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Please use this identifier to cite or link to this item: https://doi.org/10.1042/CS20130326
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dc.titleDetection of mutations in KLHL3 and CUL3 in families with fhht (familial hyperkalaemic hypertension or gordon's syndrome)
dc.contributor.authorGlover M.
dc.contributor.authorWare J.S.
dc.contributor.authorHenry A.
dc.contributor.authorWolley M.
dc.contributor.authorWalsh R.
dc.contributor.authorWain L.V.
dc.contributor.authorXu S.
dc.contributor.authorHoff W.G.V.
dc.contributor.authorTobin M.D.
dc.contributor.authorHall I.P.
dc.contributor.authorCook S.
dc.contributor.authorGordon R.D.
dc.contributor.authorStowasser M.
dc.contributor.authorO'shaughnessy K.M.
dc.date.accessioned2019-01-15T08:25:49Z
dc.date.available2019-01-15T08:25:49Z
dc.date.issued2014
dc.identifier.citationGlover M., Ware J.S., Henry A., Wolley M., Walsh R., Wain L.V., Xu S., Hoff W.G.V., Tobin M.D., Hall I.P., Cook S., Gordon R.D., Stowasser M., O'shaughnessy K.M. (2014). Detection of mutations in KLHL3 and CUL3 in families with fhht (familial hyperkalaemic hypertension or gordon's syndrome). Clinical Science 126 (10) : 721-726. ScholarBank@NUS Repository. https://doi.org/10.1042/CS20130326
dc.identifier.issn1435221
dc.identifier.urihttp://scholarbank.nus.edu.sg/handle/10635/150853
dc.description.abstractThe study of families with rare inherited forms of hypo- and hyper-tension has been one of the most successful strategies to probe the molecular pathophysiology of blood pressure control and has revealed dysregulation of distal nephron Na+ reabsorption to be a common mechanism. FHHt (familial hyperkalaemic hypertension; also known as Gordon's syndrome) is a salt-dependent form of hypertension caused by mutations in the regulators of the thiazide-sensitive Na+-CI-transporter NCC [also known as SLC12A3 (solute carrier family 12 member 3)] and is effectively treated by thiazide diuretics and/or dietary salt restriction. Variation in at least four genes can cause FHHt, including WNK1 [With No lysine (=K) 1] and WNK4, KLHL3 (kelch-like family member 3), and CUL3 (cullin 3). In the present study we have identified novel disease-causing variants in CUL3 and KLHL3 segregating in 63% of the pedigrees with previously unexplained FHHt, confirming the importance of these recently described FHHt genes. We have demonstrated conclusively, in two unrelated affected individuals, that rare intronic variants in CUL3 cause the skipping of exon 9 as has been proposed previously. KLHL3 variants all occur in kelch-repeat domains and so probably disrupt WNK complex binding. We have found no evidence of any plausible disease-causing variants within SLC4A8 (an alternative thiazide-sensitive sodium transporter) in this population. The results of the present study support the existing evidence that the CUL3 and KLHL3 gene products are physiologically important regulators of thiazide-sensitive distal nephron NaCl reabsorption, and hence potentially interesting novel anti-hypertensive drug targets. As a third of our non-WNK FHHt families do not have plausible CUL3 or KLHL3 variants, there are probably additional, as yet undiscovered, regulators of the thiazide-sensitive pathways. ? The Authors Journal compilation. ? 2014 Biochemical Society.
dc.sourceScopus
dc.subjectDiuretic
dc.subjectGordon's syndrome
dc.subjectHyperkalaemia
dc.subjectHypertension
dc.subjectPseudohypoaldosteronism
dc.subjectThiazide
dc.typeArticle
dc.contributor.departmentDUKE-NUS MEDICAL SCHOOL
dc.description.doi10.1042/CS20130326
dc.description.sourcetitleClinical Science
dc.description.volume126
dc.description.issue10
dc.description.page721-726
dc.description.codenCSCIA
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