Protein scaffolds in the coupling of synaptic exocytosis and endocytosis

Haucke, Volker; Neher, Erwin; Sigrist, Stephan J.

doi:10.1038/nrn2948

Cited by 234 publications

(258 citation statements)

References 121 publications

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“…Previous analysis in this model examined the temperature-sensitive (TS) DYNAMIN mutant shibire and revealed a rapid role for endocytic mechanisms in maintaining neurotransmitter release during synaptic activity (15,16). Subsequent work has extended these findings and showed that inhibition of DYNAMIN or AP-2 disrupts fast refilling of the release-ready synaptic vesicle pool (17)(18)(19). The results reported here demonstrate colocalization of CLATHRIN and DAB at the active zone (AZ) and provide functional and ultrastructural evidence supporting their participation in rapid CLATHRIN-dependent endocytic mechanisms that may clear neurotransmitter release sites for subsequent synaptic vesicle priming and refilling of the release-ready vesicle pool.…”

mentioning

confidence: 77%

The DISABLED protein functions in CLATHRIN-mediated synaptic vesicle endocytosis and exoendocytic coupling at the active zone

Kawasaki

Iyer

Posey

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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Members of the DISABLED (DAB) family of proteins are known to play a conserved role in endocytic trafficking of cell surface receptors by functioning as monomeric CLATHRIN-associated sorting proteins that recruit cargo proteins into endocytic vesicles. Here, we report a Drosophila disabled mutant revealing a novel role for DAB proteins in chemical synaptic transmission. This mutant exhibits impaired synaptic function, including a rapid activitydependent reduction in neurotransmitter release and disruption of synaptic vesicle endocytosis. In presynaptic boutons, Drosophila DAB and CLATHRIN were highly colocalized within two distinct classes of puncta, including relatively dim puncta that were located at active zones and may reflect endocytic mechanisms operating at neurotransmitter release sites. Finally, broader analysis of endocytic proteins, including DYNAMIN, supported a general role for CLATHRIN-mediated endocytic mechanisms in rapid clearance of neurotransmitter release sites for subsequent vesicle priming and refilling of the release-ready vesicle pool.I ntensive study of chemical synaptic transmission has led to detailed molecular models of synaptic vesicle endocytosis (1-4). Ongoing efforts seek to define the underlying molecular components and interactions further as well as their spatial organization with respect to neurotransmitter release sites. The present study reveals novel molecular mechanisms and interactions in synaptic vesicle endocytosis involving a member of the DISABLED family of Phosphotyrosine Binding (PTB) domain proteins. In Drosophila, the disabled (dab) gene, the founding member of the dab gene family, was first identified in a screen for genetic modifiers of abelson (5). Although putative dab mutations were subsequently mapped to a different gene (6), recent studies have established functional interactions of Drosophila DISABLED (dDAB) and ABELSON (7). Proteins closely related to dDAB, including mouse DAB-2 (mDAB-2) and the single Caenorhabditis elegans family member ceDAB-1, function as CLATHRIN-associated adaptors in endocytic trafficking of cell surface receptors (8-10). These DABs have been shown to interact with CLATHRIN, the α-ADAPTIN (AP-2) adaptor complex, and other components of the endocytic machinery through conserved binding motifs (8-10) (Fig. 1A). Notably, mDAB-2, ceDAB-1, and dDAB share a PTB/DAB Homology (DH) domain near the N terminus (Fig. 1B), which interacts with specific vesicle cargo proteins and phosphatidylinositol-4,5-diphosphate (11, 12). Neither DAB proteins nor PTB domain interactions have been previously implicated in synaptic vesicle trafficking.The present study reveals a role for DAB proteins in synaptic vesicle endocytosis and extends previous work on interactions of endocytic and exocytic mechanisms in neurotransmitter release. Here, we use a glutamatergic neuromuscular synapse of the Drosophila adult as a model for genetic analysis of molecular mechanisms determining conserved properties of glutamatergic synapse function (13,14). Previous analysis i...

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confidence: 77%

The DISABLED protein functions in CLATHRIN-mediated synaptic vesicle endocytosis and exoendocytic coupling at the active zone

Kawasaki

Iyer

Posey

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…CME is important for both presynaptic and postsynaptic functions and both functions have been implicated in schizophrenia [73][74][75] . In presynaptic axon terminals, CME is required for the retrieval of synaptic vesicle proteins following neurotransmitter release, and for the recycling of vesicles back to the reserve pool 7 . Also, in presynaptic terminals, protein kinase C (PKC)-induced internalization of DAT from the synapse is clathrin-and dynamin-dependent 76 .…”

Section: Altered Cme May Contribute To Synaptic Pathologymentioning

confidence: 99%

“…The route taken is, at least in part, determined by members of the Rab family of GTPases 5 , which are associated with distinct endosomal populations and which are central to ensuring that vesicle cargos find their correct destinations [6][7] .…”

Section: Introductionmentioning

confidence: 99%

Hypothesis review: are clathrin-mediated endocytosis and clathrin-dependent membrane and protein trafficking core pathophysiological processes in schizophrenia and bipolar disorder?

et al. 2011

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Clathrin mediated endocytosis (CME) is the best characterized mechanism governing cellular membrane-and protein trafficking. In this hypothesis review, we integrate recent evidence implicating CME and related cellular trafficking mechanisms in the pathophysiology of psychotic disorders such as schizophrenia and bipolar disorder. The evidence includes proteomic and genomic findings implicating proteins and genes of the CME interactome. Additionally, several important candidate genes for schizophrenia, such as dysbindin, are involved in processes closely linked to CME and membrane trafficking. We discuss that key aspects of psychosis neuropathology such as synaptic dysfunction, white matter changes, and aberrant neurodevelopment are all influenced by CME, and that other cellular trafficking mechanisms previously linked to psychoses interact with CME in important ways. Furthermore, many antipsychotic drugs have been shown to affect clathrin-interacting proteins. We propose that the targeted pharmacological manipulation of CME may offer fruitful opportunities for novel treatments of schizophrenia.

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“…Similar to nerve terminals, in which endocytosis supports high rates of synaptic vesicle recycling (1,2), neuroendocrine cells undergo vigorous membrane trafficking to regulate large dense-core vesicle (LDCV) release and cellular functions. However, the mechanisms by which endocytosis influences secretory function are unclear, and the molecular nature of endocytosis in these cells remains poorly understood.…”

Section: Introductionmentioning

confidence: 99%