Phosphoinositides, Major Actors in Membrane Trafficking and Lipid Signaling Pathways

Craene, Johan-Owen De; Bertazzi, Dimitri L.; Bär, Séverine; Friant, Sylvie

doi:10.3390/ijms18030634

Cited by 165 publications

(167 citation statements)

References 136 publications

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“…The PH‐Akt (GFP) probe is reactive to both PI (3,4)P2 and PI (3,4,5)P3 lipids (Manning & Cantley, ). These lipids have distinct biosynthetic and metabolic schemes (De Craene, Bertazzi, Bär, & Friant, ). To gain more insight into which of these phosphoinositides is displayed on LPVMs, we sought to determine whether the precursor lipids for PI (3,4)P2 and PI (3,4,5)P3 are also displayed on LPVs.…”

Section: Resultsmentioning

confidence: 99%

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

Zhang

Prasad

Despointes

et al. 2018

Cellular Microbiology

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Miltefosine is an important drug for the treatment of leishmaniasis; however, its mechanism of action is still poorly understood. In these studies, we tested the hypothesis that like in cancer cells, miltefosine's efficacy in leishmaniasis is due to its inhibition of Akt activation in host cells. We show using pharmacologic agents that block Akt activation by different mechanisms and also using an inducible knockdown approach that miltefosine loses its efficacy when its access to Akt1 is limited. Interestingly, limitation of Akt activation results in clearance of established Leishmania infections. We then show, using fluorophore-tagged probes that bind to phosphoinositides, that Leishmania parasitophorous vacuole membranes (LPVMs) display the relevant phosphoinositides to which Akt can be recruited and activated continuously. Taken together, we propose that the acquisition of PI(4) P and the display of PI (3,4)P2 on LPVMs initiate the machinery that supports continuous Akt activation and sensitivity to miltefosine.

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Section: Resultsmentioning

confidence: 99%

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

Zhang

Prasad

Despointes

et al. 2018

Cellular Microbiology

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“…For example, X-ray crystallography, coarse-grained MD, and reconstitution in artificial membranes have demonstrated that the Arf GTPase and its GEF Brag2 form a complex that binds to the membrane via multiple PI(4,5)P2 interaction sites (36). There is also mutational and biochemical evidence that profilin-1 and gelsolin have two PI(4,5)P2 binding sites, as do TRPV1 channels (45,62), EAG1 channels (17), and Kir2.1 (14,40).…”

Section: A Network Of Pi(45)p2 Binding Sitesmentioning

confidence: 99%

A Network of Phosphatidylinositol 4,5-bisphosphate Binding Sites Regulate Gating of the Ca²⁺-activated Cl⁻ Channel ANO1 (TMEM16A)

Jiang

Cui

et al. 2019

Preprint

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ANO1 (TMEM16A) is a Ca 2+ -activated Clchannel that regulates diverse cellular functions including fluid secretion, neuronal excitability, and smooth muscle contraction. ANO1 is activated by elevation of cytosolic Ca 2+ and modulated by phosphatidylinositol 4,5-bisphosphate (PI(4,5)P2). Here we describe a closely concerted experimental and computational study, including electrophysiology, mutagenesis, functional assays, and extended sampling of lipid-protein interactions with molecular dynamics (MD) to characterize PI(4,5)P2 binding modes and sites on ANO1. ANO1 currents in excised inside-out patches activated by 270 nM Ca 2+ at +100 mV are increased by exogenous PI(4,5)P2with an EC50 = 1.24 µM. The effect of PI(4,5)P2 is dependent on membrane voltage and Ca 2+ and is explained by a stabilization of the ANO1 Ca 2+ -bound open state. Unbiased atomistic MD simulations with 1.4% PI(4,5)P2 in a phosphatidylcholine bilayer identified 8 binding sites with significant probability of binding PI(4,5)P2. Three of these sites captured 85% of all ANO1 -PI(4,5)P2interactions. Mutagenesis of basic amino acids near the membrane-cytosol interface found three regions of ANO1 critical for PI(4,5)P2 regulation that correspond to the same three sites identified by MD. PI(4,5)P2 is stabilized by hydrogen bonding between amino acid sidechains and phosphate/hydroxyl groups on PI(4,5)P2. Binding of PI(4,5)P2 alters the position of the cytoplasmic extension of TM6, which plays a crucial role in ANO1 channel gating, and increases the accessibility of the inner vestibule to Clions. We propose a model consisting of a network of three PI(4,5)P2 binding sites at the cytoplasmic face of the membrane allosterically regulating ANO1 channel gating.of the authors and does not necessarily represent the official views of the National Institutes of Health. We also acknowledge computing resources provided by Blue Waters at National Center for Supercomputing Applications, and Extreme Science and Engineering Discovery Environment (grant MCA06N060 to ET).

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“…Intracellular trafficking events are modulated by several signaling molecules, which include members of the phosphoinositide family (3–5). In particular, the phosphatidylinositol (3,5)-bisphosphate [PI(3,5)P2] is critical for the trafficking along the endolysosomal system (6–8) and has been implicated in lysosome biogenesis and autophagy (9–12).…”

Section: Introductionmentioning

confidence: 99%

PIKfyve deficiency in myeloid cells impairs lysosomal homeostasis in macrophages and promotes systemic inflammation in mice

Min

Suzuki

Weaver

et al. 2019

Preprint

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26Macrophages are professional phagocytes that are essential for host defense and 27 tissue homeostasis. Proper membrane trafficking and degradative functions of the 28 endolysosomal system is known to be critical for the function of these cells. We have 29 found that PIKfyve, the kinase that synthesizes the endosomal phosphoinositide 30 PI(3,5)P2, is an essential regulator of lysosomal biogenesis and degradative functions 31 in macrophages. Genetically engineered mice lacking PIKfyve in their myeloid cells 32 (PIKfyve fl/fl LysM-Cre) develop diffuse tissue infiltration of foamy macrophages, 33 hepatosplenomegaly, and systemic inflammation. PIKfyve loss in macrophages causes 34 enlarged endolysosomal compartments and impairs the lysosomal degradative function. 35 Moreover, PIKfyve deficiency increases the cellular levels of lysosomal proteins. 36 Although PIKfyve deficiency reduced the activation of mTORC1 pathway and was 37 associated with increased cleavage of TFEB proteins, this does not translate into 38 transcriptional activation of lysosomal genes, suggesting that PIKfyve modulates the 39 abundance of lysosomal proteins by affecting the degradation of these proteins. Taken 40 together, our study shows that PIKfyve modulation of lysosomal degradative activity and 41 protein expression is essential to maintain lysosomal homeostasis in macrophages. 42 43 44 45 46 47 48

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Phosphoinositides, Major Actors in Membrane Trafficking and Lipid Signaling Pathways

Cited by 165 publications

References 136 publications

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

A Network of Phosphatidylinositol 4,5-bisphosphate Binding Sites Regulate Gating of the Ca²⁺-activated Cl⁻ Channel ANO1 (TMEM16A)

PIKfyve deficiency in myeloid cells impairs lysosomal homeostasis in macrophages and promotes systemic inflammation in mice

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Phosphoinositides, Major Actors in Membrane Trafficking and Lipid Signaling Pathways

Cited by 165 publications

References 136 publications

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

Leishmaniaparasitophorous vacuole membranes display phosphoinositides that create conditions for continuous Akt activation and a target for miltefosine inLeishmaniainfections

A Network of Phosphatidylinositol 4,5-bisphosphate Binding Sites Regulate Gating of the Ca2+-activated Cl− Channel ANO1 (TMEM16A)

PIKfyve deficiency in myeloid cells impairs lysosomal homeostasis in macrophages and promotes systemic inflammation in mice

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A Network of Phosphatidylinositol 4,5-bisphosphate Binding Sites Regulate Gating of the Ca²⁺-activated Cl⁻ Channel ANO1 (TMEM16A)