Expression and Localization of Alpha- and Beta-carbonic Anhydrase in Helicobacter Pylori

Overview

Journal Biochim Biophys Acta

Specialties Biochemistry
Biophysics

Date 2002 Nov 26

PMID 12445482

Citations 15

Authors

Laura C Chirica

Christoffer Petersson

Marina Hurtig

Bengt-Harald Jonsson

Thomas Boren

Sven Lindskog

Affiliations

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Abstract

Helicobacter pylori, the causative agent of peptic ulcer disease, expresses two different forms of the zinc-containing enzyme carbonic anhydrase (CA) (alpha and beta), catalyzing the reversible hydration of CO(2). Presumably, the high CO(2) requirement of H. pylori implies an important role for this enzyme in the bacterial physiology. In this paper, expression of the CAs has been analyzed in three different strains of the bacterium, 26695, J99 and 17.1, and appears to be independent of CO(2) concentration in the investigated range (0.1-10%). Presence of the potent and highly specific CA inhibitor, acetazolamide, in the medium does not seem to inhibit bacterial growth at the given sulfonamide concentration. Moreover, the localization and distribution of the alpha-CA was analyzed by immunonegative staining, while SDS-digested freeze-fracture immunogold labelling was used for the beta-form of the enzyme. The latter method has the advantage of allowing assessment of protein localization to distinct cell compartments and membrane structures. The resulting electron microscopy images indicate a localization of the beta-CA in the cytosol, on the cytosolic side of the inner membrane and on the outer membrane facing the periplasmic space. The alpha-enzyme was found attached to the surface of the bacterium.

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Modak J, Modakh J, Liu Y, Machuca M, Supuran C, Roujeinikova A PLoS One. 2015; 10(5):e0127149.

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Ammonium metabolism enzymes aid Helicobacter pylori acid resistance.

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Cloning, purification and preliminary crystallographic analysis of the complex of Helicobacter pylori α-carbonic anhydrase with acetazolamide.

Modak J, Revitt-Mills S, Roujeinikova A Acta Crystallogr Sect F Struct Biol Cryst Commun. 2013; 69(Pt 11):1252-5.

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