AI Article Synopsis

  • The text discusses the role of synaptic SNARE proteins in the process of neurotransmission, specifically how their folding and assembly facilitate the fusion of vesicles with plasma membranes.
  • It explains that the first step in this process involves the formation of a t-SNARE complex on the target membrane, which is essential but prone to misfolding.
  • Using single-molecule studies, the research modeled the t-SNARE complex structure and revealed how it transitions between states, ultimately enabling efficient synaptic vesicle fusion.

Article Abstract

Synaptic soluble N-ethylmaleimide-sensitive factor attachment protein receptors (SNAREs) couple their stepwise folding to fusion of synaptic vesicles with plasma membranes. In this process, three SNAREs assemble into a stable four-helix bundle. Arguably, the first and rate-limiting step of SNARE assembly is the formation of an activated binary target (t)-SNARE complex on the target plasma membrane, which then zippers with the vesicle (v)-SNARE on the vesicle to drive membrane fusion. However, the t-SNARE complex readily misfolds, and its structure, stability, and dynamics are elusive. Using single-molecule force spectroscopy, we modeled the synaptic t-SNARE complex as a parallel three-helix bundle with a small frayed C terminus. The helical bundle sequentially folded in an N-terminal domain (NTD) and a C-terminal domain (CTD) separated by a central ionic layer, with total unfolding energy of ∼17 kT, where k is the Boltzmann constant and T is 300 K. Peptide binding to the CTD activated the t-SNARE complex to initiate NTD zippering with the v-SNARE, a mechanism likely shared by the mammalian uncoordinated-18-1 protein (Munc18-1). The NTD zippering then dramatically stabilized the CTD, facilitating further SNARE zippering. The subtle bidirectional t-SNARE conformational switch was mediated by the ionic layer. Thus, the t-SNARE complex acted as a switch to enable fast and controlled SNARE zippering required for synaptic vesicle fusion and neurotransmission.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5167175PMC
http://dx.doi.org/10.1073/pnas.1605748113DOI Listing

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