The tyrosine phosphatases LAR and PTPRδ act as receptors of the nidogen-tetanus toxin complex.
Sunaina SuranaDavid Villarroel-CamposElena R RhymesMaria KalyukinaChiara PanziSergey S NovoselovFederico FabrisSandy RichterMarco PirazziniGiuseppe ZanottiJames N SleighGiampietro SchiavoPublished in: The EMBO journal (2024)
Tetanus neurotoxin (TeNT) causes spastic paralysis by inhibiting neurotransmission in spinal inhibitory interneurons. TeNT binds to the neuromuscular junction, leading to its internalisation into motor neurons and subsequent transcytosis into interneurons. While the extracellular matrix proteins nidogens are essential for TeNT binding, the molecular composition of its receptor complex remains unclear. Here, we show that the receptor-type protein tyrosine phosphatases LAR and PTPRδ interact with the nidogen-TeNT complex, enabling its neuronal uptake. Binding of LAR and PTPRδ to the toxin complex is mediated by their immunoglobulin and fibronectin III domains, which we harnessed to inhibit TeNT entry into motor neurons and protect mice from TeNT-induced paralysis. This function of LAR is independent of its role in regulating TrkB receptor activity, which augments axonal transport of TeNT. These findings reveal a multi-subunit receptor complex for TeNT and demonstrate a novel trafficking route for extracellular matrix proteins. Our study offers potential new avenues for developing therapeutics to prevent tetanus and dissecting the mechanisms controlling the targeting of physiological ligands to long-distance axonal transport in the nervous system.
Keyphrases
- extracellular matrix
- binding protein
- escherichia coli
- spinal cord
- spinal cord injury
- type diabetes
- oxidative stress
- small molecule
- adipose tissue
- risk assessment
- transcription factor
- diabetic rats
- insulin resistance
- dna binding
- endothelial cells
- skeletal muscle
- protein kinase
- cancer therapy
- brain injury
- subarachnoid hemorrhage