Molecular and functional characterization of human pendrin and its allelic variants.

[pendred syndrome]

Pendrin (SLC 26 A 4 , PDS ) is an electroneutral anion exchanger transporting I (-), Cl (-), HCO (3 )(-), OH (-), SCN (-) and formate . In the thyroid , pendrin is expressed at the apical membrane of the follicular epithelium and may be involved in mediating apical iodide efflux into the follicle ; in the inner ear , it plays a crucial role in the conditioning of the pH and ion composition of the endolymph ; in the kidney , it may exert a role in pH homeostasis and regulation of blood pressure . Mutations of the pendrin gene can lead to syndromic and non-syndromic hearing loss with EVA (enlarged vestibular aqueduct ). Functional tests of mutated pendrin allelic variants found in patients with Pendred syndrome or non-syndromic EVA (ns-EVA ) revealed that the pathological phenotype is due to the reduction or loss of function of the ion transport activity . The diagnosis of Pendred syndrome and ns-EVA can be difficult because of the presence of phenocopies of Pendred syndrome and benign polymorphisms occurring in the general population . As a consequence , defining whether or not an allelic variant is pathogenic is crucial . Recently , we found that the two parameters used so far to assess the pathogenic potential of a mutation , i .e . low incidence in the control population , and substitution of evolutionary conserved amino acids , are not always reliable for predicting the functionality of pendrin allelic variants ; actually , we identified mutations occurring with the same frequency in the cohort of hearing impaired patients and in the control group of normal hearing individuals . Moreover , we identified functional polymorphisms affecting highly conserved amino acids . As a general rule however , we observed a complete loss of function for all truncations and amino acid substitutions involving a proline . In this view , clinical and radiological studies should be combined with genetic and molecular studies for a definitive diagnosis . In performing genetic studies , the possibility that the mutation could affect regions other than the pendrin coding region , such as its promoter region and /or the coding regions of functionally related genes (FOXI 1 , KCNJ 10 ), should be taken into account . The presence of benign polymorphisms in the population suggests that genetic studies should be corroborated by functional studies ; in this context , the existence of hypo-functional variants and possible differences between the I (-)/Cl (-) and Cl (-)/HCO (3 )(-) exchange activities should be carefully evaluated .

Diseases
Validation

Diseases presenting "the presence of phenocopies of pendred syndrome" symptom

pendred syndrome

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