Familial pure proximal renal tubular acidosis--a clinical and genetic study

doi:10.1093/ndt/gfm583

NDT Advance Access originally published online on September 19, 2007
Nephrology Dialysis Transplantation 2008 23(4):1211-1215; doi:10.1093/ndt/gfm583

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Familial pure proximal renal tubular acidosis—a clinical and genetic study

Ze’ev Katzir¹, Dganit Dinour², Haike Reznik-Wolf², Andrea Nissenkorn³ and Eliezer Holtzman²

¹ Nephrology and Hypertension Institute, Pediatric Nephrology Services, E. Wolfson Medical Center, Holon ² Nephrology and Hypertension Institute, Chaim Sheba Medical Center, Tel Hashomer ³ Department of Pediatrics, E. Wolfson Medical Center, Holon, Israel

Ze’ev Katzir, Pediatric Nephrology Services, E. Wolfson Medical Center, Holon, Israel. E-mail: katzir{at}wolfson.health.gov.il

Abstract

Background. Inherited proximal renal tubular acidosis (pRTA)is commonly associated with more generalized proximal tubulardysfunctions and occasionally with other organ system defects.Inherited combined pRTA and distal RTA with osteopetrosis andpure pRTA associated with ocular abnormalities, a rare diseasewhich has been recently described. Only one family with pureisolated pRTA has been reported so far and the genetic causefor this disease is unknown.

Objectives. We report a unique family with isolated pRTA. Theaim of the project was to define the phenotype and to try tofind the gene defect causing the disease.

Methods. Clinical and metabolic evaluation of all family memberswas performed and a family pedigree was constructed. DNA wasextracted from blood samples of affected and unaffected familymembers. We amplified by PCR and sequenced the coding areasand splice-sites of the genes that contribute to HCO^–₃reclamation in the proximal tubule. The genes studied were asfollows: CA II, CA IV, CA XIV, NCB1, Na⁺/H⁺ exchanger (NHE)-3,NHE-8, the regulatory proteins of NHE3, NHRF1 and NHRF2 andthe Cl^–/HCO^–₃ exchanger, SLC26A6.

Results. The father and all four children had RTA with bloodHCO^–₃ levels of 11–14 meq/l and urine pH of 5.3–5.4.Increased HCO^–₃ fractional excretion after bicarbonateloading to 40–60% confirmed the diagnosis pRTA. No othertubular dysfunction was found, and no organ system dysfunctionwas detected, besides short stature. No mutation was found inall candidate genes studied.

Conclusions. We presented a second family in the literaturewith familial isolated pure pRTA. The mode of inheritance iscompatible with an autosomal dominant disease. Because of thesmall size of the family, wide genome search was not applicableand the gene candidate approach was chosen. Nine important candidategenes were extensively studied but the molecular basis of thedisease was not yet found and genotyping nine important genecandidates were negative.

Received for publication: 21. 5.06
Accepted in revised form: 31. 7.07

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