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      Botulinum neurotoxin: a marvel of protein design.

      Annual review of biochemistry
      Botulinum Toxins, chemistry, genetics, toxicity, Endocytosis, Neurotoxins, Protein Structure, Tertiary

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          Abstract

          Botulinum neurotoxin (BoNT), the causative agent of botulism, is acknowledged to be the most poisonous protein known. BoNT proteases disable synaptic vesicle exocytosis by cleaving their cytosolic SNARE (soluble NSF attachment protein receptor) substrates. BoNT is a modular nanomachine: an N-terminal Zn(2+)-metalloprotease, which cleaves the SNAREs; a central helical protein-conducting channel, which chaperones the protease across endosomes; and a C-terminal receptor-binding module, consisting of two subdomains that determine target specificity by binding to a ganglioside and a protein receptor on the cell surface and triggering endocytosis. For BoNT, functional complexity emerges from its modular design and the tight interplay between its component modules--a partnership with consequences that surpass the simple sum of the individual component's action. BoNTs exploit this design at each step of the intoxication process, thereby achieving an exquisite toxicity. This review summarizes current knowledge on the structure of individual modules and presents mechanistic insights into how this protein machine evolved to this level of sophistication. Understanding the design principles underpinning the function of such a dynamic modular protein remains a challenging task.

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          Journal
          20233039
          10.1146/annurev.biochem.051908.125345

          Chemistry
          Botulinum Toxins,chemistry,genetics,toxicity,Endocytosis,Neurotoxins,Protein Structure, Tertiary
          Chemistry
          Botulinum Toxins, chemistry, genetics, toxicity, Endocytosis, Neurotoxins, Protein Structure, Tertiary

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