Novel NCC mutants and functional analysis in a new cohort of patients with Gitelman syndrome

Glaudemans, Bob; Yntema, Helger G.; San‐Cristobal, Pedro; Schoots, Jeroen; Pfundt, Rolph; Kamsteeg, E.-J.; Bindels, René J. M.; Knoers, Nine V A M; Hoenderop, Joost G. J.; Hoefsloot, Lies H.

doi:10.1038/ejhg.2011.189

Cited by 66 publications

(70 citation statements)

References 30 publications

(36 reference statements)

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“…The assumption that GS is caused by a defect in the NCCT cotransporter in the renal distal tubule has been proven by the identification of numerous variations in the SLC12A3 gene in patients with GS [1,4,19,21]. In the present study the specific involvement of this cotransporter in the etiology of this disorder is further substantiated by the finding that the proband is homozygous for the S615L variation.…”

Section: Discussionsupporting

confidence: 57%

“…Onset is usually in adult life, but cases with onset in childhood are also known [1]. GS is characterized by hypomagnesemia, hypokalemia, metabolic alkalosis, hypocalciuria and hyperreninemic hyperaldosteronism.…”

Section: Introductionmentioning

confidence: 99%

“…The clinical spectrum is wide and includes: cramps, myalgies, muscle weakness, tetania, and paralysis [2]. GS is mostly caused by loss of function mutations in the solute carrier family 12, member 3 (SLC12A3 gene) which consists of 26 exons and is located on the long arm of 16 th chromosome [1]; this gene encodes the thiazide-sensitive sodium-chloride cotransporter (NCCT), expressed in the distal convoluted tubule of the kidney [3].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

Parreira¹,

Ar²,

S³

et al. 2015

Rheumatology (Sunnyvale)

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Gitelman syndrome (GS) is a rare autossomal recessive inherited tubulopathy, characterized by defective tubular reabsorption of magnesium and potassium, mostly caused by mutations in the SLC12A3 gene. The association of GS with chondrocalcinosis (CC) has been described in the literature as a typical example of hypomagnesemiainduced crystal deposition disease.We are presenting one case where the genetic cause for GS was identified in a proband with secondary early onset CC. A 60 years-old male patient with CC, hypomagnesemia and hypokalemia was identified in our hospital as a result of clinical and laboratory assessments. The clinical diagnosis of GS was performed and SLC12A3 gene was screened in the proband; variants detected were further searched in family members.The proband was homozygous for the S615L mutation; additionally, only one from the seven family members which were heterozygous presents CC. The presence of CC in two other individuals is most likely sporadic, in agreement with their advanced age.

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Section: Discussionsupporting

confidence: 57%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

Parreira¹,

Ar²,

S³

et al. 2015

Rheumatology (Sunnyvale)

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“…Gender and the type of mutation contribute to phenotypic variability, with males and patients with homozygous deep intronic mutations exhibiting a more severe phenotype [64,65]. Novel mutations are still being identified in Gitelman syndrome and these genetic defects lead to impaired production, processing, insertion or regulation of the NCC protein (type I, II, III or IV mutations) [32,113,123]. Although Gitelman syndrome is usually a relatively benign disorder that often remains subclinical for many years, a recent report suggests that the electrolyte disorders associated with Gitelman syndrome may result in chronic kidney disease and glucose intolerance [113].…”

Section: Gitelman Syndromementioning

confidence: 99%

The sodium chloride cotransporter SLC12A3: new roles in sodium, potassium, and blood pressure regulation

Moes

Lubbe

Zietse

et al. 2013

Pflugers Arch - Eur J Physiol

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SLC12A3 encodes the thiazide-sensitive sodium chloride cotransporter (NCC), which is primarily expressed in the kidney, but also in intestine and bone. In the kidney, NCC is located in the apical plasma membrane of epithelial cells in the distal convoluted tubule. Although NCC reabsorbs only 5 to 10 % of filtered sodium, it is important for the fine-tuning of renal sodium excretion in response to various hormonal and non-hormonal stimuli. Several new roles for NCC in the regulation of sodium, potassium, and blood pressure have been unraveled recently. For example, the recent discoveries that NCC is activated by angiotensin II but inhibited by dietary potassium shed light on how the kidney handles sodium during hypovolemia (high angiotensin II) and hyperkalemia. The additive effect of angiotensin II and aldosterone maximizes sodium reabsorption during hypovolemia, whereas the inhibitory effect of potassium on NCC increases delivery of sodium to the potassium-secreting portion of the nephron. In addition, great steps have been made in unraveling the molecular machinery that controls NCC. This complex network consists of kinases and ubiquitinases, including WNKs, SGK1, SPAK, Nedd4-2, Cullin-3, and Kelch-like 3. The pathophysiological significance of this network is illustrated by the fact that modification of each individual protein in the network changes NCC activity and results in salt-dependent hypotension or hypertension. This review aims to summarize these new insights in an integrated manner while identifying unanswered questions.

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“…1 To date, .160 mutations, including missense, nonsense, frameshift, and splice-site mutations, as well as gene rearrangements, have been documented in GS. 2 Among them, only a small number of missense mutations have been reported as exhibiting reduced function or as being nonfunctional. [3][4][5][6] Because the precise molecular basis of the residual missense mutations in GS remains unknown, novel approaches to clarify these issues are urgently needed.…”

mentioning

confidence: 99%

Exonic Mutations in the SLC12A3 Gene Cause Exon Skipping and Premature Termination in Gitelman Syndrome

Takeuchi

Mishima

Shima

et al. 2015

Journal of the American Society of Nephrology

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A variety of genetic backgrounds cause the loss of function of thiazide-sensitive sodium chloride cotransporter, encoded by SLC12A3, responsible for the phenotypes in Gitelman syndrome. Recently, the phenomenon of exon skipping, in which exonic mutations result in abnormal splicing, has been associated with various diseases. Specifically, mutations in exonic splicing enhancer (ESE) sequences can promote exon skipping. Here, we used a bioinformatics program to analyze 88 missense mutations in the SLC12A3 gene and identify candidate mutations that may induce exon skipping. The three candidate mutations that reduced ESE scores the most were further investigated by minigene assay, and two (p.A356V and p.M672I) caused abnormal splicing in vitro. Furthermore, we identified the p.M672I (c.2016G.A) mutation in a patient with Gitelman syndrome and found that this single nucleotide mutation causes exclusion of exon 16 in the SLC12A3 mRNA transcript. Functional analyses revealed that the protein encoded by the aberrant SLC12A3 transcript does not transport sodium. These results suggest that aberrant exon skipping is one previously unrecognized mechanism by which missense mutations in SLC12A3 can lead to Gitelman syndrome.

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Novel NCC mutants and functional analysis in a new cohort of patients with Gitelman syndrome

Cited by 66 publications

References 30 publications

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

The sodium chloride cotransporter SLC12A3: new roles in sodium, potassium, and blood pressure regulation

Exonic Mutations in the SLC12A3 Gene Cause Exon Skipping and Premature Termination in Gitelman Syndrome

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Novel NCC mutants and functional analysis in a new cohort of patients with Gitelman syndrome

Cited by 66 publications

References 30 publications

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

The sodium chloride cotransporter SLC12A3: new roles in sodium, potassium, and blood pressure regulation

Exonic Mutations in the SLC12A3 Gene Cause Exon Skipping and Premature Termination in Gitelman Syndrome

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GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)

GitelmanÃ¢ÂÂs Syndrome Associated with Chondrocalcinosis: A Case Study from the Azores Islands (Portugal)