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This volume focuses on the transport of medically relevant
bacterial protein toxins into mammalian cells, and on novel
pharmacological strategies to inhibit toxin uptake. The first
chapters review our current understanding of the cell-surface
receptors and cellular transport processes of Clostridium botulinum
neurotoxins, Clostridium botulinum C3 toxin, Clostridium difficile
toxins, binary clostridial enterotoxins, anthrax toxins and
diphtheria toxin. In brief, specific binding/transport (B) subunits
deliver the enzyme (A) subunits into the cytosol, where the latter
modify their substrates, producing cytotoxic effects and the
characteristic toxin-associated diseases. Key mechanisms for the
transport of the A subunits from endosomes into the cytosol and the
role of trans-membrane pores formed by the B subunits and host cell
chaperones for this process are reviewed. The book's closing
chapters focus on compounds which inhibit the transport of the A
subunits from endosomes into the cytosol and therefore might lead
to novel therapeutic strategies for toxin-associated diseases.
These substances include pharmacological inhibitors of the host
cell chaperones involved, as well as multivalent and heterocyclic
molecules that specifically block the toxins' translocation
channels. This volume offers an up-to-date resource for scientists.
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