by real-time PCR, immunofluorescent staining, and immunoblotting. Compared with Wnk4(+/+) littermate controls, Wnk4(D561A/+) mice manifested hypercalciuria despite no significant differences in serum creatinine, ionized Ca(2+), PTH, and 1,25 hydroxylvitamin D(3) levels. There was no significant difference in TRPV5 expression, but a significant increase in TRPV6 and CBP-D28k was observed in Wnk4(D561A/+) mice. Despite no significant change in Na(+)/H(+) exchanger 3 expression, Na(+)-K(+)-2Cl(-) cotransporter 2 expression was significantly attenuated and urine Ca(2+) excretion rate in response to furosemide was blunted in Wnk4(D561A/+) mice. Decreased Ca(2+) reabsorption in the upstream nephron, especially in the thick ascending loops of Henle, with a secondary adaptive increase in TRPV6 and CBP-D28k expression in the distal tubules might be involved in the hypercalciuria of PHAII.

Published

2010

26. Hypophosphatemic rickets with hypercalciuria due to mutation in SLC34A3/type IIc sodium-phosphate cotransporter: presentation as hypercalciuria and nephrolithiasis.

Author

Tencza AL, Ichikawa S, Dang A, Kenagy D, McCarthy E, Econs MJ, and Levine MA

Subjects

Child, Exons genetics, Familial Hypophosphatemic Rickets pathology, Female, Femur pathology, Heterozygote, Humans, Magnetic Resonance Imaging, Male, Nuclear Family, Polymerase Chain Reaction, Tibia pathology, Familial Hypophosphatemic Rickets genetics, Hypercalciuria genetics, Mutation, Missense, Nephrolithiasis genetics, Sodium-Phosphate Cotransporter Proteins, Type IIc genetics

Abstract

Context: Hereditary hypophosphatemic rickets with hypercalciuria (HHRH) is a metabolic disorder due to homozygous loss-of-function mutations in the SLC34A3 gene encoding the renal type IIc sodium-phosphate cotransporter (NaPi-IIc). The typical presentation is severe rickets and hypophosphatemia, and hypercalciuria is often discovered later or overlooked., Objective: We sought to determine the genetic basis for severe hypercalciuria and nephrolithiasis/nephrocalcinosis in an adolescent male with elevated serum levels of calcitriol but normal serum levels of calcium and phosphorus., Design and Setting: We used PCR to analyze the SLC34A3 gene in the proband and members of his family., Results: The proband was a compound heterozygote for two SLC34A3 missense mutations, a novel c.544C-->T in exon 6 that results in replacement of arginine at position 182 by tryptophan (R182W) and c.575C-->T in exon 7 that results in replacement of serine at position 192 by leucine (S192L). The R182W and S192L alleles were inherited from the mother and father, respectively, both of whom had hypercalciuria. A clinically unaffected brother was heterozygous for S192L., Conclusion: We report a novel mutation in the SLC34A3 gene in a patient with an unusual presentation of HHRH. This report emphasizes that moderate and severe hypercalciuria can be manifestations of heterozygous or homozygous loss-of-function mutations in the SLC34A3 gene, respectively, providing further evidence for a gene dosage effect in determining the phenotype. HHRH may be an underdiagnosed condition that can masquerade as idiopathic hypercalciuria or osteopenia.

Published

2009

27. A novel loss-of-function mutation, Gln459Arg, of the calcium-sensing receptor gene associated with apparent autosomal recessive inheritance of familial hypocalciuric hypercalcemia.

Author

Lietman SA, Tenenbaum-Rakover Y, Jap TS, Yi-Chi W, De-Ming Y, Ding C, Kussiny N, and Levine MA

Subjects

Amino Acid Substitution, Arginine genetics, Calcium blood, Cell Line, Child, Preschool, Chromosome Disorders genetics, Exons genetics, Female, Gene Silencing, Glutamine genetics, Heterozygote, Humans, Hypercalcemia complications, Hypercalciuria complications, Male, Parathyroid Hormone blood, Pedigree, Transfection, Genes, Recessive genetics, Hypercalcemia genetics, Hypercalciuria genetics, Mutation, Receptors, Calcium-Sensing genetics

Abstract

Context: Mutations that inactivate one allele of the gene encoding the calcium sensing receptor (CaSR) cause autosomal dominant familial hypocalciuric hypercalcemia (FHH), whereas homozygous mutations cause neonatal severe hyperparathyroidism., Objective: We describe the identification and biochemical characterization of a novel CASR gene mutation that caused apparent autosomal recessive FHH in an extended consanguineous kindred., Design: The study design involved direct sequence analysis of the CaSR gene, clinical and biochemical analyses of patients, and in vitro immunobiochemical studies of the mutant CaSR., Results: A novel inactivating mutation (Q459R) was identified in exon 4 of both alleles of the CASR in the proband, who presented with asymptomatic hypercalcemia and hypocalciuria at age 2 yr. The proband's parents were heterozygous for the Q459R mutation consistent with autosomal recessive inheritance of FHH. Among 13 family members that were studied, eight subjects were heterozygous for the Q459R mutation and five had normal genotypes. All heterozygous subjects were asymptomatic and normocalcemic apart from one subject who was mildly hypercalcemic. The Q459R mutant CaSR was normally expressed at the cell membrane but retained only 30-50% of the calcium-dependent activity of the wild-type CaSR., Conclusion: We identified a novel loss-of-function Q459R mutation in the CASR gene that exhibits mildly reduced sensitivity to calcium and that is associated with apparent autosomal recessive transmission of FHH. This study demonstrates the importance of genetic testing in FHH to distinguish between de novo and inherited mutations of the CASR gene and assist in management decisions.

Published

2009

28. Familial hyperkalemia and hypertension: pathogenetic insights based on lithium clearance.

Author

Mayan H, Melnikov S, Novikov I, Holtzman EJ, and Farfel Z

Subjects

Adult, Calcium blood, Calcium urine, Female, Humans, Hypercalciuria genetics, Male, Metabolic Clearance Rate, Middle Aged, Pedigree, Potassium blood, Receptors, Drug physiology, Solute Carrier Family 12, Member 3, Symporters physiology, Hyperkalemia genetics, Hypertension genetics, Lithium metabolism, Mutation, Protein Serine-Threonine Kinases genetics

Abstract

Context: Familial hyperkalemia and hypertension (FHHt) is caused by mutations in WNK kinases. Its pathogenesis is not completely understood., Objective: Our objective was to investigate the mechanism of hypercalciuria in FHHt., Design and Setting: We conducted a study of a large family with FHHt and WNK4 Q565E mutation and of control subjects at a referral medical center., Subjects: Forty-six members of a family with FHHt and WNK4 Q565E mutation, 23 of them affected, and 12 control subjects participated., Main Outcome Measures: Urinary calcium and sodium concentrations, endogenous lithium clearance, age of hypertension appearance were assessed., Results: In 40 urine samples of 20 affected subjects, urinary calcium was correlated to urinary sodium (r = 0.567; P = 0.0001). In 28 urinary samples of 22 unaffected members, no correlation was found (r = 0.285; P = 0.14). Mean ratio of urinary calcium to urinary sodium was 2.7-fold higher in affected compared with unaffected members (58.7 +/- 25.9 vs. 22.1 +/- 14.0 micromol/mmol, P < 0.0001). Endogenous lithium clearance in eight affected members was about 50% lower than in 12 controls (16.2 +/- 7.7 vs. 28.8 +/- 9.8 ml/min, P = 0.0073). Hypertension was detected in males 12 yr earlier than in females (26.0 +/- 7.5 vs. 37.9 +/- 11.3 yr; P = 0.031)., Conclusions: Hypercalciuria in FHHt seems to be dependent on urinary sodium. According to molecular studies, FHHt patients are presumed to have increased distal nephron sodium reabsorption and therefore decreased proximal reabsorption of sodium, lithium, and calcium. The observed decreased lithium clearance reflects probable abnormal renal handling of lithium, i.e. distal nephron lithium reabsorption. Therefore, hypercalciuria may result from proximal nephron aberration. Finally, earlier appearance of hypertension in males may be the result of sex-hormone activity.

Published

2009

29. TRPV5 gene polymorphisms in renal hypercalciuria.

Author

Renkema KY, Lee K, Topala CN, Goossens M, Houillier P, Bindels RJ, and Hoenderop JG

Subjects

Amino Acid Substitution, Animals, Base Sequence, Cell Line, Cohort Studies, DNA Primers genetics, Heterozygote, Homozygote, Humans, Hypercalciuria complications, Hypercalciuria metabolism, Kidney Calculi etiology, Kidney Calculi genetics, Mice, Models, Molecular, Patch-Clamp Techniques, Recombinant Proteins genetics, Recombinant Proteins metabolism, TRPV Cation Channels chemistry, TRPV Cation Channels metabolism, Hypercalciuria genetics, Polymorphism, Single Nucleotide, TRPV Cation Channels genetics

Abstract

Background: Kidney stone formation is a major socioeconomic problem in humans, involving pain, recurrent treatment and renal insufficiency. As most renal precipitates contain calcium as a major component, hypercalciuria is the main risk factor for renal stone formation. Different forms of hypercalciuria can be classified, which primarily arise from defects in the main organs involved in calcium homeostasis. A distinction can be made between renal, absorptive and resorptive hypercalciuria, originating from disturbed calcium handling in kidney, intestine and bone, respectively. A positive family history predisposes individuals to an increased risk of stone formation, which strongly indicates the involvement of genetic susceptibility factors. TRPV5 is the renal epithelial calcium channel that is the gatekeeper protein in active calcium reabsorption in the kidney. TRPV5 gene ablation in mice leads to severe hypercalciuria, implying that TRPV5 is an interesting candidate gene for renal hypercalciuria in humans. This study aims to identify and functionally characterize TRPV5 gene aberrations in patients with renal hypercalciuria., Methods: The TRPV5 coding region and intron-exon boundaries were screened for gene mutations in 20 subjects displaying renal hypercalciuria after which identified non-synonymous polymorphisms were functionally characterized by patch-clamp analysis. Wild-type and TRPV5 channels including polymorphisms were transiently expressed in human embryonic kidney (HEK) 293 cells and functionally characterized by path-clamp analysis., Results: Genotyping TRPV5 in renal hypercalciuria patients revealed three non-synonymous and five synonymous polymorphisms. Electrophysiological characterization of the TRPV5 mutants did not reveal significant functional changes compared to wild-type TRPV5 channel recordings., Conclusions: In this specific patient cohort, our data do not support a primary role for TRPV5 in the pathogenesis of renal hypercalciuria. However, TRPV5 cannot be excluded as a candidate gene in hypercalciuria.

Published

2009

30. Hydrochlorothiazide in CLDN16 mutation.

Author

Zimmermann B, Plank C, Konrad M, Stöhr W, Gravou-Apostolatou C, Rascher W, and Dötsch J

Subjects

Adolescent, Adult, Calcium urine, Child, Child, Preschool, Claudins, Creatinine urine, Dose-Response Relationship, Drug, Female, Humans, Hypercalciuria genetics, Infant, Magnesium urine, Male, Mutation, Nephrocalcinosis genetics, Potassium blood, Potassium urine, Tight Junctions metabolism, Treatment Outcome, Hydrochlorothiazide pharmacology, Hydrochlorothiazide therapeutic use, Hypercalciuria drug therapy, Loop of Henle drug effects, Magnesium blood, Membrane Proteins deficiency, Nephrocalcinosis drug therapy, Sodium Potassium Chloride Symporter Inhibitors pharmacology, Sodium Potassium Chloride Symporter Inhibitors therapeutic use

Abstract

Background: Hydrochlorothiazide (HCT) is applied in the therapy of familial hypomagnesaemia with hypercalciuria and nephrocalcinosis (FHHNC) caused by claudin-16 (CLDN16) mutation. However, the short-term efficacy of HCT to reduce hypercalciuria in FHHNC has not yet been demonstrated in a clinical trial., Methods: Four male and four female patients with FHHNC and CLDN16 mutation, under long-standing HCT therapy (0.4-1.2 mg/kg, median 0.9 mg/kg, dose according to calciuria), aged 0.7-22.4 years, were included in a clinical study to investigate the effect of HCT on calciuria. The study design consisted of three periods: continued therapy for 4 weeks, HCT withdrawal for 6 weeks and restart of therapy at the same dose for 4 weeks. Calciuria and magnesiuria were assessed weekly as Ca/creat and Mg/creat ratio, every 2 weeks in 24 h urine, and serum Mg, K and kaliuria (s-Mg, s-K and K/creat) at weeks 0, 6, 10 and 14. The data of each study period were averaged and analysed by Friedman and Wilcoxon test., Results: Ca/creat was significantly reduced by HCT (median before/at/after withdrawal 0.76/1.24/0.77 mol/mol creat; n = 8, P<0.05). The reduction of Ca/24 h by HCT was not statistically significant (0.13/0.19/0.13 mmol/kg x 24 h; n = 5). Serum Mg (0.51/0.64/0.56 mmol/l; n = 8, P<0.05) and Serum K (3.65/4.35/3.65 mmol/l; n = 8, P<0.05) were significantly higher during withdrawal. However, Mg/creat (0.98/0.90/0.90 mol/mol creat; n = 8), Mg/24 h (0.14/0.12/0.18 mmol/kg x 24h; n = 5) and K/creat (6.3/8.4/6.2 mol/mol creat; n = 8) remained statistically unchanged during withdrawal., Conclusions: We demonstrated that HCT is effective in reducing hypercalciuria due to CLDN16 mutation on a short-term basis. However, the efficacy of HCT to attenuate disease progression remains to be elucidated.

Published

2006