Journal
NATURE
Volume 505, Issue 7481, Pages 108-+Publisher
NATURE PUBLISHING GROUP
DOI: 10.1038/nature12732
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Funding
- UCB Pharma, UCB NewMedicines
- Swiss National Science Foundation [310030B_138659]
- Netherlands Organization for Scientific Research (NWO-ALW-VICI)
- Netherlands Organization for Health Research and Development (ZonMW-TOP)
- Swiss National Science Foundation (SNF) [310030B_138659] Funding Source: Swiss National Science Foundation (SNF)
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Botulinum neurotoxin A (BoNT/A) belongs to the most dangerous class of bioweapons(1). Despite this, BoNT/A is used to treat a wide range of common medical conditions such as migraines and a variety of ocular motility and movement disorders(2). BoNT/A is probably best known for its use as an antiwrinkle agent in cosmetic applications (including Botox and Dysport)(3). BoNT/A application causes long-lasting flaccid paralysis of muscles through inhibiting the release of the neurotransmitter acetylcholine by cleaving synaptosomal-associated protein 25 (SNAP-25) within presynaptic nerve terminals(4). Two types of BoNT/A receptor have been identified, both of which are required for BoNT/A toxicity and are therefore likely to cooperate with each other(5): gangliosides and members of the synaptic vesicle glycoprotein 2 (SV2) family, which are putative transporter proteins that are predicted to have 12 transmembrane domains, associate with the receptor-binding domain of the toxin(5). Recently, fibroblast growth factor receptor 3 (FGFR3) has also been reported to be a potential BoNT/A receptor(6). In SV2 proteins, the BoNT/A-binding site has been mapped to the luminal domain(7), but the molecular details of the interaction between BoNT/A and SV2 are unknown. Here we determined the high-resolution crystal structure of the BoNT/A receptor-binding domain (BoNT/A-RBD) in complex with the SV2C luminal domain (SV2C-LD). SV2C-LD consists of a right-handed, quadrilateral beta-helix that associates with BoNT/A-RBD mainly through backbone-to-backbone interactions at open beta-strand edges, in a manner that resembles the inter-strand interactions in amyloid structures. Competition experiments identified a peptide that inhibits the formation of the complex. Our findings provide a strong platform for the development of novel antitoxin agents and for the rational design of BoNT/A variants with improved therapeutic properties.
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