| Literature DB >> 31669294 |
Daniel Coronado-Velázquez1, Angélica Silva-Olivares1, Federico Castro-Muñozledo2, Luis Fernando Lares-Jiménez3, Libia Zulema Rodríguez-Anaya4, Mineko Shibayama1, Jesús Serrano-Luna5.
Abstract
Acanthamoeba spp. are free-living amoebae with a worldwide distribution. These amoebae can cause granulomatous amoebic encephalitis and amoebic keratitis in humans. Proteases are considered virulence factors in pathogenic Acanthamoeba. The objective of this study was to evaluate the behavior of Acanthamoeba mauritaniensis, a nonpathogenic amoeba. We analyzed the cytopathic effect of A. mauritaniensis on RCE1(5 T5) and MDCK cells and compared it to that of Acanthamoeba castellanii. A partial biochemical characterization of proteases was performed in total crude extracts (TCE) and conditioned medium (CM). Finally, we evaluated the effect of proteases on tight junction (TJ) proteins and the transepithelial electrical resistance of MDCK cells. The results showed that this amoeba can induce substantial damage to RCE1(5T5) and MDCK cells. Moreover, the zymograms and Azocoll assays of amoebic TCE and CM revealed different protease activities, with serine proteases being the most active. Furthermore, A. mauritaniensis induced the alteration and degradation of MDCK cell TJ proteins with serine proteases. After genotyping this amoeba, we determined that it is an isolate of Acanthamoeba genotype T4D. From these data, we suggest that A. mauritaniensis genotype T4D behaves similarly to the A. castellanii strain.Entities:
Keywords: Acanthamoeba mauritaniensis T4D; Cytopathic effect; Epithelial cells; PMSF; Proteases; Tight junction proteins
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Year: 2019 PMID: 31669294 DOI: 10.1016/j.parint.2019.102002
Source DB: PubMed Journal: Parasitol Int ISSN: 1383-5769 Impact factor: 2.230