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Open AccessJournal ArticleDOI

Phospholipase D Stimulates Release of Nascent Secretory Vesicles from the trans-Golgi Network

TLDR
It is demonstrated that immunoaffinity-purified human PLD1 stimulated nascent secretory vesicle budding from the TGN and ARF-1 stimulated endogenous PLD activity in Golgi membranes approximately threefold and this activation correlated with its enhancement of vesicles budding.
Abstract
Phospholipase D (PLD) is a phospholipid hydrolyzing enzyme whose activation has been implicated in mediating signal transduction pathways, cell growth, and membrane trafficking in mammalian cells. Several laboratories have demonstrated that small GTP-binding proteins including ADP-ribosylation factor (ARF) can stimulate PLD activity in vitro and an ARF-activated PLD activity has been found in Golgi membranes. Since ARF-1 has also been shown to enhance release of nascent secretory vesicles from the TGN of endocrine cells, we hypothesized that this reaction occurred via PLD activation. Using a permeabilized cell system derived from growth hormone and prolactin-secreting pituitary GH3 cells, we demonstrate that immunoaffinity-purified human PLD1 stimulated nascent secretory vesicle budding from the TGN approximately twofold. In contrast, a similarly purified but enzymatically inactive mutant form of PLD1, designated Lys898Arg, had no effect on vesicle budding when added to the permeabilized cells. The release of nascent secretory vesicles from the TGN was sensitive to 1% 1-butanol, a concentration that inhibited PLD-catalyzed formation of phosphatidic acid. Furthermore, ARF-1 stimulated endogenous PLD activity in Golgi membranes approximately threefold and this activation correlated with its enhancement of vesicle budding. Our results suggest that ARF regulation of PLD activity plays an important role in the release of nascent secretory vesicles from the TGN.

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Sorting and storage during secretory granule biogenesis: looking backward and looking forward.

TL;DR: This review summarizes and evaluates current information about how secretory proteins are thought to be sorted for the regulated secretory pathway and how these activities are positioned with respect to other post-Golgi sorting events that must occur in parallel.
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PHOSPHOINOSITIDE LIPIDS AS SIGNALING MOLECULES: Common Themes for Signal Transduction, Cytoskeletal Regulation, and Membrane Trafficking

TL;DR: Common themes of localized signal generation and the spatially localized recruitment of effector proteins appear to underlie mechanisms employed in signal transduction, cytoskeletal, and membrane trafficking events.
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Neuropathology, biochemistry, and biophysics of α-synuclein aggregation

TL;DR: This paper provides an overview of the biochemistry, biophysics, and neuropathology of α‐synuclein aggregation and possesses remarkable conformational plasticity.
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Synucleins in synaptic plasticity and neurodegenerative disorders.

TL;DR: A hypothesis whereby synuclein supports localized, experience‐dependent turnover of synaptic membranes may be important for lifelong learning and memory functions and may be especially vulnerable to disruption in aging‐associated neurodegenerative diseases is outlined.
Journal ArticleDOI

Phospholipase D: a lipid centric review.

TL;DR: This review focuses on the lipid precursors and products of mammalian PLD metabolism, especially phosphatidic acid and the roles this lipid performs in the mediation of the functions of PLD.
References
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Journal ArticleDOI

Involvement of Ral GTPase in v-Src-induced phospholipase D activation

TL;DR: RalA is involved in the tyrosine kinase activation of PLD through its unique N terminus, and that PLD is a downstream target of a Ras/Ral GTPase cascade.
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Activation of rat liver phospholipase D by the small GTP-binding protein RhoA.

TL;DR: Findings support a role for GTP-binding proteins of the Rho family in the activation of membrane-associated phospholipase D and implicate RhoA as the major protein involved.
Journal ArticleDOI

Signal transduction and membrane traffic: The PITP/phosphoinositide connection

TL;DR: It is shown that Golgi membranes must maintain a relatively high Ptdlns/PtdCho ratio to sustain normal secretory activity and the possibility that the role played by PITP in polyphosphoinositide synthesis may also explain its involvement in intracellular vesicular traffic.
Journal ArticleDOI

ARF: a key regulatory switch in membrane traffic and organelle structure

TL;DR: The small GTP-binding protein ADP ribosylation factor regulates, through a GTP cycle, the reversible binding of cytosolic coat proteins to Golgi membranes, and controls the production and lifetime of coated-membrane structures.
Journal ArticleDOI

Arf proteins: the membrane traffic police?

TL;DR: Can a single molecular mechanism link all the activities of Arf proteins?
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