Mutations in the chloride-bicarbonate exchanger gene
            <i>AE1</i>
            cause autosomal dominant but not autosomal recessive distal renal tubular acidosis

Karet, Fiona E.; Gaínza, Francisco J.; Györy, Á. Z.; Unwin, Robert J.; Wrong, Oliver; Tanner, Michael; Nayır, Ahmet; Alpay, Harika; Santos, Fernando; Hulton, Sally‐Anne; Bakkaloğlu, Ayşı̇n; Özen, Seza; Cunningham, Miles G.; Pietro, Antonio Di; Walker, W. Gordon; Rp, Lifton

doi:10.1073/pnas.95.11.6337

Cited by 246 publications

(190 citation statements)

References 29 publications

(26 reference statements)

Supporting

Mentioning

188

Contrasting

Order By: Relevance

“…In distal RTA (dRTA), the kidney fails to produce an appropriately acid urine in the presence of systemic metabolic acidosis or after acid loading, due to impaired hydrogen ion secretion in the distal nephron. Both autosomal dominant (OMIM 179800) (1)(2)(3)(4)(5) and autosomal recessive (OMIM 602722) (6, 7) patterns have been observed in kindreds with primary dRTA, and the spectrum of clinical severity is wide. Proximal RTA (pRTA) is caused by an impairment of bicarbonate absorption in the proximal tubule (PT) and is characterized by a decreased renal HCO 3 Ϫ threshold (8).…”

mentioning

confidence: 99%

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

Dinour

Chang²,

Satoh³

et al. 2004

Journal of Biological Chemistry

165

182

View full text Add to dashboard Cite

In humans and terrestrial vertebrates, the kidney controls systemic pH in part by absorbing filtered bicarbonate in the proximal tubule via an electrogenic Na ؉ /HCO 3 ؊ cotransporter (NBCe1/SLC4A4). Recently, human genetics revealed that NBCe1 is the major renal contributor to this process. Homozygous point mutations in NBCe1 cause proximal renal tubular acidosis (pRTA), glaucoma, and cataracts (Igarashi, T., Inatomi, J., Sekine, T., Cha, S. H., Kanai, Y., Kunimi, M., Tsukamoto, K., Satoh, H., Shimadzu, M., Tozawa, F., Mori, T., Shiobara, M., Seki, G., and Endou, H. (1999) Nat. Genet. 23, 264 -266). We have identified and functionally characterized a novel, homozygous, missense mutation (S427L) in NBCe1, also resulting in pRTA and similar eye defects without mental retardation. To understand the pathophysiology of the syndrome, we expressed wild-type (WT) NBCe1 and S427L-NBCe1 in Xenopus oocytes. Function was evaluated by measuring intracellular pH (HCO 3 ؊ transport) and membrane currents using microelectrodes. HCO 3 ؊ -elicited currents for S427L were ϳ10% of WT NBCe1, and CO 2 -induced acidification was ϳ4-fold faster. Na ؉ -dependent HCO 3 ؊ transport (currents and acidification) was also ϳ10% of WT. Current-voltage (I-V) analysis reveals that S427L has no reversal potential in HCO 3 ؊ , indicating that under physiological ion gradient conditions, NaHCO 3 could not move out of cells as is needed for renal HCO 3 ؊ absorption and ocular pressure homeostasis. I-V analysis without Na ؉ further shows that the S427L-mediated NaHCO 3 efflux mode is depressed or absent. These experiments reveal that voltage-and Na ؉ -dependent transport by S427L-hkNBCe1 is unfavorably altered, thereby causing both insufficient HCO 3 ؊ absorption by the kidney (proximal RTA) and inappropriate anterior chamber fluid transport (glaucoma).

show abstract

mentioning

confidence: 99%

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

Dinour

Chang²,

Satoh³

et al. 2004

Journal of Biological Chemistry

165

182

View full text Add to dashboard Cite

show abstract

“…Human genetic studies have recently identified essential elements for pH homeostasis. To date, three genes in which mutations cause distal renal tubular acidosis have been identified (4)(5)(6). One of these genes, AE1, is essential for normal renal bicarbonate reabsorption.…”

mentioning

confidence: 99%

The B1-subunit of the H⁺ATPase is required for maximal urinary acidification

Finberg

Wagner

Bailey

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

130

163

View full text Add to dashboard Cite

The multisubunit vacuolar-type H ؉ ATPases mediate acidification of various intracellular organelles and in some tissues mediate H ؉ secretion across the plasma membrane. Mutations in the B1-subunit of the apical H ؉ ATPase that secretes protons in the distal nephron cause distal renal tubular acidosis in humans, a condition characterized by metabolic acidosis with an inappropriately alkaline urine. To examine the detailed cellular and organismal physiology resulting from this mutation, we have generated mice deficient in the B1-subunit (Atp6v1b1 ؊/؊ mice). Urine pH is more alkaline and metabolic acidosis is more severe in Atp6v1b1 ؊/؊ mice after oral acid challenge, demonstrating a failure of normal urinary acidification. In Atp6v1b1 ؊/؊ mice, the normal urinary acidification induced by a lumen-negative potential in response to furosemide infusion is abolished. After an acute intracellular acidification, Na ؉ -independent pH recovery rates of individual Atp6v1b1 ؊/؊ intercalated cells of the cortical collecting duct are markedly reduced and show no further decrease after treatment with the selective H ؉ ATPase inhibitor concanamycin. Apical expression of the alternative B-subunit isoform, B2, is increased in Atp6v1b1 ؊/؊ medulla and colocalizes with the H ؉ ATPase E-subunit; however, the greater severity of metabolic acidosis in Atp6v1b1 ؊/؊ mice after oral acid challenge indicates that the B2-subunit cannot fully functionally compensate for the loss of B1. Our results indicate that the B1 isoform is the major B-subunit isoform that incorporates into functional, plasma membrane H ؉ ATPases in intercalated cells of the cortical collecting duct and is required for maximal urinary acidification.collecting duct ͉ intercalated cell ͉ pH homeostasis ͉ renal tubular acidosis ͉ vacuolar H ϩ ATPase

show abstract

“…Two families with dominant forms of dRTA have been reported to express distinct truncation mutations in the AE1 C-terminal tail (23,24). The AE1 901X mutation was associated with normal eAE1 polypeptide abundance and function in red cells, and exhibits wild-type (wt) Cl Ϫ influx in Xenopus oocytes (25), properties shared with the dominant dRTA AE1 mutant R589H (26,27).…”

mentioning

confidence: 99%

Deficient HCO3- Transport in an AE1 Mutant with Normal Cl- Transport Can be Rescued by Carbonic Anhydrase II Presented on an Adjacent AE1 Protomer

Dahl¹,

Jiang

Chernova

et al. 2003

Journal of Biological Chemistry

View full text Add to dashboard Cite

؊ exchange by an AE1 missense mutant devoid of CA2 binding, with activity further enhanced by CA2 co-expression. The same transport-incompetent AE1 mutants failed to rescue Cl ؊ /HCO 3 ؊ exchange by the AE1 truncation mutant 896X, despite preservation of the latter's core CA2 binding site. These data increase the minimal extent of a functionally defined CA2 binding site in AE1. The inter-protomeric rescue of HCO 3 ؊ transport within the AE1 dimer shows functional proximity of the C-terminal cytoplasmic tail of one protomer to the anion translocation pathway in the adjacent protomer within the AE1 heterodimer. The data strongly support the hypothesis that an intact transbilayer anion translocation pathway is completely contained within an AE1 monomer.

show abstract

Mutations in the chloride-bicarbonate exchanger gene AE1 cause autosomal dominant but not autosomal recessive distal renal tubular acidosis

Cited by 246 publications

References 29 publications

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

The B1-subunit of the H⁺ATPase is required for maximal urinary acidification

Deficient HCO3- Transport in an AE1 Mutant with Normal Cl- Transport Can be Rescued by Carbonic Anhydrase II Presented on an Adjacent AE1 Protomer

Contact Info

Product

Resources

About

Mutations in the chloride-bicarbonate exchanger gene AE1 cause autosomal dominant but not autosomal recessive distal renal tubular acidosis

Cited by 246 publications

References 29 publications

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

A Novel Missense Mutation in the Sodium Bicarbonate Cotransporter (NBCe1/SLC4A4) Causes Proximal Tubular Acidosis and Glaucoma through Ion Transport Defects

The B1-subunit of the H+ATPase is required for maximal urinary acidification

Deficient HCO3- Transport in an AE1 Mutant with Normal Cl- Transport Can be Rescued by Carbonic Anhydrase II Presented on an Adjacent AE1 Protomer

Contact Info

Product

Resources

About

The B1-subunit of the H⁺ATPase is required for maximal urinary acidification