Characterization of the Essential Transport Function of the AIDA-I Autotransporter and Evidence Supporting Structural Predictions

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Journal of Bacteriology, November 1999, p. 7014-7020, Vol. 181, No. 22
0021-9193/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

Characterization of the Essential Transport Function of the AIDA-I Autotransporter and Evidence Supporting Structural Predictions

Jochen Maurer,¹^, Joachim Jose,¹^, and Thomas F. Meyer¹^,²^,^*

Abteilung Infektionsbiologie, Max-Planck-Institut für Biologie, D-72076 Tübingen,¹ and Abteilung Molekulare Biologie, Max-Planck-Institut für Infektionsbiologie, D-10117 Berlin,² Germany

Received 22 April 1999/Accepted 5 September 1999

The current model for autodisplay suggests a mechanism that allows a passenger protein to be translocated across the outermembrane by coordinate action of a C-terminal $beta$ -barrel and itspreceding linking region. The passenger protein, linker, and $beta$ -barrelare together termed the autotransporter, while the linker and $beta$ -barrel are here referred to as the translocation unit (TU).We characterized the minimal TU necessary for autodisplay withthe adhesin-involved-in-diffuse-adherence (AIDA-I) autotransporter.The assumed $beta$ -barrel structure at the C terminus of the AIDA-Iautotransporter was studied by constructing a set of seven AIDA-I-choleratoxin B subunit fusion proteins containing various portions ofAIDA-I. Surface exposure of the cholera toxin B moiety was assessedby dot blot experiments and trypsin accessibility of the chimericproteins expressed in Escherichia coli JK321 or UT5600. Exportof cholera toxin B strictly depended on a complete predicted $beta$ -barrelregion. The absolute necessity for export of a linking regionand its influence on expression as an integral part of the TUwas also demonstrated. The different electrophoretic mobilitiesof native and denatured chimeras indicated that the proposed $beta$ -barrelresides within the C-terminal 312 amino acids of AIDA-I. Togetherthese data provide evidence for the predicted $beta$ -barrel structureand support our formerly proposed model of membrane topology ofthe AIDA-Iautotransporter.

^* Corresponding author. Mailing address: Max-Planck-Institut für Infektionsbiologie, Abteilung Molekulare Biologie, Monbijoustrasse2, D-10117 Berlin, Germany. Phone: 49 30 28 46 04 02. Fax: 4930 28 46 04 01. E-mail: meyer{at}mpiib-berlin.mpg.de.

Present address: Creatogen GmbH, D-86156 Augsburg,Germany.

Present address: Universität des Saarlandes, Pharmazeutische und Medizinische Chemie, D-66123 Saarbrücken,Germany.

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