Toxins (Mar 2011)

Re-Assembled Botulinum Neurotoxin Inhibits CNS Functions without Systemic Toxicity

  • Bazbek Davletov,
  • Giampietro Schiavo,
  • Dhevahi Niranjan,
  • Ornella Rossetto,
  • Michael H. Hastings,
  • Marco Pirazzini,
  • Matteo Caleo,
  • Enrico Ferrari,
  • Elizabeth S. Maywood,
  • Laura Restani

DOI
https://doi.org/10.3390/toxins3040345
Journal volume & issue
Vol. 3, no. 4
pp. 345 – 355

Abstract

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The therapeutic potential of botulinum neurotoxin type A (BoNT/A) has recently been widely recognized. BoNT/A acts to silence synaptic transmission via specific proteolytic cleavage of an essential neuronal protein, SNAP25. The advantages of BoNT/A-mediated synaptic silencing include very long duration, high potency and localized action. However, there is a fear of possible side-effects of BoNT/A due to its diffusible nature which may lead to neuromuscular blockade away from the injection site. We recently developed a “protein-stapling” technology which allows re-assembly of BoNT/A from two separate fragments. This technology allowed, for the first time, safe production of this popular neuronal silencing agent. Here we evaluated the re-assembled toxin in several CNS assays and assessed its systemic effects in an animal model. Our results show that the re-assembled toxin is potent in inhibiting CNS function at 1 nM concentration but surprisingly does not exhibit systemic toxicity after intraperitoneal injection even at 200 ng/kg dose. This shows that the re-assembled toxin represents a uniquely safe tool for neuroscience research and future medical applications.

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