Presynaptic targeting of botulinum neurotoxin type A requires a tripartite PSG‐Syt1‐SV2 plasma membrane nanocluster for synaptic vesicle entry.

The unique nerve terminal targeting of botulinum neurotoxin type A (BoNT/A) is due to its capacity to bind two receptors on the neuronal plasma membrane: polysialoganglioside (PSG) and synaptic vesicle glycoprotein 2 (SV2). Whether and how PSGs and SV2 may coordinate other proteins for BoNT/A recruitment and internalization remains unknown. Here, we demonstrate that the targeted endocytosis of BoNT/A into synaptic vesicles (SVs) requires a tripartite surface nanocluster. Live‐cell super‐resolution imaging and electron microscopy of catalytically inactivated BoNT/A wildtype and receptor‐binding‐deficient mutants in cultured hippocampal neurons demonstrated that BoNT/A must bind coincidentally to a PSG and SV2 to target synaptic vesicles. We reveal that BoNT/A simultaneously interacts with a preassembled PSG‐synaptotagmin‐1 (Syt1) complex and SV2 on the neuronal plasma membrane, facilitating Syt1‐SV2 nanoclustering that controls endocytic sorting of the toxin into synaptic vesicles. Syt1 CRISPRi knockdown suppressed BoNT/A‐ and BoNT/E‐induced neurointoxication as quantified by SNAP‐25 cleavage, suggesting that this tripartite nanocluster may be a unifying entry point for selected botulinum neurotoxins that hijack this for synaptic vesicle targeting. Synopsis: Synaptic targeting of botulinum neurotoxins is mediated by interaction with toxin‐type‐specific receptors and complex gangliosides, such as polysialoganglioside (PSG). This study shows that botulinum neurotoxin type A (BoNT/A) uptake and sorting into synaptic vesicles requires a tripartite nanocluster on the neuronal plasma membrane. Live‐cell super‐resolution and electron microscopy in primary hippocampal neurons shows BoNT/A synaptic vesicle targeting depends on a tripartite PSG‐synaptotagmin 1 (Syt1)‐synaptic vesicle protein 2 (SV2) nanocluster on the plasma membrane.Coincidental binding of BoNT/A to a preassembled PSG‐Syt1 complex and SV2 facilitates Syt1‐SV2 nanoclustering on the neuronal plasma membrane and endocytic sorting of the toxin into synaptic vesicles.Syt1 is required for the BoNT/A and BoNT/E neurointoxication, suggesting a general mechanism of entry for clostridial botulinum neurotoxins. [ABSTRACT FROM AUTHOR]