| Literature DB >> 28771254 |
Smail Hadj-Rabia1,2, Gaelle Brideau3, Yasser Al-Sarraj4, Rachid C Maroun5, Marie-Lucile Figueres3, Stéphanie Leclerc-Mercier2,6, Eric Olinger7, Stéphanie Baron3,8, Catherine Chaussain9, Dominique Nochy10, Rowaida Z Taha4, Bertrand Knebelmann11, Vandana Joshi5, Patrick A Curmi5, Marios Kambouris4,12,13, Rosa Vargas-Poussou3,14, Christine Bodemer1,2, Olivier Devuyst7, Pascal Houillier3,8, Hatem El-Shanti4,15,16.
Abstract
PurposeWe aimed to identify the genetic cause to a clinical syndrome encompassing hypohidrosis, electrolyte imbalance, lacrimal gland dysfunction, ichthyosis, and xerostomia (HELIX syndrome), and to comprehensively delineate the phenotype.MethodsWe performed homozygosity mapping, whole-genome sequencing, gene sequencing, expression studies, functional tests, protein bioinformatics, and histological characterization in two unrelated families with HELIX syndrome.ResultsWe identified biallelic missense mutations (c.386C>T, p.S131L and c.2T>C, p.M1T) in CLDN10B in six patients from two unrelated families. CLDN10B encodes Claudin-10b, an integral tight junction (TJ) membrane-spanning protein expressed in the kidney, skin, and salivary glands. All patients had hypohidrosis, renal loss of NaCl with secondary hyperaldosteronism and hypokalemia, as well as hypolacrymia, ichthyosis, xerostomia, and severe enamel wear. Functional testing revealed that patients had a decreased NaCl absorption in the thick ascending limb of the loop of Henle and a severely decreased secretion of saliva. Both mutations resulted in reduced or absent Claudin-10 at the plasma membrane of epithelial cells.ConclusionCLDN10 mutations cause a dysfunction in TJs in several tissues and, subsequently, abnormalities in renal ion transport, ectodermal gland homeostasis, and epidermal integrity.Entities:
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Year: 2017 PMID: 28771254 DOI: 10.1038/gim.2017.71
Source DB: PubMed Journal: Genet Med ISSN: 1098-3600 Impact factor: 8.822