Mice with a Targeted Disruption of the AE2 Cl-/HCO3- Exchanger Are Achlorhydric

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2004 May 5

PMID 15123620

Citations 78

Authors

Lara R Gawenis

Clara Ledoussal

Louise M Judd

Vikram Prasad

Seth L Alper

Alan Stuart-Tilley

Alison L Woo

Christina Grisham

L Philip Sanford

Thomas Doetschman

Marian L Miller

Gary E Shull

Affiliations

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Abstract

The AE2 Cl-/HCO3- exchanger is expressed in numerous cell types, including epithelial cells of the kidney, respiratory tract, and alimentary tract. In gastric epithelia, AE2 is particularly abundant in parietal cells, where it may be the predominant mechanism for HCO3- efflux and Cl- influx across the basolateral membrane that is needed for acid secretion. To investigate the hypothesis that AE2 is critical for parietal cell function and to assess its importance in other tissues, homozygous null mutant (AE2(-/-)) mice were prepared by targeted disruption of the AE2 (Slc4a2) gene. AE2(-/-) mice were emaciated, edentulous (toothless), and exhibited severe growth retardation, and most of them died around the time of weaning. AE2(-/-) mice exhibited achlorhydria, and histological studies revealed abnormalities of the gastric epithelium, including moderate dilation of the gastric gland lumens and a reduction in the number of parietal cells. There was little evidence, however, that parietal cell viability was impaired. Ultrastructural analysis of AE2(-/-) gastric mucosa revealed abnormal parietal cell structure, with severely impaired development of secretory canaliculi and few tubulovesicles but normal apical microvilli. These results demonstrate that AE2 is essential for gastric acid secretion and for normal development of secretory canalicular and tubulovesicular membranes in mouse parietal cells.

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