Publication | Open Access
SMN Requirement for Synaptic Vesicle, Active Zone and Microtubule Postnatal Organization in Motor Nerve Terminals
88
Citations
62
References
2011
Year
Synaptic TransmissionMicrotubule MaturationCytoskeletonNeurotransmissionPeripheral NerveCellular NeurobiologyPeripheral Nervous SystemSocial SciencesNeuromuscular JunctionNeurologyActive ZoneNeurogeneticsMotor Nerve TerminalsNervous SystemSurvival Motor NeuronSynaptic PlasticityNeurodegenerative DiseasesDevelopmental BiologyNeurophysiologyNeuroanatomyMotor SystemDegenerative DiseaseNeuromuscular DevelopmentSmn RequirementSpinal Muscular AtrophyNeuroscienceMolecular NeurobiologyMedicine
Low levels of the Survival Motor Neuron (SMN) protein produce Spinal Muscular Atrophy (SMA), a severe monogenetic disease in infants characterized by muscle weakness and impaired synaptic transmission. We report here severe structural and functional alterations in the organization of the organelles and the cytoskeleton of motor nerve terminals in a mouse model of SMA. The decrease in SMN levels resulted in the clustering of synaptic vesicles (SVs) and Active Zones (AZs), reduction in the size of the readily releasable pool (RRP), and the recycling pool (RP) of synaptic vesicles, a decrease in active mitochondria and limiting of neurofilament and microtubule maturation. We propose that SMN is essential for the normal postnatal maturation of motor nerve terminals and that SMN deficiency disrupts the presynaptic organization leading to neurodegeneration.
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