Insights into the structure and assembly of a bacterial cellulose secretion system

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作者
Petya Violinova Krasteva
Joaquin Bernal-Bayard
Laetitia Travier
Fernando Ariel Martin
Pierre-Alexandre Kaminski
Gouzel Karimova
Rémi Fronzes
Jean-Marc Ghigo
机构
[1] Institut Pasteur,G5 Biologie Structurale de la Sécrétion Bactérienne
[2] 25–28 rue du Docteur Roux,CNRS, UMR3528
[3] Institut Pasteur,Structural Biology of Biofilms Group
[4] 25–28 rue du Docteur Roux,Unité de Génétique des Biofilms, Département de Microbiologie
[5] Institute for Integrative Biology of the Cell (I2BC),Unité de Biologie des Bactéries Pathogènes à Gram
[6] CEA,Positif
[7] CNRS,Unité de Biochimie des Interactions Macromoléculaires
[8] Université Paris Sud,Structure et Fonction des Nanomachines Bactériennes
[9] Institut Pasteur,CNRS, UMR5234
[10] Institut Pasteur,Unité de Biologie des Infections
[11] 25–28 rue du Docteur Roux,MedILS, Mediterranean Institute for Life Sciences
[12] Institut Pasteur,undefined
[13] 25–28 rue du Docteur Roux,undefined
[14] Institut Européen de Chimie et Biologie,undefined
[15] Rue Robert Escarpit,undefined
[16] Université de Bordeaux,undefined
[17] 146 rue Léo Saignat,undefined
[18] INSERM U1117,undefined
[19] Institut Pasteur,undefined
[20] 25–28 rue du Docteur Roux,undefined
[21] Meštovićevo šetalište 45,undefined
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摘要
Secreted exopolysaccharides present important determinants for bacterial biofilm formation, survival, and virulence. Cellulose secretion typically requires the concerted action of a c-di-GMP-responsive inner membrane synthase (BcsA), an accessory membrane-anchored protein (BcsB), and several additional Bcs components. Although the BcsAB catalytic duo has been studied in great detail, its interplay with co-expressed subunits remains enigmatic. Here we show that E. coli Bcs proteins partake in a complex protein interaction network. Electron microscopy reveals a stable, megadalton-sized macromolecular assembly, which encompasses most of the inner membrane and cytosolic Bcs components and features a previously unobserved asymmetric architecture. Heterologous reconstitution and mutational analyses point toward a structure–function model, where accessory proteins regulate secretion by affecting both the assembly and stability of the system. Altogether, these results lay the foundation for more comprehensive models of synthase-dependent exopolysaccharide secretion in biofilms and add a sophisticated secretory nanomachine to the diverse bacterial arsenal for virulence and adaptation.
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