A Highlights from MBoC Selection: Mutations that disrupt Ca2+-binding activity endow Doc2β with novel functional properties during synaptic transmission

摘要

Double C2-domain protein (Doc2) is a Ca²⁺-binding protein implicated in asynchronous and spontaneous neurotransmitter release. Here we demonstrate that each of its C2 domains senses Ca²⁺; moreover, the tethered tandem C2 domains display properties distinct from the isolated domains. We confirm that overexpression of a mutant form of Doc2β, in which two acidic Ca²⁺ ligands in the C2A domain and two in the C2B domain have been neutralized, results in markedly enhanced asynchronous release in synaptotagmin 1–knockout neurons. Unlike wild-type (wt) Doc2β, which translocates to the plasma membrane in response to increases in [Ca²⁺]i, the quadruple Ca²⁺-ligand mutant does not bind Ca²⁺ but is constitutively associated with the plasma membrane; this effect is due to substitution of Ca²⁺ ligands in the C2A domain. When overexpressed in wt neurons, Doc2β affects only asynchronous release; in contrast, Doc2β Ca²⁺-ligand mutants that constitutively localize to the plasma membrane enhance both the fast and slow components of synaptic transmission by increasing the readily releasable vesicle pool size; these mutants also increase the frequency of spontaneous release events. Thus, mutations in the C2A domain of Doc2β that were intended to disrupt Ca²⁺ binding result in an anomalous enhancement of constitutive membrane-binding activity and endow Doc2β with novel functional properties.