Clustered phosphatidylinositol 4,5 bisphosphate accumulation and ezrin phosphorylation in response to CLIC5A

Al-Momany, Abass; Li, Laiji; Alexander, R. Todd; Ballermann, Barbara J.

doi:10.1242/jcs.147744

Cited by 25 publications

(29 citation statements)

References 72 publications

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“…For example, cytoplasmic proteins such as ezrin4142, syntaxin-143 have also been described to induce or interact with PIP 2 nanoclusters. As a general mechanism, proteins with basic interfaces can recruit acidic lipids that, in turn, can facilitate recruitment and clustering of these proteins into nanodomains4445.…”

Section: Discussionmentioning

confidence: 99%

Self assembly of HIV-1 Gag protein on lipid membranes generates PI(4,5)P2/Cholesterol nanoclusters

Yandrapalli

Lubart

Tanwar

et al. 2016

Sci Rep

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The self-assembly of HIV-1 Gag polyprotein at the inner leaflet of the cell host plasma membrane is the key orchestrator of virus assembly. The binding between Gag and the plasma membrane is mediated by specific interaction of the Gag matrix domain and the PI(4,5)P2 lipid (PIP2). It is unknown whether this interaction could lead to local reorganization of the plasma membrane lipids. In this study, using model membranes, we examined the ability of Gag to segregate specific lipids upon self-assembly. We show for the first time that Gag self-assembly is responsible for the formation of PIP2 lipid nanoclusters, enriched in cholesterol but not in sphingomyelin. We also show that Gag mainly partition into liquid-disordered domains of these lipid membranes. Our work strongly suggests that, instead of targeting pre-existing plasma membrane lipid domains, Gag is more prone to generate PIP2/Cholesterol lipid nanodomains at the inner leaflet of the plasma membrane during early events of virus assembly.

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Section: Discussionmentioning

confidence: 99%

Self assembly of HIV-1 Gag protein on lipid membranes generates PI(4,5)P2/Cholesterol nanoclusters

Yandrapalli

Lubart

Tanwar

et al. 2016

Sci Rep

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“…In bone marrow-derived macrophages, CLIC4 is observed in the nucleus and its expression increases with lipopolysaccharide (LPS) stimulation (Domingo-Fernandez, Coll, Kearney, Breit, & O'Neill, 2017). Hepatocellular cancer (HCC) cell lines (HepG2, Huh7, and SNU387) have native CLIC5 in the nucleus (Flores-Tellez, Lopez, Vasquez Garzon, & Villa-Trevino, 2015) and ectopic expression in HeLa cells localizes CLIC5 to the nucleus (Al-Momany, Li, Alexander, & Ballermann, 2014). These findings indicate that CLIC1 is a native nuclear membrane channel and that other CLICs can translocate to nucleus under certain conditions or when overexpressed.…”

Section: Nucleusmentioning

confidence: 99%

Three Decades of Chloride Intracellular Channel Proteins: From Organelle to Organ Physiology

et al. 2018

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Intracellular organelles are membranous structures central for maintaining cellular physiology and the overall health of the cell. To maintain cellular function, intracellular organelles are required to tightly regulate their ionic homeostasis. Any imbalance in ionic concentrations can disrupt energy production (mitochondria), protein degradation (lysosomes), DNA replication (nucleus), or cellular signaling (endoplasmic reticulum). Ionic homeostasis is also important for volume regulation of intracellular organelles and is maintained by cation and anion channels as well as transporters. One of the major classes of ion channels predominantly localized to intracellular membranes is chloride intracellular channel proteins (CLICs). They are non-canonical ion channels with six homologs in mammals, existing as either soluble or integral membrane protein forms, with dual functions as enzymes and channels. Provided in this overview is a brief introduction to CLICs, and a summary of recent information on their localization, biophysical properties, and physiological roles. © 2018 by John Wiley & Sons, Inc.

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“…In a COS7-cell overexpression system, CLIC5A promotes the clustering of phosphatidylinositol (4,5)-bisphosphate [PtdIns(4,5)P 2 ] at the plasma membrane through its interaction with PI5P4K isoforms, which is thought to facilitate actin-dependent membrane remodeling (Al-Momany et al, 2014). Whether these interactions are direct and whether and how CLIC4 and CLIC5 are capable of regulating PIPK activity remains unclear.…”

Section: Clic Interactorsmentioning

confidence: 99%

“…Biochemical and colocalization studies suggest that, upon recruitment to the plasma membrane, both CLIC4 and CLIC5 function in a complex with ERM and/or actin-binding scaffold proteins, such as Na + /H + exchange regulatory factor 2 (NHERF2, officially known as SLC9A3R2) and the above-mentioned ERM proteins (Al-Momany et al, 2014;Berryman and Bretscher, 2000;Berryman et al, 2004;Ponsioen et al, 2009;Salles et al, 2014;Tavasoli et al, 2016a;Viswanatha et al, 2013). The association of CLIC4 and CLIC5 with the actin cytoskeleton and the finding that CLICs traffic between distinct subcellular compartments upon receptor stimulation (see below) strongly suggest a role for CLIC proteins in actin-dependent membrane trafficking.…”

Section: Clic Interactorsmentioning

confidence: 99%

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Emerging biological roles of Cl− intracellular channel proteins

Argenzio

Moolenaar

2016

Journal of Cell Science

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Cl− intracellular channels (CLICs) are a family of six evolutionary conserved cytosolic proteins that exist in both soluble and membraneassociated forms; however, their functions have long been elusive. Soluble CLICs adopt a glutathione S-transferase (GST)-fold, can induce ion currents in artificial membranes and show oxidoreductase activity in vitro, but there is no convincing evidence of CLICs having such activities in vivo. Recent studies have revealed a role for CLIC proteins in Rho-regulated cortical actin dynamics as well as vesicular trafficking and integrin recycling, the latter of which are under the control of Rab GTPases. In this Commentary, we discuss the emerging roles of CLIC proteins in these processes and the lessons learned from genetargeting studies. We also highlight outstanding questions regarding the molecular function(s) of these important but still poorly understood proteins.

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Clustered phosphatidylinositol 4,5 bisphosphate accumulation and ezrin phosphorylation in response to CLIC5A

Cited by 25 publications

References 72 publications

Self assembly of HIV-1 Gag protein on lipid membranes generates PI(4,5)P2/Cholesterol nanoclusters

Self assembly of HIV-1 Gag protein on lipid membranes generates PI(4,5)P2/Cholesterol nanoclusters

Three Decades of Chloride Intracellular Channel Proteins: From Organelle to Organ Physiology

Emerging biological roles of Cl− intracellular channel proteins

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