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Type II (proteic) toxin-antitoxin (TA) operons are widely spread in bacteria and archaea. They are organized as operons in which, usually, the antitoxin gene precedes the cognate toxin gene. The antitoxin generally acts as a transcriptional self-repressor, whereas the toxin acts as a co-repressor, both proteins constituting a harmless complex. When bacteria encounter a stressful environment, TAs are triggered. The antitoxin protein is unstable and will be degraded by host proteases, releasing the free toxin to halt essential processes. The result is a cessation of cell growth or even death. Because of their ubiquity and the essential processes targeted, TAs have been proposed as good candidates for development of novel antimicrobials. We discuss here the possible druggability of TAs as antivirals and antibacterials, with focus on the potentials and the challenges that their use may find in the 'real' world. We present strategies to develop TAs as antibacterials in view of novel technologies, such as the use of very small molecules (fragments) as inhibitors of protein-protein interactions. Appropriate fragments could disrupt the T:A interfaces leading to the release of the targeted TA pair. Possible ways of delivery and formulation of Tas are also discussed.
Drug discovery, Bacterial Toxins, Review Article, Bacterial Infections, Antivirals, Antiviral Agents, Anti-Bacterial Agents, Toxin-antitoxin operons, Virus Diseases, Drug delivery, Antibacterials, Animals, Humans, Inhibitors of protein-protein interactions, Antitoxins
Drug discovery, Bacterial Toxins, Review Article, Bacterial Infections, Antivirals, Antiviral Agents, Anti-Bacterial Agents, Toxin-antitoxin operons, Virus Diseases, Drug delivery, Antibacterials, Animals, Humans, Inhibitors of protein-protein interactions, Antitoxins
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| influence This indicator reflects the overall/total impact of an article in the research community at large, based on the underlying citation network (diachronically). | Top 10% | |
| impulse This indicator reflects the initial momentum of an article directly after its publication, based on the underlying citation network. | Top 1% |
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