Authors
EH Stover, KJ Borthwick, C Bavalia, N Eady, DM Fritz, N Rungroj, ABS Giersch, CC Morton, PR Axon, I Akil, EA Al-Sabban, DM Baguley, S Bianca, AYŞİN Bakkaloglu, Z Bircan, D Chauveau, MJ Clermont, A Guala, SA Hulton, H Kroes, G Li Volti, S Mir, H Mocan, A Nayir, Seza Ozen, J Rodriguez Soriano, SA Sanjad, V Tasic, CM Taylor, R Topaloglu, AN Smith, FE Karet
Publication date
2002/11/1
Journal
Journal of medical genetics
Volume
39
Issue
11
Pages
796-803
Publisher
BMJ Publishing Group Ltd
Description
Autosomal recessive distal renal tubular acidosis (rdRTA) is characterised by severe hyperchloraemic metabolic acidosis in childhood, hypokalaemia, decreased urinary calcium solubility, and impaired bone physiology and growth. Two types of rdRTA have been differentiated by the presence or absence of sensorineural hearing loss, but appear otherwise clinically similar. Recently, we identified mutations in genes encoding two different subunits of the renal α-intercalated cell’s apical H+-ATPase that cause rdRTA. Defects in the B1 subunit gene ATP6V1B1, and the a4 subunit gene ATP6V0A4, cause rdRTA with deafness and with preserved hearing, respectively.
We have investigated 26 new rdRTA kindreds, of which 23 are consanguineous. Linkage analysis of seven novel SNPs and five polymorphic markers in, and tightly linked to, ATP6V1B1 and ATP6V0A4 suggested that four families do not link to either …
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Scholar articles
EH Stover, KJ Borthwick, C Bavalia, N Eady, DM Fritz… - Journal of medical genetics, 2002