BFA-sensitive and insensitive exocytic pathways in Entamoeba histolytica trophozoites: Their relationship to pathogenesis

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Abstract

Entamoeba histolytica manifests its pathogenicity through several cellular processes triggered by external stimuli that activate signal transduction pathways. The intense secretory activity resulting from stimulation is not correlated with a typical endoplasmic reticulum (ER) or Golgi organization, and little is known in this parasite about endocytic/exocytic pathways. The interactions of trophozoites with fibronectin (FN) and cultured mammalian cells, which elicit secretory activities, were chosen to study mechanisms that regulate cytoplamic traffic. Results showed that Brefeldin A (BFA) induced redistribution of the vesicular network recognized by antibodies against amoebic proteins PDI and ERD2. Furthermore, BFA diminished traffic to the plasma membrane of the β1 integrin-like FN receptor and the heavy subunit of the Gal/GaINAc lectin, required for adhesion to FN and target cells, respectively. However, BFA did not prevent thiol-proteinase secretion or inhibit the traffic of de novo synthesized proteinases. These data suggest that two distinct transport systems occur in E. histolytica, one similar to classical membrane protein transport and another independent of BFA and inducible by external stimuli. Actin-myosin contractility of the cortical cytoskeleton seems necessary for the final release of exported proteinases and the proper function of the surface proteins involved in adhesion.

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Manning-Cela, R., Marquez, C., Franco, E., Talamas-Rohana, P., & Meza, I. (2003, December). BFA-sensitive and insensitive exocytic pathways in Entamoeba histolytica trophozoites: Their relationship to pathogenesis. Cellular Microbiology. https://doi.org/10.1046/j.1462-5822.2003.00332.x

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