A Synaptotagmin Isoform Switch during the Development of an Identified CNS Synapse

Various Synaptotagmin (Syt) isoform genes are found in mammals, but it is unknown whether Syts can function redundantly in a given nerve terminal, or whether isoforms can be switched during the development of a nerve terminal. Here, we investigated the possibility of a developmental Syt isoform switch using the calyx of Held as a model synapse. At mature calyx synapses, fast Ca2+-driven transmitter release depended entirely on Syt2, but the release phenotype of Syt2 knockout (KO) mice was weaker at immature calyces, and absent at pre-calyceal synapses early postnatally. Instead, conditional genetic inactivation shows that Syt1 mediates fast release at pre-calyceal synapses, as well as a fast release component resistant to Syt2 deletion in immature calyces. This demonstrates a developmental Syt1-Syt2 isoform switch at an identified synapse, a mechanism that could fine-tune the speed, reliability, and plasticity of transmitter release at fast releasing CNS synapses.

A Synaptotagmin Isoform Switch during the Development of an Identified CNS Synapse

Reconstruction of nerve functional topography using recruitment curves enables selective electrical stimulation

Principles of Network Plasticity in Neocortical Microcircuits

Principles of Network Plasticity in Neocortical Microcircuits

Reconstruction of nerve functional topography using recruitment curves enables selective electrical stimulation