AI Article Synopsis
- Clostridium botulinum neurotoxins, which cause botulism, are recognized as high-risk bioterrorism agents by the CDC due to their mechanism of inducing flaccid paralysis by blocking neurotransmitter release.
- A series of peptide inhibitors were developed through structure-based drug design, with the most effective peptide, RRGF, showing strong inhibition of the botulinum serotype A protease at very low concentrations.
- The research led to the creation of a new pharmacophore model based on detailed atomic interactions from cocrystal structures, providing an improved understanding of enzyme-inhibitor interactions over previous models.
Article Abstract
Clostridium botulinum neurotoxins are classified as Category A bioterrorism agents by the Centers for Disease Control and Prevention (CDC). The seven serotypes (A-G) of the botulinum neurotoxin, the causative agent of the disease botulism, block neurotransmitter release by specifically cleaving one of the three SNARE (soluble N-ethylmaleimide-sensitive factor attachment protein receptor) proteins and induce flaccid paralysis. Using a structure-based drug-design approach, a number of peptide inhibitors were designed and their inhibitory activity against botulinum serotype A (BoNT/A) protease was determined. The most potent peptide, RRGF, inhibited BoNT/A protease with an IC(50) of 0.9 µM and a K(i) of 358 nM. High-resolution crystal structures of various peptide inhibitors in complex with the BoNT/A protease domain were also determined. Based on the inhibitory activities and the atomic interactions deduced from the cocrystal structures, the structure-activity relationship was analyzed and a pharmacophore model was developed. Unlike the currently available models, this pharmacophore model is based on a number of enzyme-inhibitor peptide cocrystal structures and improved the existing models significantly, incorporating new features.
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