Affiliation:
1. Department of Biological Sciences University at Buffalo, Buffalo, New York 14260
Abstract
ABSTRACT
Bacterially derived exotoxins kill eukaryotic cells by inactivating factors and/or pathways that are universally conserved among eukaryotic organisms. The genes that encode these exotoxins are commonly found in bacterial viruses (bacteriophages). In the context of mammals, these toxins cause diseases ranging from cholera to diphtheria to enterohemorrhagic diarrhea. Phage-carried exotoxin genes are widespread in the environment and are found with unexpectedly high frequency in regions lacking the presumed mammalian “targets,” suggesting that mammals are not the primary targets of these exotoxins. We suggest that such exotoxins may have evolved for the purpose of bacterial antipredator defense. We show here that
Tetrahymena thermophila
, a bacterivorous predator, is killed when cocultured with bacteria bearing a Shiga toxin (Stx)-encoding temperate bacteriophage. In cocultures with
Tetrahymena
, the Stx-encoding bacteria display a growth advantage over those that do not produce Stx.
Tetrahymena
is also killed by purified Stx. Disruption of the gene encoding the StxB subunit or addition of an excess of the nontoxic StxB subunit substantially reduced Stx holotoxin toxicity, suggesting that this subunit mediates intake and/or trafficking of Stx by
Tetrahymena
. Bacterially mediated
Tetrahymena
killing was blocked by mutations that prevented the bacterial SOS response (
recA
mutations) or by enzymes that breakdown H
2
O
2
(catalase), suggesting that the production of H
2
O
2
by
Tetrahymena
signals its presence to the bacteria, leading to bacteriophage induction and production of Stx.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
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