AI Article Synopsis

  • AISs are crucial for generating action potentials and maintaining protein, lipid, and organelle distribution in neurons, but their stabilization and mechanisms of neuronal polarity are not fully understood.
  • Researchers used advanced techniques like proximity biotinylation and mass spectrometry to identify proteins associated with the AIS, revealing many previously unidentified biotinylated proteins.
  • The study highlights the role of these proteins in interacting with known AIS components and how their absence can disrupt AIS structure and function, offering new insights into AIS organization and stability.

Article Abstract

Axon initial segments (AISs) generate action potentials and regulate the polarized distribution of proteins, lipids, and organelles in neurons. While the mechanisms of AIS Na and K channel clustering are understood, the molecular mechanisms that stabilize the AIS and control neuronal polarity remain obscure. Here, we use proximity biotinylation and mass spectrometry to identify the AIS proteome. We target the biotin-ligase BirA* to the AIS by generating fusion proteins of BirA* with NF186, Ndel1, and Trim46; these chimeras map the molecular organization of AIS intracellular membrane, cytosolic, and microtubule compartments. Our experiments reveal a diverse set of biotinylated proteins not previously reported at the AIS. We show many are located at the AIS, interact with known AIS proteins, and their loss disrupts AIS structure and function. Our results provide conceptual insights and a resource for AIS molecular organization, the mechanisms of AIS stability, and polarized trafficking in neurons.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6941957PMC
http://dx.doi.org/10.1038/s41467-019-13658-5DOI Listing

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