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Effect of Epsilon Toxin–GFP on MDCK Cells and Renal Tubules In Vivo
Author(s) -
Alex Soler-Jover,
Juan Blasi,
Inma Gómez de Aranda,
Piedad Navarro,
Maryse Gibert,
Michel R. Popoff,
Mireia MartínSatué
Publication year - 2004
Publication title -
journal of histochemistry and cytochemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.971
H-Index - 124
eISSN - 1551-5044
pISSN - 0022-1554
DOI - 10.1369/jhc.4a6254.2004
Subject(s) - toxin , green fluorescent protein , recombinant dna , immunotoxin , microbiology and biotechnology , cytotoxicity , biology , kidney , in vivo , clostridium perfringens , chemistry , in vitro , biochemistry , endocrinology , bacteria , genetics , gene
Epsilon toxin (∊-toxin), produced by Clostridium perfringens types B and D, causes fatal enterotoxemia, also known as pulpy kidney disease, in livestock. Recombinant ∊-toxin–green fluorescence protein (∊-toxin–GFP) and ∊-prototoxin–GFP were successfully expressed in Escherichia coli. MTT assays on MDCK cells confirmed that recombinant ∊-toxin–GFP retained the cytotoxicity of the native toxin. Direct fluorescence analysis of MDCK cells revealed a homogeneous peripheral pattern that was temperature sensitive and susceptible to detergent. ∊-Toxin–GFP and ∊-prototoxin-GFP bound to endothelia in various organs of injected mice, especially the brain. However, fluorescence mainly accumulated in kidneys. Mice injected with ∊-toxin–GFP showed severe kidney alterations, including hemorrhagic medullae and selective degeneration of distal tubules. Moreover, experiments on kidney cryoslices demonstrated specific binding to distal tubule cells of a range of species. We demonstrate with new recombinant fluorescence tools that ∊-toxin binds in vivo to endothelial cells and renal tubules, where it has a strong cytotoxic effect. Our binding experiments indicate that an ∊-toxin receptor is expressed on renal distal tubules of mammalian species, including human. (J Histochem Cytochem 52:931–942, 2004)

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