Genome-Wide Analysis of Antigen 43 (Ag43) Variants: New Insights in Their Diversity, Distribution and Prevalence in Bacteria

Author:

Ageorges Valentin1ORCID,Wawrzyniak Ivan2ORCID,Ruiz Philippe1ORCID,Bicep Cédric2,Zorgani Mohamed A.1,Paxman Jason J.3ORCID,Heras Begoña3,Henderson Ian R.4,Leroy Sabine1,Bailly Xavier5,Sapountzis Panagiotis1ORCID,Peyretaillade Eric2,Desvaux Mickaël1ORCID

Affiliation:

1. INRAE, UCA, UMR0454 MEDIS, 63000 Clermont-Ferrand, France

2. UCA, CNRS, UMR6023 LMGE, 63000 Clermont-Ferrand, France

3. Department of Biochemistry and Chemistry, La Trobe Institute for Molecular Science, La Trobe University, Bundoora, VIC 3086, Australia

4. Institute for Molecular Biosciences, University of Queensland, St. Lucia, QLD 4067, Australia

5. INRAE, UCA, VetAgro Sup, UMR0346 EPIA, 63122 Saint Genes Champanelle, France

Abstract

Antigen 43 (Ag43) expression induces aggregation and biofilm formation that has consequences for bacterial colonisation and infection. Ag43 is secreted through the Type 5 subtype “a” secretion system (T5aSS) and is a prototypical member of the family of self-associating autotransporters (SAATs). As a T5aSS protein, Ag43 has a modular architecture comprised of (i) a signal peptide, (ii) a passenger domain that can be subdivided into three subdomains (SL, EJ, and BL), (iii) an autochaperone (AC) domain, and (iv) an outer membrane translocator. The cell-surface SL subdomain is directly involved in the “Velcro-handshake” mechanism resulting in bacterial autoaggregation. Ag43 is considered to have a ubiquitous distribution in E. coli genomes and many strains harbour multiple agn43 genes. However, recent phylogenetic analyses indicated the existence of four distinct Ag43 classes exhibiting different propensities for autoaggregation and interactions. Given the knowledge of the diversity and distribution of Ag43 in E. coli genomes is incomplete, we have performed a thorough in silico investigation across bacterial genomes. Our comprehensive analyses indicate that Ag43 passenger domains cluster in six phylogenetic classes associated with different SL subdomains. The diversity of Ag43 passenger domains is a result of the association of the SL subtypes with two different EJ-BL-AC modules. We reveal that agn43 is almost exclusively present among bacterial species of the Enterobacteriaceae family and essentially in the Escherichia genus (99.6%) but that it is not ubiquitous in E. coli. The gene is typically present as a single copy but up to five copies of agn43 with different combinations of classes can be observed. The presence of agn43 as well as its different classes appeared to differ between Escherichia phylogroups. Strikingly, agn43 is present in 90% of E. coli from E phylogroup. Our results shed light on Ag43 diversity and provide a rational framework for investigating its role in E. coli ecophysiology and physiopathology.

Funder

INRAE

Région Auvergne FRI-IRP

ANR

UCA (Université Clermont Auvergne) Emergence

Région Auvergne—FEDER

CPER-ARA (Contrats de Plan État Région, Auvergne-Rhône-Alpes) défi AUDACE, action ICARES

Publisher

MDPI AG

Subject

Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Computer Science Applications,Spectroscopy,Molecular Biology,General Medicine,Catalysis

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