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Dive into the research topics where Alicia Alonso is active.

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Featured researches published by Alicia Alonso.


Bioscience Reports | 2000

Membrane Fusion Induced by Phospholipase C and Sphingomyelinases

Félix M. Goñi; Alicia Alonso

In the past decade lipid vesicle fusion induced by either bacterial PC-preferring phospholipase C, phosphatidylinositol-specific phospholipase C, sphingomyelinase, or a combination of phospholipase C and sphingomyelinase has been demonstrated. In the present paper, the experimental evidence is reviewed, and discussed in terms of the underlying molecular mechanisms of fusion, and of the possible physiological relevance of these findings.


Biophysical Journal | 2012

Accumulated Bending Energy Elicits Neutral Sphingomyelinase Activity in Human Red Blood Cells

David Jesús Palma López; Meritxell Egido-Gabás; Iván López-Montero; Jon V. Busto; Josefina Casas; Marie Garnier; Francisco Monroy; Banafshé Larijani; Félix M. Goñi; Alicia Alonso

We propose that accumulated membrane bending energy elicits a neutral sphingomyelinase (SMase) activity in human erythrocytes. Membrane bending was achieved by osmotic or chemical processes, and SMase activity was assessed by quantitative thin-layer chromatography, high-performance liquid chromatography, and electrospray ionization-mass spectrometry. The activity induced by hypotonic stress in erythrocyte membranes had the pH dependence, ion dependence, and inhibitor sensitivity of mammalian neutral SMases. The activity caused a decrease in SM contents, with a minimum at 6 min after onset of the hypotonic conditions, and then the SM contents were recovered. We also elicited SMase activity by adding lysophosphatidylcholine externally or by generating it with phospholipase A(2). The same effect was observed upon addition of chlorpromazine or sodium deoxycholate at concentrations below the critical micellar concentration, and even under hypertonic conditions. A unifying factor of the various agents that elicit this SMase activity is the accumulated membrane bending energy. Both hypo-and hypertonic conditions impose an increased curvature, whereas the addition of surfactants or phospholipase A(2) activation increases the outer monolayer area, thus leading to an increased bending energy. The fact that this latent SMase activity is tightly coupled to the membrane bending properties suggests that it may be related to the general phenomenon of stress-induced ceramide synthesis and apoptosis.


Biophysical Journal | 2014

A Cholesterol Recognition Motif in Human Phospholipid Scramblase 1

Itziar M.D. Posada; Jacques Fantini; F. Xabier Contreras; Francisco J. Barrantes; Alicia Alonso; Félix M. Goñi

Human phospholipid scramblase 1 (SCR) catalyzes phospholipid transmembrane (flip-flop) motion. This protein is assumed to bind the membrane hydrophobic core through a transmembrane domain (TMD) as well as via covalently bound palmitoyl residues. Here, we explore the possible interaction of the SCR TMD with cholesterol by using a variety of experimental and computational biophysical approaches. Our findings indicate that SCR contains an amino acid segment at the C-terminal region that shows a remarkable affinity for cholesterol, although it lacks the CRAC sequence. Other 3-OH sterols, but not steroids lacking the 3-OH group, also bind this region of the protein. The newly identified cholesterol-binding region is located partly at the C-terminal portion of the TMD and partly in the first amino acid residues in the SCR C-terminal extracellular coil. This finding could be related to the previously described affinity of SCR for cholesterol-rich domains in membranes.


Methods of Molecular Biology | 2010

Electroformation of Giant Unilamellar Vesicles from Native Membranes and Organic Lipid Mixtures for the Study of Lipid Domains under Physiological Ionic-Strength Conditions

L. Ruth Montes; Hasna Ahyayauch; Maitane Ibarguren; Jesús Sot; Alicia Alonso; Luis A. Bagatolli; Félix M. Goñi

Giant unilamellar vesicles (GUVs) constitute a cell-sized model membrane system that allows direct visualization of particular membrane-related phenomena, such as domain formation, at the level of single vesicles using fluorescence microscopy-related techniques. Currently available protocols for the preparation of GUVs work only at very low salt concentrations, thus precluding experimentation under physiological conditions. In addition, the GUVs thus obtained lack membrane compositional asymmetry. Here we show how to prepare GUVs using a new protocol based on the electroformation method either from native membranes or organic lipid mixtures at physiological ionic strength. Additionally, we describe methods to test whether membrane proteins and glycosphingolipids preserve their natural orientation after electroformation of GUVs composed of native membranes.


Biophysical Journal | 2013

In situ synthesis of fluorescent membrane lipids (ceramides) using click chemistry

L. Ruth Montes; Maria Garrido; José Luis Abad; Antonio Delgado; Félix M. Goñi; Alicia Alonso

Ceramide analogues containing azide groups either in the polar head or in the hydrocarbon chains are non-fluorescent. When incorporated into phospholipid bilayers, they can react in situ with a non-fluorescent 1,8-naphthalimide using click chemistry giving rise to fluorescent ceramide derivatives emitting at ≈440 nm. When incorporated into giant unilamellar vesicles, two-photon excitation at 760 nm allows visualization of the ceramide-containing bilayers. This kind of method may be of general applicability in the study of model and cell membranes.


Biophysical Journal | 2012

Thermally Nduced Fusion of Protein Free Lipid Vesicles

Maitane Ibarguren; Paul H.H. Bomans; Peter M. Frederik; Boris Tenchov; Alicia Alonso; Félix M. Goñi

In an attempt to develop a minimal model system of cell membrane fusion in the absence of external catalysts we have used large unilamellar vesicles consisting of a phospholipid (dioleoylphosphatidylcholine), cholesterol and diacylglycerol in a 50:50:3 mol ratio. In this protein-free system, fusion occurs just by thermal fluctuations, above 60°C. Under our conditions cholesterol is essential to produce vesicle aggregation, but fusion is only observed when small amounts of diacylglycerol are added. Vesicle fusion occurs only under conditions when X-ray diffraction and cryo-transmission electron microscopy of the lipid mixtures used in vesicle preparation show inverted lipid phase formation (hexagonal and cubic).


Biophysical Journal | 2010

Detergent Effects on Membranes at Sub-Solubilizing Concentrations: Transmembrane Lipid Motion, Bilayer Permeabilization and Vesicle Lysis/reassembly are Independent Phenomena

Hasna Ahyayauch; Mohammed Bennouna; Alicia Alonso; Félix M. Goñi


Chemistry and Physics of Lipids | 2009

Biophysical properties and membrane organization of ceramides, ceramide-1-phosphate and other simple sphingolipids

Félix M. Goñi; Alicia Alonso


Biophysical Journal | 2009

Ceramide-Enriched Membrane Domains in Red Blood Cells and the Mechanism of Sphingomyelinase-Induced Hot-Cold Hemolysis

Félix M. Goñi; Ruth L. Montes; David Jesús Palma López; Luis A. Bagatolli; Martin Stonehouse; Michael L. Vasil; Bill X. Wu; Yusuf A. Hannun; Alicia Alonso


Biophysical Journal | 2016

Lipid Modulation of LC3/GABARAP-Mediated Autophagosomal Elongation

Alicia Alonso; Ane Landajuela; Javier H. Hervas; Zurine Anton; L. Ruth Montes; David Gil; Mikel Valle; J. Francisco Rodriguez; Félix M. Goñi

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Félix M. Goñi

Spanish National Research Council

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Hasna Ahyayauch

Spanish National Research Council

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L. Ruth Montes

Spanish National Research Council

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David Jesús Palma López

Spanish National Research Council

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Itziar M.D. Posada

Spanish National Research Council

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Jesús Sot

Spanish National Research Council

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Jon V. Busto

Spanish National Research Council

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Maitane Ibarguren

Spanish National Research Council

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Ana R. Viguera

Spanish National Research Council

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Ane Landajuela

Spanish National Research Council

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