Novel mutations in the thiazide-sensitive NaCl cotransporter gene in patients with Gitelman syndrome with predominant localization to the C-terminal domain

Lemmink, Henny H.; Knoers, Nine V A M; Károlyi, Lothar; Dijk, Hans van; Niaudet, Patrick; Antignac, Corinne; Guay‐Woodford, Lisa M.; Goodyer, Paul; Carel, Jean Claude; Hermes, A.; Seyberth, Hannsjörg W.; Monnens, L.A.H.; Heuvel, L.P.W.J. van den

doi:10.1046/j.1523-1755.1998.00070.x

Cited by 152 publications

(143 citation statements)

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“…The S615L identified in this study was previously described by Cruz and co-workers [18] in a study involved 36 kindreds from the United States, Canada and England and later reported in a study by Syrén et al [22]. Although the SLC12A3 variations reported in previous studies are distributed throughout the whole protein [4,23], the study of Lemmink (1998) indicates that the carboxyterminal end represents a hot spot for variations [4]. S615L is located at the intracellular C-terminal end of the SLC12A3 protein.…”

Section: Discussionsupporting

confidence: 63%

“…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%

“…S615L is located at the intracellular C-terminal end of the SLC12A3 protein. It is conceivable that structural alterations due to SLC12A3 variations in the C-terminal domain interfere with phosphorylation of the NCCT protein and as such with its regulation [4].…”

Section: Discussionmentioning

confidence: 99%

“…At present, according to the Human Gene Mutation Database (http:// www.hgmd.cf.ac.uk/), more than 100 different variants have been identified in patients with GS. They are missense, non-sense, frameshift, and splice-site variations and are scattered throughout the transporter protein with a possible clustering of variations in the carboxy-terminal tail [4].…”

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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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: 63%

Section: Discussionsupporting

confidence: 57%

Section: Discussionmentioning

confidence: 99%

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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“…In addition, we included one further variant in NCCT found once in FHS, R861C, which has previously been reported as disease-causing 23,24 and was found in 4 of our European Caucasian GS subjects (homozygous in 1). This non-conservative substitution is at a position conserved among all vertebrates.…”

Section: Mutations In Slc12a1 Slc12a3 and Kcnj1 In Fhsmentioning

confidence: 99%

Rare independent mutations in renal salt handling genes contribute to blood pressure variation

et al. 2008

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The effects of alleles in many genes are believed to contribute to common complex diseases such as hypertension. Whether risk alleles comprise a small number of common variants or many rare independent mutations at trait loci is largely unknown. We screened members of the Framingham Heart Study (FHS) for variation in three genes -SLC12A3 (NCCT), SLC12A1 (NKCC2) and KCNJ1 (ROMK)-causing rare recessive diseases featuring large reductions in blood pressure. Using comparative genomics, genetics, and biochemistry, we identified subjects with mutations proven or inferred to be functional. These mutations, all heterozygous and rare, produce clinically significant blood pressure reduction and protect from development of hypertension. Our findings implicate many rare alleles that alter renal salt handling in blood pressure variation in the general population, and identify alleles with health benefit that are nonetheless under purifying selection. These findings have implications for the genetic architecture of hypertension and other common complex traits.Correspondence to: Richard Lifton richard.lifton@yale.edu 203-737-4420 Howard Hughes Medical Institute, Yale University School of Medicine, TAC Room S341D, 1 Gilbert Street, New Haven, CT 06510, USA. Accession Numbers. GenBank mRNA sequences are as follows: NCCT/SLC12A3 (NM_000339); NKCC2/SLC12A1 (NM_000338); ROMK/KCNJ1 (NM_000220, NM_153764-7). GenBank protein sequences are as follows: SLC12A3 orthologs: Human (NP_000330), mouse (NP_062288), rat (NP_062218), rabbit (AAC33139), dog (XP_535292), cow (XP_871112), chicken (XP_414059), zebrafish (NP_001038545) and winter flounder (AAL26926); SLC12A1orthologs: Human (NP_000329), mouse (NP_899197), rat (NP_062007), rabbit (AAB03494), dog (XP_850426), chicken (XP_413814), zebrafish (NP_001002080) and Tetraodon (CAF99849); SLC12A1-3 invertebrate orthologs: S. purpuratus (XP_783014), C. elegans (NP_502704) and D. melanogaster (NP_648572); KCNJ1 orthologs: Human (NP_72245), mouse (NP_062633), rat (NP_058719), dog (XP_546403), chicken (XP_425795), cow (XP_585917), frog (AAH79788), zebrafish (XP_684541), fugu (ABB87033), C.elegans (NP_509138), S. purpuratus (XP_789112) and D. melanogaster (NP_651131); Other human paralogs: SLC12A2 (NP_001037), SLC12A4 (NP_005063), SLC12A5 (NP_065759), SLC12A6 (NP_005126) and SLC12A7 (NP_006589), KCNJ2 (NP_000882), KCNJ3 (NP_002230) KCNJ4 (NP_004972), KCNJ5 (NP_000881), KCNJ6 (NP_002231), KCNJ8 (NP_004973), KCNJ9 (NP_004974), KCNJ10 (NP_002232), KCNJ11 (NP_000516), KCNJ12 (NP_066292), KCNJ13 (NP_002233), KCNJ14 (NP_733838), KCNJ15 (NP_733933) and KCNJ16 (NP_733938). NIH Public AccessAuthor Manuscript Nat Genet. Author manuscript; available in PMC 2013 September 08. NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author ManuscriptHypertension affects 1 billion people world-wide and is a major contributor to death from stroke, myocardial infarction, end-stage renal disease and congestive heart failure. Although epidemiologic studies have demonstrated high heritability of blood pressure...

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Detecting pathogenic deep intronic variants in Gitelman syndrome

Rossanti

Horinouchi

Sakakibara

et al. 2022

American J of Med Genetics Pt A

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Gitelman syndrome (GS) is a rare, autosomal recessive, salt-losing tubulopathy caused by loss of function in the SLC12A3 gene (NM_000339.2), which encodes the natrium chloride cotransporter. The detection of homozygous or compound heterozygous SLC12A3 variants is expected in GS, but 18%-40% of patients with clinical GS carry only one mutant allele. Previous reports identified some pathogenic deep intronic variants in SLC12A3. Here, we report the screening of SLC12A3 deep intronic variants in 13 patients with suspected GS carrying one mutated SLC12A3 allele. Variant screening used the HaloPlex Target Enrichment System Kit capturing whole introns and the promotor region of SLC12A3, followed by SureCall variant analysis. Rare intronic variants (<1% frequency) were identified, and pathogenicity evaluated by the minigene system. Deep intronic variant screening detected seven rare SLC12A3 variants from six patients. Only one variant showed pathogenicity in the minigene system (c.602-16G>A, intron 4) through activation of a cryptic acceptor site. No variants were detected in the promotor region. Deep intronic screening identified only one pathogenic variant in patients with suspected GS carrying monoallelic SLC12A3 variants. Our results suggest that deep intronic variants partially explain the cause of monoallelic variants in patients with GS.

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Novel mutations in the thiazide-sensitive NaCl cotransporter gene in patients with Gitelman syndrome with predominant localization to the C-terminal domain

Cited by 152 publications

References 28 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)

Rare independent mutations in renal salt handling genes contribute to blood pressure variation

Detecting pathogenic deep intronic variants in Gitelman syndrome

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Novel mutations in the thiazide-sensitive NaCl cotransporter gene in patients with Gitelman syndrome with predominant localization to the C-terminal domain

Cited by 152 publications

References 28 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)

Rare independent mutations in renal salt handling genes contribute to blood pressure variation

Detecting pathogenic deep intronic variants in Gitelman syndrome

Contact Info

Product

Resources

About

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)