Molecular assembly of botulinum neurotoxin progenitor complexes.

Botulinum neurotoxin (BoNT) is produced by Clostridium botulinum and associates with nontoxic neurotoxin-associated proteins to form high-molecular weight progenitor complexes (PCs). The PCs are required for the oral toxicity of BoNT in the context of food-borne botulism and are thought to protect BoNT from destruction in the gastrointestinal tract and aid in absorption from the gut lumen. The PC can differ in size and protein content depending on the C.

Structural analysis of botulinum neurotoxin type G receptor binding .

Botulinum neurotoxin (BoNT) binds peripheral neurons at the neuromuscular junction through a dual-receptor mechanism that includes interactions with ganglioside and protein receptors. The receptor identities vary depending on BoNT serotype (A-G). BoNT/B and BoNT/G bind the luminal domains of synaptotagmin I and II, homologous synaptic vesicle proteins.

Thiacrown Pt(II) complexes with group 15 donor ligands: pentacoordination in Pt(II) complexes.

We report the synthesis and full characterization for a series of thiacrown complexes of Pt(II) incorporating the fluxional trithiacrown ligand 1,4,7-trithiacyclononane ([9]aneS3) and several group 15 donors ligands. Reaction of [Pt([9]aneS3)Cl2] with a full stoichiometric equivalent of the group 15 donor (L = 2 x AsPh3, SbPh3 or 1,2-bis(diphenylarsenio) ethane (dpae) followed by metathesis with NH4PF6 yields [Pt([9]aneS3)L](PF6)2. We also report the analogous Pd(II) complex with dpae.