N-linked glycosylation of SV2 is required for binding and uptake of botulinum neurotoxin A.
Guorui YaoSicai ZhangStefan MahrholdKwok-Ho LamDaniel SternKarine BagramyanKay PerryMarkus KalkumAndreas RummelMin DongRongsheng JinPublished in: Nature structural & molecular biology (2016)
Botulinum neurotoxin serotype A1 (BoNT/A1), a licensed drug widely used for medical and cosmetic applications, exerts its action by invading motoneurons. Here we report a 2.0-Å-resolution crystal structure of the BoNT/A1 receptor-binding domain in complex with its neuronal receptor, glycosylated human SV2C. We found that the neuronal tropism of BoNT/A1 requires recognition of both the peptide moiety and an N-linked glycan on SV2. This N-glycan-which is conserved in all SV2 isoforms across vertebrates-is essential for BoNT/A1 binding to neurons and for its potent neurotoxicity. The glycan-binding interface on SV2 is targeted by a human BoNT/A1-neutralizing antibody currently licensed as an antibotulism drug. Our studies reveal a new paradigm of host-pathogen interactions, in which pathogens exploit conserved host post-translational modifications, thereby achieving highly specific receptor binding while also tolerating genetic changes across multiple isoforms of receptors.
Keyphrases
- binding protein
- endothelial cells
- dna binding
- transcription factor
- induced pluripotent stem cells
- healthcare
- genome wide
- dengue virus
- spinal cord
- cell surface
- pluripotent stem cells
- gene expression
- single cell
- emergency department
- cancer therapy
- spinal cord injury
- klebsiella pneumoniae
- drug delivery
- multidrug resistant
- brain injury
- anti inflammatory
- subarachnoid hemorrhage