AUTHOR=Pérez-Reytor Diliana , Pavón Alequis , Lopez-Joven Carmen , Ramírez-Araya Sebastián , Peña-Varas Carlos , Plaza Nicolás , Alegría-Arcos Melissa , Corsini Gino , Jaña Víctor , Pavez Leonardo , del Pozo Talia , Bastías Roberto , Blondel Carlos J. , Ramírez David , García Katherine 

TITLE=Analysis of the Zonula occludens Toxin Found in the Genome of the Chilean Non-toxigenic Vibrio parahaemolyticus Strain PMC53.7

JOURNAL=Frontiers in Cellular and Infection Microbiology

VOLUME=10

YEAR=2020

URL=https://www.frontiersin.org/journals/cellular-and-infection-microbiology/articles/10.3389/fcimb.2020.00482

DOI=10.3389/fcimb.2020.00482

ISSN=2235-2988

ABSTRACT=<p><italic>Vibrio parahaemolyticus</italic> non-toxigenic strains are responsible for about 10% of acute gastroenteritis associated with this species, suggesting they harbor unique virulence factors. <italic>Zonula occludens</italic> toxin (Zot), firstly described in <italic>Vibrio cholerae</italic>, is a secreted toxin that increases intestinal permeability. Recently, we identified Zot-encoding genes in the genomes of highly cytotoxic Chilean <italic>V. parahaemolyticus</italic> strains, including the non-toxigenic clinical strain PMC53.7. To gain insights into a possible role of Zot in <italic>V. parahaemolyticus</italic>, we analyzed whether it could be responsible for cytotoxicity. However, we observed a barely positive correlation between Caco-2 cell membrane damage and Zot mRNA expression during PMC53.7 infection and non-cytotoxicity induction in response to purified PMC53.7-Zot. Unusually, we observed a particular actin disturbance on cells infected with PMC53.7. Based on this observation, we decided to compare the sequence of PMC53.7-Zot with Zot of human pathogenic species such as <italic>V. cholerae, Campylobacter concisus, Neisseria meningitidis</italic>, and other <italic>V. parahaemolyticus</italic> strains, using computational tools. The PMC53.7-Zot was compared with other toxins and identified as an endotoxin with conserved motifs in the N-terminus and a variable C-terminal region and without FCIGRL peptide. Notably, the C-terminal diversity among Zots meant that not all of them could be identified as toxins. Structurally, PMC53.7-Zot was modeled as a transmembrane protein. Our results suggested that it has partial 3D structure similarity with <italic>V. cholerae</italic>-Zot. Probably, the PMC53.7-Zot would affect the actin cytoskeletal, but, in the absence of FCIGRL, the mechanisms of actions must be elucidated.</p>