The Ca2+ sensor synaptotagmin-1 and the SNARE complex cooperate to trigger neurotransmitter release. Structural studies elucidated three distinct synaptotagmin-1-SNARE complex binding modes involving 'polybasic', 'primary' and 'tripartite' interfaces of synaptotagmin-1. We investigated these interactions using NMR and fluorescence spectroscopy. Synaptotagmin-1 binds to the SNARE complex through the polybasic and primary interfaces in solution. Ca2+-free synaptotagmin-1 binds to SNARE complexes anchored on PIP2-containing nanodiscs. R398Q/R399Q and E295A/Y338W mutations at the primary interface, which strongly impair neurotransmitter release, disrupt and enhance synaptotagmin-1-SNARE complex binding, respectively. Ca2+ induces tight binding of synaptotagmin-1 to PIP2-containing nanodiscs, disrupting synaptotagmin-1-SNARE interactions. Specific effects of mutations in the polybasic region on Ca2+-dependent synaptotagmin-1-PIP2-membrane interactions correlate with their effects on release. Our data suggest that synaptotagmin-1 binds to the SNARE complex through the primary interface and that Ca2+ releases this interaction, inducing PIP2/membrane binding and allowing cooperation between synaptotagmin-1 and the SNAREs in membrane fusion to trigger release.
Keywords: NMR; SNARE complex; human; membrane fusion; molecular biophysics; mouse; nanodiscs; neuroscience; neurotransmitter release; rat; structural biology; synaptotagmin-1.
Inside the brain, cells called neurons relay messages from one place to another in the form of electrical signals. When an electrical signal reaches a junction between two neurons (known as a synapse) it triggers small particles called calcium ions to enter one of the cells. This influx of calcium causes vesicles to fuse with the membrane surrounding the neuron and release molecules called neurotransmitters into the small gap between the two neurons. These molecules travel across the gap to activate an electrical signal in the second neuron which then carries the message onwards. A protein known as synaptotagmin-1 senses calcium ions at synapses and works together with a group of proteins known as the SNARE complex to help vesicles fuse with the cell membrane. Previous studies have reported three different structures of synaptotagmin-1 bound to the SNARE complex in a different way. But it was unclear which of these binding states actually result in the release of neurotransmitters. To address this question, Voleti, Jaczynska and Rizo studied how and when synptotagmin-1 and the SNARE complex bind together using two approaches known as NMR spectroscopy and fluorescence spectroscopy. The experiments suggest that before calcium enters the synapse, synaptotagmin-1 is already bound to a surface on the SNARE complex. This binding inhibits the release of neurotransmitters and has been reported in previous studies. Adding calcium ions causes synaptotagmin-1 to be released from the SNARE complex. This allows synaptotagmin-1 to interact with the membrane and cooperate with the SNARE complex to trigger vesicle fusion. Finding out how neurons release neurotransmitters at synapses may help us to understand how the brain works. This could provide new insights into how defects in the synapse lead to neurological disorders, such as schizophrenia, and potentially aid the development of new treatments for such conditions.
© 2020, Voleti et al.