Abstract | AIMS: METHODS: Nine dRTA families from Cyprus and one from Greece were analyzed for mutations in ATP6V1B1 gene by DNA resequencing and PCR-RFLPs. Clinical diagnosis was performed by standard criteria. Prenatal diagnosis was performed for one Cypriot family. RESULTS: Results show that 7/9 dRTA cases in Cyprus are caused by 229+1G>T and R157C founder mutations in ATP6V1B1 gene. 229+1G>T mutation was estimated to be older than 400 years. No genotype- phenotype correlation was found with SNHL. A known (L81P) and a novel mutation (912delT) were found in the Greek family. Prenatal diagnosis was performed for one Cypriot family, after parents' demand, showing that the embryo was a heterozygous carrier. CONCLUSION: Existence of only two ATP6V1B1 mutations in the Cypriot population is a diagnostic advantage. The age of onset of SNHL varies in our patients and probably is not related to ATP6V1B1 genotypes. Effective therapy for most of the syndrome symptoms is not satisfactory for some parents who choose prenatal diagnosis to ensure their child's health.
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Authors | Avraam Elia, Konstantinos Voskarides, Panayiota Demosthenous, Aikaterini Michalopoulou, Maria-Adamantia Malliarou, Eleni Georgaki, Yiannis Athanasiou, Charalambos Patsias, Alkis Pierides, Constantinos Deltas |
Journal | Nephron. Clinical practice
(Nephron Clin Pract)
Vol. 117
Issue 3
Pg. c206-12
( 2011)
ISSN: 1660-2110 [Electronic] Switzerland |
PMID | 20805693
(Publication Type: Comparative Study, Journal Article, Research Support, Non-U.S. Gov't)
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Copyright | Copyright © 2010 S. Karger AG, Basel. |
Chemical References |
- ATP6V1B1 protein, human
- Vacuolar Proton-Translocating ATPases
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Topics |
- Acidosis, Renal Tubular
(diagnosis, epidemiology, genetics)
- Adult
- Child
- Child, Preschool
- Cyprus
(epidemiology)
- Female
- Founder Effect
- Humans
- Infant
- Male
- Mutation
(genetics)
- Pregnancy
- Pregnancy Complications
(diagnosis, genetics)
- Prenatal Diagnosis
(methods)
- Vacuolar Proton-Translocating ATPases
(genetics)
- Young Adult
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