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  4. Structural Hot Spots Determine Functional Diversity of the Candida glabrata Epithelial Adhesin Family
 
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Structural Hot Spots Determine Functional Diversity of the Candida glabrata Epithelial Adhesin Family

Journal
Journal of Biological Chemistry
Journal Volume
290
Journal Issue
32
Pages
19597-19613
Date Issued
2015
Author(s)
Diderrich R
Kock M
MANUEL MAESTRE-REYNA  
Keller P
Steuber H
Rupp S
Essen L.-O
Mösch H.-U.
DOI
10.1074/jbc.M115.655654
URI
https://www.scopus.com/inward/record.uri?eid=2-s2.0-84939159972&doi=10.1074%2fjbc.M115.655654&partnerID=40&md5=a7cefc035ad9376081cf347f309977ed
https://scholars.lib.ntu.edu.tw/handle/123456789/624878
Abstract
For host colonization, the human fungal pathogen Candida glabrata is known to utilize a large family of highly related surface-exposed cell wall proteins, the lectin-like epithelial adhesins (Epas). To reveal the structure-function relationships within the entire Epa family, we have performed a large scale functional analysis of the adhesion (A) domains of 17 Epa paralogs in combination with three-dimensional structural studies of selected members with cognate ligands. Our study shows that most EpaA domains exert lectin-like functions and together recognize a wide variety of glycans with terminal galactosides for conferring epithelial cell adhesion. We further identify several conserved and variable structural features within the diverse Epa ligand binding pockets, which affect affinity and specificity. These features rationalize why mere phylogenetic relationships within the Epa family are weak indicators for functional classification and explain how Epa-like adhesins have evolved in C. glabrata and related fungal species. © 2015 by The American Society for Biochemistry and Molecular Biology, Inc.
Other Subjects
Cell adhesion; Ligands; Proteins; Yeast; Cell wall proteins; Epithelial cell adhesion; Functional classification; Functional diversity; Phylogenetic relationships; Structural feature; Structural studies; Structure-function relationship; Candida; adhesin; epithelial adhesin; galactoside; protein Epa1A; protein Epa6A; protein Epa7A; protein EpaA; unclassified drug; cell adhesion molecule; fungal protein; lectin; polysaccharide; protein binding; recombinant protein; Article; binding affinity; binding site; Candida glabrata; controlled study; host pathogen interaction; human; human cell; ligand binding; microbial adhesion; microbial diversity; nonhuman; priority journal; protein analysis; protein binding; protein domain; protein function; structure activity relation; amino acid sequence; Candida glabrata; chemical structure; chemistry; Escherichia coli; evolution; gene expression; genetic variability; genetics; metabolism; molecular genetics; phylogeny; sequence alignment; X ray crystallography; Candida glabrata; Amino Acid Sequence; Binding Sites; Biological Evolution; Candida glabrata; Cell Adhesion Molecules; Crystallography, X-Ray; Escherichia coli; Fungal Proteins; Gene Expression; Genetic Variation; Lectins; Models, Molecular; Molecular Sequence Data; Phylogeny; Polysaccharides; Protein Binding; Protein Interaction Domains and Motifs; Recombinant Proteins; Sequence Alignment
Type
journal article

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