Your search keyword '"González-Ros JM"' showing total 69 results

1. Role of the transient receptor potential vanilloid 1 in inflammation and sepsis

Author

Devesa I, Planells-Cases R, Fernández-Ballester GJ, González-Ros JM, Ferrer-Montiel AV, and Fernández-Carvajal AM

Subjects

Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950

Abstract

Isabel Devesa1, Rosa Planells-Cases2, Gregorio Fernández-Ballester1, José Manuel González-Ros1, Antonio Ferrer-Montiel1, Asia Fernández-Carvajal11Instituto de Biología Molecular y Celular, Universidad Miguel Hernández, Alicante; 2Centro de Investigación Príncipe Felipe, Valencia, SpainAbstract: The transient receptor potential vanilloid 1 (TRPV1) is a thermoreceptor that responds to noxious temperatures, as well as to chemical agonists, such as vanilloids and protons. In addition, its channel activity is notably potentiated by proinflammatory mediators released upon tissue damage. The TRPV1 contribution to sensory neuron sensitization by proalgesic agents has signaled this receptor as a prime target for analgesic and anti-inflammatory drug intervention. However, TRPV1 antagonists have notably failed in clinical and preclinical studies because of their unwanted side effects. Recent reports have unveiled previously unrecognized anti-inflammatory and protective functions of TRPV1 in several diseases. For instance, this channel has been suggested to play an anti-inflammatory role in sepsis. Therefore, the use of potent TRPV1 antagonists as a general strategy to treat inflammation must be cautiously considered, given the deleterious effects that may arise from inhibiting the population of channels that have a protective function. The use of TRPV1 antagonists may be limited to treating those pathologies where enhanced receptor activity contributes to the inflamed state. Alternatively, therapeutic paradigms, such as reduction of inflammatory-mediated increase of receptor expression in the cell surface, may be a better strategy to prevent abrogation of the TRPV1 subpopulation involved in anti-inflammatory and protective processes.Keywords: transient receptor potential, nociceptor, capsaicin, pain, ion channel, analgesia

Published

2011

2. Steady-state and time-resolved fluorescent methodologies to characterize the conformational landscape of the selectivity filter of K + channels.

Author

Renart ML, Giudici AM, González-Ros JM, and Poveda JA

Subjects

Streptomyces lividans metabolism, Streptomyces lividans genetics, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Spectrometry, Fluorescence methods, Protein Binding, Fluorescent Dyes chemistry, Ion Channel Gating, Potassium Channels chemistry, Potassium Channels metabolism, Protein Conformation

Abstract

A variety of equilibrium and non-equilibrium methods have been used in a multidisciplinary approach to study the conformational landscape associated with the binding of different cations to the pore of potassium channels. These binding processes, and the conformational changes resulting therefrom, modulate the functional properties of such integral membrane properties, revealing these permeant and blocking cations as true effectors of such integral membrane proteins. KcsA, a prototypic K + channel from Streptomyces lividans, has been extensively characterized in this regard. Here, we revise several fluorescence-based approaches to monitor cation binding under different experimental conditions in diluted samples, analyzing the advantages and disadvantages of each approach. These studies have contributed to explain the selectivity, conduction, and inactivation properties of K + channels at the molecular level, together with the allosteric communication between the two gates that control the ion channel flux, and how they are modulated by lipids., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Jose Antonio Poveda Larrosa reports administrative support, article publishing charges, and equipment, drugs, or supplies were provided by Spain Ministry of Science and Innovation., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

3. Anionic Phospholipids Shift the Conformational Equilibrium of the Selectivity Filter in the KcsA Channel to the Conductive Conformation: Predicted Consequences on Inactivation.

Author

Renart ML, Giudici AM, Coll-Díez C, González-Ros JM, and Poveda JA

Abstract

Here, we report an allosteric effect of an anionic phospholipid on a model K + channel, KcsA. The anionic lipid in mixed detergent-lipid micelles specifically induces a change in the conformational equilibrium of the channel selectivity filter (SF) only when the channel inner gate is in the open state. Such change consists of increasing the affinity of the channel for K + , stabilizing a conductive-like form by maintaining a high ion occupancy in the SF. The process is highly specific in several aspects: First, lipid modifies the binding of K + , but not that of Na + , which remains unperturbed, ruling out a merely electrostatic phenomenon of cation attraction. Second, no lipid effects are observed when a zwitterionic lipid, instead of an anionic one, is present in the micelles. Lastly, the effects of the anionic lipid are only observed at pH 4.0, when the inner gate of KcsA is open. Moreover, the effect of the anionic lipid on K + binding to the open channel closely emulates the K + binding behaviour of the non-inactivating E71A and R64A mutant proteins. This suggests that the observed increase in K + affinity caused by the bound anionic lipid should result in protecting the channel against inactivation.

Published

2023

4. Xenopus Oocytes as a Powerful Cellular Model to Study Foreign Fully-Processed Membrane Proteins.

Author

Ivorra I, Alberola-Die A, Cobo R, González-Ros JM, and Morales A

Abstract

The use of Xenopus oocytes in electrophysiological and biophysical research constitutes a long and successful story, providing major advances to the knowledge of the function and modulation of membrane proteins, mostly receptors, ion channels, and transporters. Earlier reports showed that these cells are capable of correctly expressing heterologous proteins after injecting the corresponding mRNA or cDNA. More recently, the Xenopus oocyte has become an outstanding host-cell model to carry out detailed studies on the function of fully-processed foreign membrane proteins after their microtransplantation to the oocyte. This review focused on the latter overall process of transplanting foreign membrane proteins to the oocyte after injecting plasma membranes or purified and reconstituted proteins. This experimental approach allows for the study of both the function of mature proteins, with their native stoichiometry and post-translational modifications, and their putative modulation by surrounding lipids, mostly when the protein is purified and reconstituted in lipid matrices of defined composition. Remarkably, this methodology enables functional microtransplantation to the oocyte of membrane receptors, ion channels, and transporters from different sources including human post-mortem tissue banks. Despite the large progress achieved over the last decades on the structure, function, and modulation of neuroreceptors and ion channels in healthy and pathological tissues, many unanswered questions remain and, most likely, Xenopus oocytes will continue to help provide valuable responses.

Published

2022

5. Molecular Events behind the Selectivity and Inactivation Properties of Model NaK-Derived Ion Channels.

Author

Giudici AM, Renart ML, Coutinho A, Morales A, González-Ros JM, and Poveda JA

Subjects

Bacterial Proteins metabolism, Binding Sites, Ion Channels metabolism, Ions metabolism, Protein Conformation, Sodium metabolism, Potassium metabolism, Potassium Channels metabolism

Abstract

Y55W mutants of non-selective NaK and partly K + -selective NaK2K channels have been used to explore the conformational dynamics at the pore region of these channels as they interact with either Na + or K + . A major conclusion is that these channels exhibit a remarkable pore conformational flexibility. Homo-FRET measurements reveal a large change in W55-W55 intersubunit distances, enabling the selectivity filter (SF) to admit different species, thus, favoring poor or no selectivity. Depending on the cation, these channels exhibit wide-open conformations of the SF in Na + , or tight induced-fit conformations in K + , most favored in the four binding sites containing NaK2K channels. Such conformational flexibility seems to arise from an altered pattern of restricting interactions between the SF and the protein scaffold behind it. Additionally, binding experiments provide clues to explain such poor selectivity. Compared to the K + -selective KcsA channel, these channels lack a high affinity K + binding component and do not collapse in Na + . Thus, they cannot properly select K + over competing cations, nor reject Na + by collapsing, as K + -selective channels do. Finally, these channels do not show C-type inactivation, likely because their submillimolar K + binding affinities prevent an efficient K + loss from their SF, thus favoring permanently open channel states.

Published

2022

6. Probing the Structural Dynamics of the Activation Gate of KcsA Using Homo-FRET Measurements.

Author

Díaz-García C, Renart ML, Poveda JA, Giudici AM, González-Ros JM, Prieto M, and Coutinho A

Subjects

Bacterial Proteins genetics, Hydrogen-Ion Concentration, Molecular Dynamics Simulation, Potassium Channels genetics, Protein Conformation, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Fluorescence Resonance Energy Transfer methods, Ion Channel Gating, Potassium metabolism, Potassium Channels chemistry, Potassium Channels metabolism

Abstract

The allosteric coupling between activation and inactivation processes is a common feature observed in K + channels. Particularly, in the prokaryotic KcsA channel the K + conduction process is controlled by the inner gate, which is activated by acidic pH, and by the selectivity filter (SF) or outer gate, which can adopt non-conductive or conductive states. In a previous study, a single tryptophan mutant channel (W67 KcsA) enabled us to investigate the SF dynamics using time-resolved homo-Förster Resonance Energy Transfer (homo-FRET) measurements. Here, the conformational changes of both gates were simultaneously monitored after labelling the G116C position with tetramethylrhodamine (TMR) within a W67 KcsA background. At a high degree of protein labeling, fluorescence anisotropy measurements showed that the pH-induced KcsA gating elicited a variation in the homo-FRET efficiency among the conjugated TMR dyes (TMR homo-FRET), while the conformation of the SF was simultaneously tracked (W67 homo-FRET). The dependence of the activation p K a of the inner gate with the ion occupancy of the SF unequivocally confirmed the allosteric communication between the two gates of KcsA. This simple TMR homo-FRET based ratiometric assay can be easily extended to study the conformational dynamics associated with the gating of other ion channels and their modulation.

Published

2021

7. Peimine, an Anti-Inflammatory Compound from Chinese Herbal Extracts, Modulates Muscle-Type Nicotinic Receptors.

Author

Alberola-Die A, Encinar JA, Cobo R, Fernández-Ballester G, González-Ros JM, Ivorra I, and Morales A

Subjects

Animals, Drugs, Chinese Herbal pharmacology, Muscles metabolism, Oocytes metabolism, Receptors, Nicotinic genetics, Xenopus laevis, Anti-Inflammatory Agents pharmacology, Cevanes pharmacology, Gene Expression Regulation drug effects, Muscles drug effects, Oocytes drug effects, Plant Extracts pharmacology, Receptors, Nicotinic metabolism

Abstract

Fritillaria bulbs are used in Traditional Chinese Medicine to treat several illnesses. Peimine (Pm), an anti-inflammatory compound from Fritillaria , is known to inhibit some voltage-dependent ion channels and muscarinic receptors, but its interaction with ligand-gated ion channels remains unexplored. We have studied if Pm affects nicotinic acetylcholine receptors (nAChRs), since they play broad functional roles, both in the nervous system and non-neuronal tissues. Muscle-type nAChRs were incorporated to Xenopus oocytes and the action of Pm on the membrane currents elicited by ACh ( I ACh s) was assessed. Functional studies were combined with virtual docking and molecular dynamics assays. Co-application of ACh and Pm reversibly blocked I ACh , with an IC 50 in the low micromolar range. Pm inhibited nAChR by: (i) open-channel blockade, evidenced by the voltage-dependent inhibition of I Ach , (ii) enhancement of nAChR desensitization, revealed by both an accelerated I ACh decay and a decelerated I ACh deactivation, and (iii) resting-nAChR blockade, deduced from the I ACh inhibition elicited by Pm when applied before ACh superfusion. In good concordance, virtual docking and molecular dynamics assays demonstrated that Pm binds to different sites at the nAChR, mostly at the transmembrane domain. Thus, Pm from Fritillaria bulbs, considered therapeutic herbs, targets nAChRs with high affinity, which might account for its anti-inflammatory actions.

Published

2021

8. Tetraoctylammonium, a Long Chain Quaternary Ammonium Blocker, Promotes a Noncollapsed, Resting-Like Inactivated State in KcsA.

Author

Giudici AM, Díaz-García C, Renart ML, Coutinho A, Prieto M, González-Ros JM, and Poveda JA

Subjects

Bacterial Proteins antagonists & inhibitors, Bacterial Proteins genetics, Binding Sites, Fluorescence Resonance Energy Transfer, Hydrogen-Ion Concentration, Mutagenesis, Site-Directed, Potassium chemistry, Potassium metabolism, Potassium Channels genetics, Protein Stability, Protein Structure, Tertiary, Quaternary Ammonium Compounds metabolism, Sodium chemistry, Sodium metabolism, Temperature, Bacterial Proteins metabolism, Potassium Channels metabolism, Quaternary Ammonium Compounds chemistry

Abstract

Alkylammonium salts have been used extensively to study the structure and function of potassium channels. Here, we use the hydrophobic tetraoctylammonium (TOA + ) to shed light on the structure of the inactivated state of KcsA, a tetrameric prokaryotic potassium channel that serves as a model to its homologous eukaryotic counterparts. By the combined use of a thermal denaturation assay and the analysis of homo-Förster resonance energy transfer in a mutant channel containing a single tryptophan (W67) per subunit, we found that TOA + binds the channel cavity with high affinity, either with the inner gate open or closed. Moreover, TOA + bound at the cavity allosterically shifts the equilibrium of the channel's selectivity filter conformation from conductive to an inactivated-like form. The inactivated TOA + -KcsA complex exhibits a loss in the affinity towards permeant K + at pH 7.0, when the channel is in its closed state, but maintains the two sets of K + binding sites and the W67-W67 intersubunit distances characteristic of the selectivity filter in the channel resting state. Thus, the TOA + -bound state differs clearly from the collapsed channel state described by X-ray crystallography and claimed to represent the inactivated form of KcsA.

Published

2021

9. Mechanisms of Blockade of the Muscle-Type Nicotinic Receptor by Benzocaine, a Permanently Uncharged Local Anesthetic.

Author

Cobo R, Nikolaeva-Koleva M, Alberola-Die A, Fernández-Ballester G, González-Ros JM, Ivorra I, and Morales A

Subjects

Acetylcholine, Anesthetics, Local pharmacology, Animals, Benzocaine pharmacology, Muscles, Oocytes, Receptors, Nicotinic

Abstract

Most local anesthetics (LAs) are amine compounds bearing one or several phenolic rings. Many of them are protonated at physiological pH, but benzocaine (Bzc) is permanently uncharged, which is relevant because the effects of LAs on nicotinic acetylcholine (ACh) receptors (nAChRs) depend on their presence as uncharged or protonated species. The aims of this study were to assess the effects of Bzc on nAChRs and to correlate them with its binding to putative interacting sites on this receptor. nAChRs from Torpedo electroplaques were microtransplanted to Xenopus oocytes and currents elicited by ACh (I ACh s), either alone or together with Bzc, were recorded at different potentials. Co-application of ACh with increasing concentrations of Bzc showed that Bzc reversibly blocked nAChRs. I ACh inhibition by Bzc was voltage-independent, but the I ACh rebound elicited when rinsing Bzc suggests an open-channel blockade. Besides, ACh and Bzc co-application enhanced nAChR desensitization. When Bzc was just pre-applied it also inhibited I ACh , by blocking closed (resting) nAChRs. This blockade slowed down the kinetics of both the I ACh activation and the recovery from blockade. The electrophysiological results indicate that Bzc effects on nAChRs are similar to those of 2,6-dimethylaniline, an analogue of the hydrophobic moiety of lidocaine. Furthermore, docking assays on models of the nAChR revealed that Bzc and DMA binding sites on nAChRs overlap fairly well. These results demonstrate that Bzc inhibits nAChRs by multiple mechanisms and contribute to better understanding both the modulation of nAChRs and how LAs elicit some of their clinical side effects. This article is part of a Special Issue entitled: Honoring Ricardo Miledi - outstanding neuroscientist of XX-XXI centuries., Competing Interests: Declaration of Competing Interest The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be considered as a potential conflict of interest. The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be considered as a potential conflict of interest., (Copyright © 2019 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2020

10. Modulation of Function, Structure and Clustering of K + Channels by Lipids: Lessons Learnt from KcsA.

Author

Renart ML, Giudici AM, Díaz-García C, Molina ML, Morales A, González-Ros JM, and Poveda JA

Subjects

Animals, Binding Sites physiology, Cluster Analysis, Protein Binding physiology, Protein Interaction Maps physiology, Bacterial Proteins metabolism, Ion Channel Gating physiology, Lipid Bilayers metabolism, Potassium Channels metabolism

Abstract

KcsA, a prokaryote tetrameric potassium channel, was the first ion channel ever to be structurally solved at high resolution. This, along with the ease of its expression and purification, made KcsA an experimental system of choice to study structure-function relationships in ion channels. In fact, much of our current understanding on how the different channel families operate arises from earlier KcsA information. Being an integral membrane protein, KcsA is also an excellent model to study how lipid-protein and protein-protein interactions within membranes, modulate its activity and structure. In regard to the later, a variety of equilibrium and non-equilibrium methods have been used in a truly multidisciplinary effort to study the effects of lipids on the KcsA channel. Remarkably, both experimental and "in silico" data point to the relevance of specific lipid binding to two key arginine residues. These residues are at non-annular lipid binding sites on the protein and act as a common element to trigger many of the lipid effects on this channel. Thus, processes as different as the inactivation of channel currents or the assembly of clusters from individual KcsA channels, depend upon such lipid binding.

Published

2020

11. Modulation of the potassium channel KcsA by anionic phospholipids: Role of arginines at the non-annular lipid binding sites.

Author

Poveda JA, Giudici AM, Renart ML, Millet O, Morales A, González-Ros JM, Oakes V, Furini S, and Domene C

Subjects

Anions metabolism, Arginine metabolism, Bacterial Proteins chemistry, Bacterial Proteins physiology, Binding Sites, Ion Channel Gating, Kinetics, Lipid Bilayers chemistry, Models, Molecular, Mutation genetics, Patch-Clamp Techniques, Phosphatidylglycerols chemistry, Phospholipids metabolism, Polymorphism, Single Nucleotide genetics, Potassium Channels genetics, Potassium Channels metabolism, Potassium Channels physiology, Potassium Channels, Voltage-Gated physiology, Protein Binding, Streptomyces lividans chemistry, Streptomyces lividans metabolism, Bacterial Proteins genetics, Bacterial Proteins metabolism, Membrane Lipids chemistry, Potassium Channels, Voltage-Gated genetics, Potassium Channels, Voltage-Gated metabolism

Abstract

The role of arginines R64 and R89 at non-annular lipid binding sites of KcsA, on the modulation of channel activity by anionic lipids has been investigated. In wild-type (WT) KcsA reconstituted into asolectin lipid membranes, addition of phosphatidic acid (PA) drastically reduces inactivation in macroscopic current recordings. Consistent to this, PA increases current amplitude, mean open time and open probability at the single channel level. Moreover, kinetic analysis reveals that addition of PA causes longer open channel lifetimes and decreased closing rate constants. Effects akin to those of PA on WT-KcsA are observed when R64 and/or R89 are mutated to alanine, regardless of the added anionic lipids. We interpret these results as a consequence of interactions between the arginines and the anionic PA bound to the non-annular sites. NMR data shows indeed that at least R64 is involved in binding PA. Moreover, molecular dynamics (MD) simulations predict that R64, R89 and surrounding residues such as T61, mediate persistent binding of PA to the non-annular sites. Channel inactivation depends on interactions within the inactivation triad (E71-D80-W67) behind the selectivity filter. Therefore, it is expected that such interactions are affected when PA binds the arginines at the non-annular sites. In support of this, MD simulations reveal that PA binding prevents interaction between R89 and D80, which seems critical to the effectiveness of the inactivation triad. This mechanism depends on the stability of the bound lipid, favoring anionic headgroups such as that of PA, which thrive on the positive charge of the arginines., (Copyright © 2019. Published by Elsevier B.V.)

Published

2019

12. Conformational plasticity in the KcsA potassium channel pore helix revealed by homo-FRET studies.

Author

Renart ML, Giudici AM, Poveda JA, Fedorov A, Berberan-Santos MN, Prieto M, Díaz-García C, González-Ros JM, and Coutinho A

Subjects

Anisotropy, Binding Sites, Crystallography, X-Ray methods, Fluorescence Polarization, Hydrogen-Ion Concentration, Ion Channel Gating, Potassium metabolism, Sodium metabolism, Escherichia coli metabolism, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Fluorescence Resonance Energy Transfer methods, Potassium Channels chemistry, Potassium Channels metabolism, Protein Conformation

Abstract

Potassium channels selectivity filter (SF) conformation is modulated by several factors, including ion-protein and protein-protein interactions. Here, we investigate the SF dynamics of a single Trp mutant of the potassium channel KcsA (W67) using polarized time-resolved fluorescence measurements. For the first time, an analytical framework is reported to analyze the homo-Förster resonance energy transfer (homo-FRET) within a symmetric tetrameric protein with a square geometry. We found that in the closed state (pH 7), the W67-W67 intersubunit distances become shorter as the average ion occupancy of the SF increases according to cation type and concentration. The hypothesis that the inactivated SF at pH 4 is structurally similar to its collapsed state, detected at low K + , pH 7, was ruled out, emphasizing the critical role played by the S2 binding site in the inactivation process of KcsA. This homo-FRET approach provides complementary information to X-ray crystallography in which the protein conformational dynamics is usually compromised.

Published

2019

13. Accessibility of Cations to the Selectivity Filter of KcsA in the Inactivated State: An Equilibrium Binding Study.

Author

Giudici AM, Renart ML, Díaz-García C, Morales A, Poveda JA, and González-Ros JM

Subjects

Bacterial Proteins chemistry, Cations metabolism, Models, Molecular, Potassium metabolism, Potassium Channels chemistry, Protein Binding, Protein Conformation, Protein Multimerization, Protein Stability, Sodium metabolism, Streptomyces lividans chemistry, Bacterial Proteins metabolism, Potassium Channels metabolism, Streptomyces lividans metabolism

Abstract

Cation binding under equilibrium conditions has been used as a tool to explore the accessibility of permeant and nonpermeant cations to the selectivity filter in three different inactivated models of the potassium channel KcsA. The results show that the stack of ion binding sites (S1 to S4) in the inactivated filter models remain accessible to cations as they are in the resting channel state. The inactivated state of the selectivity filter is therefore "resting-like" under such equilibrium conditions. Nonetheless, quantitative differences in the apparent K D 's of the binding processes reveal that the affinity for the binding of permeant cations to the inactivated channel models, mainly K⁺, decreases considerably with respect to the resting channel. This is likely to cause a loss of K⁺ from the inactivated filter and consequently, to promote nonconductive conformations. The most affected site by the affinity loss seems to be S4, which is interesting because S4 is the first site to accommodate K⁺ coming from the channel vestibule when K⁺ exits the cell. Moreover, binding of the nonpermeant species, Na⁺, is not substantially affected by inactivation, meaning that the inactivated channels are also less selective for permeant versus nonpermeant cations under equilibrium conditions.

Published

2019

14. Mechanisms Underlying the Strong Inhibition of Muscle-Type Nicotinic Receptors by Tetracaine.

Author

Cobo R, Nikolaeva M, Alberola-Die A, Fernández-Ballester G, González-Ros JM, Ivorra I, and Morales A

Abstract

Nicotinic acetylcholine (ACh) receptors (nAChRs) are included among the targets of a variety of local anesthetics, although the molecular mechanisms of blockade are still poorly understood. Some local anesthetics, such as lidocaine, act on nAChRs by different means through their ability to present as both charged and uncharged molecules. Thus, we explored the mechanisms of nAChR blockade by tetracaine, which at physiological pH is almost exclusively present as a positively charged local anesthetic. The nAChRs from Torpedo electroplaques were transplanted to Xenopus oocytes and the currents elicited by ACh ( I ACh s), either alone or co-applied with tetracaine, were recorded. Tetracaine reversibly blocked I ACh , with an IC 50 (i.e., the concentration required to inhibit half the maximum I ACh ) in the submicromolar range. Notably, at very low concentrations (0.1 μM), tetracaine reduced I ACh in a voltage-dependent manner, the more negative potentials produced greater inhibition, indicating open-channel blockade. When the tetracaine concentration was increased to 0.7 μM or above, voltage-independent inhibition was also observed, indicating closed-channel blockade. The I ACh inhibition by pre-application of just 0.7 μM tetracaine before superfusion of ACh also corroborated the notion of tetracaine blockade of resting nAChRs. Furthermore, tetracaine markedly increased nAChR desensitization, mainly at concentrations equal or higher than 0.5 μM. Interestingly, tetracaine did not modify desensitization when its binding within the channel pore was prevented by holding the membrane at positive potentials. Tetracaine-nAChR interactions were assessed by virtual docking assays, using nAChR models in the closed and open states. These assays revealed that tetracaine binds at different sites of the nAChR located at the extracellular and transmembrane domains, in both open and closed conformations. Extracellular binding sites seem to be associated with closed-channel blockade; whereas two sites within the pore, with different affinities for tetracaine, contribute to open-channel blockade and the enhancement of desensitization, respectively. These results demonstrate a concentration-dependent heterogeneity of tetracaine actions on nAChRs, and contribute to a better understanding of the complex modulation of muscle-type nAChRs by local anesthetics. Furthermore, the combination of functional and virtual assays to decipher nAChR-tetracaine interactions has allowed us to tentatively assign the main nAChR residues involved in these modulating actions.

Published

2018

15. Selective exclusion and selective binding both contribute to ion selectivity in KcsA, a model potassium channel.

Author

Renart ML, Montoya E, Giudici AM, Poveda JA, Fernández AM, Morales A, and González-Ros JM

Subjects

Algorithms, Amino Acid Substitution, Bacterial Proteins chemistry, Bacterial Proteins genetics, Binding Sites, Binding, Competitive, Cesium metabolism, Detergents chemistry, Detergents pharmacology, Glucosides chemistry, Glucosides pharmacology, Hot Temperature adverse effects, Kinetics, Mutation, Potassium Channel Blockers chemistry, Potassium Channel Blockers pharmacology, Potassium Channels chemistry, Potassium Channels genetics, Protein Denaturation, Protein Stability, Quaternary Ammonium Compounds chemistry, Quaternary Ammonium Compounds pharmacology, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Rubidium metabolism, Sodium metabolism, Solubility, Bacterial Proteins metabolism, Models, Molecular, Potassium metabolism, Potassium Channels metabolism, Streptomyces metabolism

Abstract

The selectivity filter in potassium channels, a main component of the ion permeation pathway, configures a stack of binding sites (sites S1-S4) to which K + and other cations may bind. Specific ion binding to such sites induces changes in the filter conformation, which play a key role in defining both selectivity and permeation. Here, using the potassium channel KcsA as a model, we contribute new evidence to reinforce this assertion. First, ion binding to KcsA blocked by tetrabutylammonium at the most cytoplasmic site in the selectivity filter (S4) suggests that such a site, when in the nonconductive filter conformation, has a higher affinity for cation binding than the most extracellular S1 site. This filter asymmetry, along with differences in intracellular and extracellular concentrations of K + versus Na + under physiological conditions, should strengthen selection of the permeant K + by the channel. Second, we used different K + concentrations to shift the equilibrium between nonconductive and conductive states of the selectivity filter in which to test competitive binding of Na + These experiments disclosed a marked decrease in the affinity of Na + to bind the channel when the conformational equilibrium shifts toward the conductive state. This finding suggested that in addition to the selective binding of K + and other permeant species over Na + , there is a selective exclusion of nonpermeant species from binding the channel filter, once it reaches a fully conductive conformation. We conclude that selective binding and selective exclusion of permeant and nonpermeant cations, respectively, are important determinants of ion channel selectivity., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

16. Towards understanding the molecular basis of ion channel modulation by lipids: Mechanistic models and current paradigms.

Author

Poveda JA, Marcela Giudici A, Lourdes Renart M, Morales A, and González-Ros JM

Subjects

Bacterial Proteins chemistry, Drug Design, Humans, Potassium Channels chemistry, Ion Channels chemistry, Membrane Lipids chemistry, Membrane Proteins chemistry

Abstract

Research on ion channel modulation has become a hot topic because of the key roles these membrane proteins play in both prokaryotic and eukaryotic organisms. In this respect, lipid modulation adds to the overall modulatory mechanisms as a potential via to find new pharmacological targets for drug design based on interfering with lipid/channel interactions. However, our knowledge in this field is scarce and often circumscribed to the sites where lipids bind and/or its final functional consequences. To fully understand this process it is necessary to improve our knowledge on its molecular basis, from the binding sites to the signalling pathways that derive in structural and functional effects on the ion channel. In this review, we have compiled information about such mechanisms and established a classification into four different modes of action. Afterwards, we have revised in more detail the lipid modulation of Cys-loop receptors and of the potassium channel KcsA, which were chosen as model channels modulated by specific lipids. This article is part of a Special Issue entitled: Membrane Lipid Therapy: Drugs Targeting Biomembranes edited by Pablo V. Escribá., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

17. Differential binding of monovalent cations to KcsA: Deciphering the mechanisms of potassium channel selectivity.

Author

Montoya E, Lourdes Renart M, Marcela Giudici A, Poveda JA, Fernández AM, Morales A, and González-Ros JM

Subjects

Bacterial Proteins chemistry, Crystallography, X-Ray, Lithium metabolism, Permeability, Potassium metabolism, Potassium Channels chemistry, Protein Conformation, Sodium metabolism, Bacterial Proteins metabolism, Potassium Channels metabolism

Abstract

This work explores whether the ion selectivity and permeation properties of a model potassium channel, KcsA, could be explained based on ion binding features. Non-permeant Na + or Li + bind with low affinity (millimolar K D 's) to a single set of sites contributed by the S1 and S4 sites seen at the selectivity filter in the KcsA crystal structure. Conversely, permeant K + , Rb + , Tl + and even Cs + bind to two different sets of sites as their concentration increases, consistent with crystallographic evidence on the ability of permeant species to induce concentration-dependent transitions between conformational states (non-conductive and conductive) of the channel's selectivity filter. The first set of such sites, assigned also to the crystallographic S1 and S4 sites, shows similarly high affinities for all permeant species (micromolar K D 's), thus, securing displacement of potentially competing non-permeant cations. The second set of sites, available only to permeant cations upon the transition to the conductive filter conformation, shows low affinity (millimolar K D 's), thus, favoring cation dissociation and permeation and results from the contribution of all S1 through S4 crystallographic sites. The differences in affinities between permeant and non-permeant cations and the similarities in binding behavior within each of these two groups, correlate fully with their permeabilities relative to K + , suggesting that binding is an important determinant of the channel's ion selectivity. Conversely, the complexity observed in permeation features cannot be explained just in terms of binding and likely relates to reported differences in the occupancy of the S2 and S3 sites by the permeant cations., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

18. Muscle-Type Nicotinic Receptor Modulation by 2,6-Dimethylaniline, a Molecule Resembling the Hydrophobic Moiety of Lidocaine.

Author

Alberola-Die A, Fernández-Ballester G, González-Ros JM, Ivorra I, and Morales A

Abstract

To identify the molecular determinants responsible for lidocaine blockade of muscle-type nAChRs, we have studied the effects on this receptor of 2,6-dimethylaniline (DMA), which resembles lidocaine's hydrophobic moiety. Torpedo marmorata nAChRs were microtransplanted to Xenopus oocytes and currents elicited by ACh ( I ACh ), either alone or co-applied with DMA, were recorded. DMA reversibly blocked I ACh and, similarly to lidocaine, exerted a closed-channel blockade, as evidenced by the enhancement of I ACh blockade when DMA was pre-applied before its co-application with ACh, and hastened I ACh decay. However, there were marked differences among its mechanisms of nAChR inhibition and those mediated by either the entire lidocaine molecule or diethylamine (DEA), a small amine resembling lidocaine's hydrophilic moiety. Thereby, the IC 50 for DMA, estimated from the dose-inhibition curve, was in the millimolar range, which is one order of magnitude higher than that for either DEA or lidocaine. Besides, nAChR blockade by DMA was voltage-independent in contrast to the increase of I ACh inhibition at negative potentials caused by the more polar lidocaine or DEA molecules. Accordingly, virtual docking assays of DMA on nAChRs showed that this molecule binds predominantly at intersubunit crevices of the transmembrane-spanning domain, but also at the extracellular domain. Furthermore, DMA interacted with residues inside the channel pore, although only in the open-channel conformation. Interestingly, co-application of ACh with DEA and DMA, at their IC 50 s, had additive inhibitory effects on I ACh and the extent of blockade was similar to that predicted by the allotopic model of interaction, suggesting that DEA and DMA bind to nAChRs at different loci. These results indicate that DMA mainly mimics the low potency and non-competitive actions of lidocaine on nAChRs, as opposed to the high potency and voltage-dependent block by lidocaine, which is emulated by the hydrophilic DEA. Furthermore, it is pointed out that the hydrophobic (DMA) and hydrophilic (DEA) moieties of the lidocaine molecule act differently on nAChRs and that their separate actions taken together account for most of the inhibitory effects of the whole lidocaine molecule on nAChRs.

Published

2016

19. Muscle-Type Nicotinic Receptor Blockade by Diethylamine, the Hydrophilic Moiety of Lidocaine.

Author

Alberola-Die A, Fernández-Ballester G, González-Ros JM, Ivorra I, and Morales A

Abstract

Lidocaine bears in its structure both an aromatic ring and a terminal amine, which can be protonated at physiological pH, linked by an amide group. Since lidocaine causes multiple inhibitory actions on nicotinic acetylcholine receptors (nAChRs), this work was aimed to determine the inhibitory effects of diethylamine (DEA), a small molecule resembling the hydrophilic moiety of lidocaine, on Torpedo marmorata nAChRs microtransplanted to Xenopus oocytes. Similarly to lidocaine, DEA reversibly blocked acetylcholine-elicited currents (I ACh ) in a dose-dependent manner (IC 50 close to 70 μM), but unlike lidocaine, DEA did not affect I ACh desensitization. I ACh inhibition by DEA was more pronounced at negative potentials, suggesting an open-channel blockade of nAChRs, although roughly 30% inhibition persisted at positive potentials, indicating additional binding sites outside the pore. DEA block of nAChRs in the resting state (closed channel) was confirmed by the enhanced I ACh inhibition when pre-applying DEA before its co-application with ACh, as compared with solely DEA and ACh co-application. Virtual docking assays provide a plausible explanation to the experimental observations in terms of the involvement of different sets of drug binding sites. So, at the nAChR transmembrane (TM) domain, DEA and lidocaine shared binding sites within the channel pore, giving support to their open-channel blockade; besides, lidocaine, but not DEA, interacted with residues at cavities among the M1, M2, M3, and M4 segments of each subunit and also at intersubunit crevices. At the extracellular (EC) domain, DEA and lidocaine binding sites were broadly distributed, which aids to explain the closed channel blockade observed. Interestingly, some DEA clusters were located at the α-γ interphase of the EC domain, in a cavity near the orthosteric binding site pocket; by contrast, lidocaine contacted with all α-subunit loops conforming the ACh binding site, both in α-γ and α-δ and interphases, likely because of its larger size. Together, these results indicate that DEA mimics some, but not all, inhibitory actions of lidocaine on nAChRs and that even this small polar molecule acts by different mechanisms on this receptor. The presented results contribute to a better understanding of the structural determinants of nAChR modulation.

Published

2016

20. Competing Lipid-Protein and Protein-Protein Interactions Determine Clustering and Gating Patterns in the Potassium Channel from Streptomyces lividans (KcsA).

Author

Molina ML, Giudici AM, Poveda JA, Fernández-Ballester G, Montoya E, Renart ML, Fernández AM, Encinar JA, Riquelme G, Morales A, and González-Ros JM

Subjects

Bacterial Proteins physiology, Lipid Bilayers, Models, Molecular, Potassium Channels physiology, Protein Binding, Bacterial Proteins metabolism, Ion Channel Gating, Lipids chemistry, Potassium Channels metabolism, Proteins metabolism, Streptomyces lividans metabolism

Abstract

There is increasing evidence to support the notion that membrane proteins, instead of being isolated components floating in a fluid lipid environment, can be assembled into supramolecular complexes that take part in a variety of cooperative cellular functions. The interplay between lipid-protein and protein-protein interactions is expected to be a determinant factor in the assembly and dynamics of such membrane complexes. Here we report on a role of anionic phospholipids in determining the extent of clustering of KcsA, a model potassium channel. Assembly/disassembly of channel clusters occurs, at least partly, as a consequence of competing lipid-protein and protein-protein interactions at nonannular lipid binding sites on the channel surface and brings about profound changes in the gating properties of the channel. Our results suggest that these latter effects of anionic lipids are mediated via the Trp(67)-Glu(71)-Asp(80) inactivation triad within the channel structure and its bearing on the selectivity filter., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

21. Lipid modulation of ion channels through specific binding sites.

Author

Poveda JA, Giudici AM, Renart ML, Molina ML, Montoya E, Fernández-Carvajal A, Fernández-Ballester G, Encinar JA, and González-Ros JM

Subjects

Binding Sites, Ions metabolism, Lipid Bilayers metabolism, Membrane Lipids metabolism, Potassium Channels metabolism, Streptomyces lividans metabolism

Abstract

Ion channel conformational changes within the lipid membrane are a key requirement to control ion passage. Thus, it seems reasonable to assume that lipid composition should modulate ion channel function. There is increasing evidence that this implicates not just an indirect consequence of the lipid influence on the physical properties of the membrane, but also specific binding of selected lipids to certain protein domains. The result is that channel function and its consequences on excitability, contractility, intracellular signaling or any other process mediated by such channel proteins, could be subjected to modulation by membrane lipids. From this it follows that development, age, diet or diseases that alter lipid composition should also have an influence on those cellular properties. The wealth of data on the non-annular lipid binding sites in potassium channel from Streptomyces lividans (KcsA) makes this protein a good model to study the modulation of ion channel structure and function by lipids. The fact that this protein is able to assemble into clusters through the same non-annular sites, resulting in large changes in channel activity, makes these sites even more interesting as a potential target to develop lead compounds able to disrupt such interactions and hopefully, to modulate ion channel function. This Article is Part of a Special Issue Entitled: Membrane Structure and Function: Relevance in the Cell's Physiology, Pathology and Therapy., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2014

22. Mutation of I696 and W697 in the TRP box of vanilloid receptor subtype I modulates allosteric channel activation.

Author

Gregorio-Teruel L, Valente P, González-Ros JM, Fernández-Ballester G, and Ferrer-Montiel A

Subjects

Allosteric Regulation, Allosteric Site, Animals, Capsaicin pharmacology, HEK293 Cells, Humans, Membrane Potentials, Rats, Sensory System Agents pharmacology, TRPV Cation Channels chemistry, Ion Channel Gating, Mutation, Missense, TRPV Cation Channels genetics, TRPV Cation Channels metabolism

Abstract

The transient receptor potential vanilloid receptor subtype I (TRPV1) channel acts as a polymodal sensory receptor gated by chemical and physical stimuli. Like other TRP channels, TRPV1 contains in its C terminus a short, conserved domain called the TRP box, which is necessary for channel gating. Substitution of two TRP box residues-I696 and W697-with Ala markedly affects TRPV1's response to all activating stimuli, which indicates that these two residues play a crucial role in channel gating. We systematically replaced I696 and W697 with 18 native l-amino acids (excluding cysteine) and evaluated the effect on voltage- and capsaicin-dependent gating. Mutation of I696 decreased channel activation by either voltage or capsaicin; furthermore, gating was only observed with substitution of hydrophobic amino acids. Substitution of W697 with any of the 18 amino acids abolished gating in response to depolarization alone, shifting the threshold to unreachable voltages, but not capsaicin-mediated gating. Moreover, vanilloid-activated responses of W697X mutants showed voltage-dependent gating along with a strong voltage-independent component. Analysis of the data using an allosteric model of activation indicates that mutation of I696 and W697 primarily affects the allosteric coupling constants of the ligand and voltage sensors to the channel pore. Together, our findings substantiate the notion that inter- and/or intrasubunit interactions at the level of the TRP box are critical for efficient coupling of stimulus sensing and gate opening. Perturbation of these interactions markedly reduces the efficacy and potency of the activating stimuli. Furthermore, our results identify these interactions as potential sites for pharmacological intervention.

Published

2014

23. Partitioning of liquid-ordered/liquid-disordered membrane microdomains induced by the fluidifying effect of 2-hydroxylated fatty acid derivatives.

Author

Ibarguren M, López DJ, Encinar JA, González-Ros JM, Busquets X, and Escribá PV

Subjects

Animals, Hydroxylation, Kinetics, Membrane Lipids chemistry, Microscopy, Fluorescence, Spectroscopy, Fourier Transform Infrared, Fatty Acids chemistry, Membrane Microdomains chemistry

Abstract

Cellular functions are usually associated with the activity of proteins and nucleic acids. Recent studies have shown that lipids modulate the localization and activity of key membrane-associated signal transduction proteins, thus regulating the cell's physiology. Membrane Lipid Therapy aims to reverse cell dysfunctions (i.e., diseases) by modulating the activity of membrane signaling proteins through regulation of the lipid bilayer structure. The present work shows the ability of a series of 2-hydroxyfatty acid (2OHFA) derivatives, varying in the acyl chain length and degree of unsaturation, to regulate the membrane lipid structure. These molecules have shown greater therapeutic potential than their natural non-hydroxylated counterparts. We demonstrated that both 2OHFA and natural FAs induced reorganization of lipid domains in model membranes of POPC:SM:PE:Cho, modulating the liquid-ordered/liquid-disordered structures ratio and the microdomain lipid composition. Fluorescence spectroscopy, confocal microscopy, Fourier transform infrared spectroscopy and differential detergent solubilization experiments showed a destabilization of the membranes upon addition of the 2OHFAs and FAs which correlated with the observed disordering effect. The changes produced by these synthetic fatty acids on the lipid structure may constitute part of their mechanism of action, leading to changes in the localization/activity of membrane proteins involved in signaling cascades, and therefore modulating cell responses., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

24. Detergent-labile, supramolecular assemblies of KcsA: relative abundance and interactions involved.

Author

Giudici AM, Molina ML, Ayala JL, Montoya E, Renart ML, Fernández AM, Encinar JA, Ferrer-Montiel AV, Poveda JA, and González-Ros JM

Subjects

Bacterial Proteins metabolism, Cross-Linking Reagents chemistry, Dose-Response Relationship, Drug, Electrophoresis methods, Electrophoresis, Gel, Two-Dimensional methods, Electrophoresis, Polyacrylamide Gel, Lipids chemistry, Models, Molecular, Potassium Channels metabolism, Protein Binding, Protein Structure, Tertiary, Bacterial Proteins chemistry, Detergents pharmacology, Potassium Channels chemistry

Abstract

In this work, we illustrate the ability of the prokaryotic potassium channel KcsA to assemble into a variety of supramolecular clusters of defined sizes containing the tetrameric KcsA as the repeating unit. Such clusters, particularly the larger ones, are markedly detergent-labile and thus, disassemble readily upon exposure to the detergents commonly used in protein purification or conventional electrophoresis analysis. This is a reversible process, as cluster re-assembly occurs upon detergent removal and without the need of added membrane lipids. Interestingly, the dimeric ensemble between two tetrameric KcsA molecules are quite resistant to detergent disassembly to individual KcsA tetramers and along with the latter, are likely the basic building blocks through which the larger clusters are organized. As to the proteins domains involved in clustering, we have observed disassembly of KcsA clusters by SDS-like alkyl sulfates. As these amphiphiles bind to inter-subunit, "non-annular" sites on the protein, these observations suggest that such sites also mediate channel-channel interactions leading to cluster assembly., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

25. Highly functionalized 1,2-diamino compounds through reductive amination of amino acid-derived β-keto esters.

Author

Pérez-Faginas P, Aranda MT, García-López MT, Infantes L, Fernández-Carvajal A, González-Ros JM, Ferrer-Montiel A, and González-Muñiz R

Subjects

Amination, Crystallography, X-Ray, Esters chemistry, Models, Molecular, Oxidation-Reduction, Reducing Agents chemistry, Stereoisomerism, Amino Acids chemistry, Diamines chemistry

Abstract

1,2-Diamine derivatives are valuable building blocks to heterocyclic compounds and important precursors of biologically relevant compounds. In this respect, amino acid-derived β-keto esters are a suitable starting point for the synthesis of β,γ-diamino ester derivatives through a two-step reductive amination procedure with either simple amines or α-amino esters. AcOH and NaBH(3)CN are the additive and reducing agents of choice. The stereoselectivity of the reaction is still an issue, due to the slow imine-enamine equilibria through which the reaction occurs, affording mixtures of diastereoisomers that can be chromatographically separated. Transformation of the β,γ-diamino esters into pyrrolidinone derivatives allows the configuration assignment of the linear compounds, and constitutes an example of their potential application in the generation of molecular diversity.

Published

2013

26. Mapping of unfolding states of integral helical membrane proteins by GPS-NMR and scattering techniques: TFE-induced unfolding of KcsA in DDM surfactant.

Author

Calcutta A, Jessen CM, Behrens MA, Oliveira CL, Renart ML, González-Ros JM, Otzen DE, Pedersen JS, Malmendal A, and Nielsen NC

Subjects

Escherichia coli enzymology, Glucosides chemistry, Light, Micelles, Models, Chemical, Models, Molecular, Molecular Conformation, Protein Conformation, Protein Denaturation, Protein Folding, Protein Structure, Secondary, Scattering, Radiation, Scattering, Small Angle, Surface-Active Agents chemistry, X-Rays, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Magnetic Resonance Spectroscopy methods, Potassium Channels chemistry, Potassium Channels metabolism

Abstract

Membrane proteins are vital for biological function, and their action is governed by structural properties critically depending on their interactions with the membranes. This has motivated considerable interest in studies of membrane protein folding and unfolding. Here the structural changes induced by unfolding of an integral membrane protein, namely TFE-induced unfolding of KcsA solubilized by the n-dodecyl β-d-maltoside (DDM) surfactant is investigated by the recently introduced GPS-NMR (Global Protein folding State mapping by multivariate NMR) (Malmendal et al., PlosONE 5, e10262 (2010)) along with dynamic light scattering (DLS) and small-angle X-ray scattering (SAXS). GPS-NMR is used as a tool for fast analysis of the protein unfolding processes upon external perturbation, and DLS and SAXS are used for further structural characterization of the unfolding states. The combination allows addressing detergent properties and protein conformations at the same time. The mapping of the states reveals that KcsA undergoes a series of rearrangements which include expansion of the tetramer in several steps followed by dissociation into monomers at 29% TFE. Supplementary studies of DDM and TFE in the absence of KcsA suggest that the disintegration of the tetramer at 29% TFE is caused by TFE dissolving the surrounding DDM rim. Above 34% TFE, KcsA collapses to a new structure that is fully formed at 44% TFE., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

27. Advances in modulating thermosensory TRP channels.

Author

Ferrer-Montiel A, Fernández-Carvajal A, Planells-Cases R, Fernández-Ballester G, González-Ros JM, Messeguer A, and González-Muñiz R

Subjects

Animals, Cold Temperature, Hot Temperature, Humans, Inflammation physiopathology, Neoplasms physiopathology, Patents as Topic, Pain physiopathology, TRPV Cation Channels metabolism

Abstract

Introduction: Thermosensory channels are a subfamily of the transient receptor potential (TRP) channel family that are activated by changes in the environmental temperature. These channels, known as thermoTRPs, cover the entire spectrum of temperatures, from noxious cold (< 15°C) to injurious heat (> 42°C). In addition, dysfunction of these channels contributes to the thermal hypersensitivity that accompanies painful conditions. Moreover, because of their wide tissue and cellular distribution, thermoTRPs are also involved in the pathophysiology of several diseases, from inflammation to cancer., Areas Covered: Although the number of thermoTRPs is increasing with the identification of novel members such as TRPM3, we will cover the recent advances in the pharmacology of the classical thermosensory channels, namely TRPV1, TRPV2, TRPV3, TRPV4, TRPM8 and TRPA1. This review will focus on the therapeutic progress carried out for all these channels and will highlight the tenet that TRPV1, TRPM8 and TRPA1 are the most exploited channels, and that the interest on TRPV3 and TRPV4 is growing with the first TRPV3 antagonist that moves into Phase-II clinical trials. In contrast, the pharmacology of TRPV2 is yet in its infancy., Expert Opinion: Despite the tremendous academic and industrial investment to develop therapeutic modulators of thermoTRPs, it apparently seems that we are still far from the first successful product, although hope is maintained high for all compounds currently in clinical trials. A major concern has been the appearance of side effects. A better knowledge of the thermosensory protein networks (signal-plexes), along with the application of system biology approaches may provide novel strategies to modulate thermoTRPs activity with improved therapeutic index. A case in point is TRPV1, where acting on interacting proteins is providing new therapeutic opportunities.

Published

2012

28. Contribution of ion binding affinity to ion selectivity and permeation in KcsA, a model potassium channel.

Author

Renart ML, Montoya E, Fernández AM, Molina ML, Poveda JA, Encinar JA, Ayala JL, Ferrer-Montiel AV, Gómez J, Morales A, and González Ros JM

Subjects

Bacterial Proteins drug effects, Bacterial Proteins genetics, Binding Sites, Ion Channel Gating, Potassium Channels drug effects, Potassium Channels genetics, Protein Denaturation, Protein Stability, Protein Structure, Quaternary, Sodium metabolism, Spectrometry, Fluorescence, Bacterial Proteins metabolism, Potassium metabolism, Potassium Channels metabolism

Abstract

Ion permeation and selectivity, key features in ion channel function, are believed to arise from a complex ensemble of energetic and kinetic variables. Here we evaluate the contribution of pore cation binding to ion permeation and selectivity features of KcsA, a model potassium channel. For this, we used E71A and M96V KcsA mutants in which the equilibrium between conductive and nonconductive conformations of the channel is differently shifted. E71A KcsA is a noninactivating channel mutant. Binding of K(+) to this mutant reveals a single set of low-affinity K(+) binding sites, similar to that seen in the binding of K(+) to wild-type KcsA that produces a conductive, low-affinity complex. This seems consistent with the observed K(+) permeation in E71A. Nonetheless, the E71A mutant retains K(+) selectivity, which cannot be explained on the basis of just its low affinity for this ion. At variance, M96V KcsA is a rapidly inactivating mutant that has lost selectivity for K(+) and also conducts Na(+). Here, low-affinity binding and high-affinity binding of both cations are detected, seemingly in agreement with both being permeating species in this mutant channel. In conclusion, binding of the ion to the channel protein seemingly explains certain gating, ion selectivity, and permeation properties. Ion binding stabilizes greatly the channel and, depending upon ion type and concentration, leads to different conformations and ion binding affinities. High-affinity states guarantee binding of specific ions and mediate ion selectivity but are nonconductive. Conversely, low-affinity states would not discriminate well among different ions but allow permeation to occur.

Published

2012

29. Mutation of Ser-50 and Cys-66 in Snapin modulates protein structure and stability.

Author

Navarro A, Encinar JA, López-Méndez B, Aguado-Llera D, Prieto J, Gómez J, Martínez-Cruz LA, Millet O, González-Ros JM, Fernández-Ballester G, Neira JL, and Ferrer-Montiel A

Subjects

Protein Conformation, Protein Stability, Protein Structure, Secondary, SNARE Proteins chemistry, SNARE Proteins genetics, SNARE Proteins metabolism, Spectroscopy, Fourier Transform Infrared, Vesicular Transport Proteins metabolism, Cysteine genetics, Mutation, Serine genetics, Vesicular Transport Proteins chemistry, Vesicular Transport Proteins genetics

Abstract

Snapin is a 15 kDa protein present in neuronal and non-neuronal cells that has been implicated in the regulation of exocytosis and endocytosis. Protein kinase A (PKA) phosphorylates Snapin at Ser-50, modulating its function. Likewise, mutation of Cys-66, which mediates protein dimerization, impairs its cellular activity. Here, we have investigated the impact of mutating these two positions on protein oligomerization, structure, and thermal stability, along with the interaction with SNARE proteins. We found that recombinant purified Snapin in solution appears mainly as dimers in equilibrium with tetramers. The protein exhibits modest secondary structure elements and notable thermal stability. Mutation of Cys-66 to Ser abolished subunit dimerization, but not higher-order oligomers. This mutant augmented the presence of α-helical structure and slightly increased the protein thermal stability. Similarly, the S50A mutant, mimicking the unphosphorylated protein, also exhibited a higher helical secondary structure content than the wild type, along with greater thermal stability. In contrast, replacement of Ser-50 with Asp (S50D), emulating the protein-phosphorylated state, produced a loss of α-helical structure, concomitant with a decrease in protein thermal stability. In vitro, the wild type and mutants weakly interacted with SNAP-25 and the reconstituted SNARE complex, although S50D exhibited the strongest binding to the SNARE complex, consistent with the observed higher cellular activity of PKA-phosphorylated Snapin. Our observations suggest that the stronger binding of S50D to SNAREs might be due to a destabilization of tetrameric assemblies of Snapin that favor the interaction of protein dimers with the SNARE proteins. Therefore, phosphorylation of Ser-50 has an important impact on the protein structure and stability that appears to underlie its functional modulation.

Published

2012

30. New strategies to develop novel pain therapies: addressing thermoreceptors from different points of view.

Author

Fernández-Carvajal A, Fernández-Ballester G, Devesa I, González-Ros JM, and Ferrer-Montiel A

Abstract

One approach to develop successful pain therapies is the modulation of dysfunctional ion channels that contribute to the detection of thermal, mechanical and chemical painful stimuli. These ion channels, known as thermoTRPs, promote the sensitization and activation of primary sensory neurons known as nociceptors. Pharmacological blockade and genetic deletion of thermoTRP have validated these channels as therapeutic targets for pain intervention. Several thermoTRP modulators have progressed towards clinical development, although most failed because of the appearance of unpredicted side effects. Thus, there is yet a need to develop novel channel modulators with improved therapeutic index. Here, we review the current state-of-the art and illustrate new pharmacological paradigms based on TRPV1 that include: (i) the identification of activity-dependent modulators of this thermoTRP channel; (ii) the design of allosteric modulators that interfere with protein-protein interaction involved in the functional coupling of stimulus sensing and gate opening; and (iii) the development of compounds that abrogate the inflammation-mediated increase of receptor expression in the neuronal surface. These new sites of action represent novel strategies to modulate pathologically active TRPV1, while minimizing an effect on the TRPV1 subpopulation involved in physiological and protective roles, thus increasing their potential therapeutic use.

Published

2011

31. Ionic channels as targets for drug design: a review on computational methods.

Author

Fernández-Ballester G, Fernández-Carvajal A, González-Ros JM, and Ferrer-Montiel A

Abstract

Ion channels are involved in a broad range of physiological and pathological processes. The implications of ion channels in a variety of diseases, including diabetes, epilepsy, hypertension, cancer and even chronic pain, have signaled them as pivotal drug targets. Thus far, drugs targeting ion channels were developed without detailed knowledge of the molecular interactions between the lead compounds and the target channels. In recent years, however, the emergence of high-resolution structures for a plethora of ion channels paves the way for computer-assisted drug design. Currently, available functional and structural data provide an attractive platform to generate models that combine substrate-based and protein-based approaches. In silico approaches include homology modeling, quantitative structure-activity relationships, virtual ligand screening, similarity and pharmacophore searching, data mining, and data analysis tools. These strategies have been frequently used in the discovery and optimization of novel molecules with enhanced affinity and specificity for the selected therapeutic targets. In this review we summarize recent applications of in silico methods that are being used for the development of ion channel drugs.

Published

2011

32. Triazine-based vanilloid 1 receptor open channel blockers: design, synthesis, evaluation, and SAR analysis.

Author

Vidal-Mosquera M, Fernández-Carvajal A, Moure A, Valente P, Planells-Cases R, González-Ros JM, Bujons J, Ferrer-Montiel A, and Messeguer A

Subjects

Analgesics chemistry, Analgesics pharmacology, Animals, Binding Sites, Drug Design, Female, Oocytes drug effects, Oocytes physiology, Patch-Clamp Techniques, Rats, Recombinant Proteins antagonists & inhibitors, Structure-Activity Relationship, Triazines chemistry, Triazines pharmacology, Xenopus, Analgesics chemical synthesis, TRPV Cation Channels antagonists & inhibitors, Triazines chemical synthesis

Abstract

The thermosensory transient receptor potential vanilloid 1 channel (TRPV1) is a polymodal receptor activated by physical and chemical stimuli. TRPV1 activity is drastically potentiated by proinflammatory agents released upon tissue damage. Given the pivotal role of TRPV1 in human pain, there is pressing need for improved TRPV1 antagonists, the development of which will require identification of new pharmacophore scaffolds. Uncompetitive antagonists acting as open-channel blockers might serve as activity-dependent blockers that preferentially modulate the activity of overactive channels, thus displaying fewer side effects than their competitive counterparts. Herein we report the design, synthesis, biological evaluation, and SAR analysis of a family of triazine-based compounds acting as TRPV1 uncompetitive antagonists. We identified the triazine 8aA as a potent, pure antagonist that inhibits TRPV1 channel activity with nanomolar efficacy and strong voltage dependency. It represents a new class of activity-dependent TRPV1 antagonists and may serve as the basis for lead optimization in the development of new analgesics.

Published

2011

33. Solid-phase synthesis of a library of amphipatic hydantoins. Discovery of new hits for TRPV1 blockade.

Author

Gerona-Navarro G, González-Muñiz R, Fernández-Carvajal A, González-Ros JM, Ferrer-Montiel A, Carreño C, Albericio F, and Royo M

Subjects

Hydantoins chemistry, Molecular Structure, Receptors, N-Methyl-D-Aspartate antagonists & inhibitors, Stereoisomerism, Structure-Activity Relationship, Drug Discovery, Hydantoins chemical synthesis, Hydantoins pharmacology, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Solid-Phase Synthesis Techniques, TRPV Cation Channels antagonists & inhibitors

Abstract

Some heterocyclic systems, called privileged scaffolds, appear frequently in bioactive products and marketed drugs. The combination of a recognized privileged scaffold (hydantoin) and a functional group with high incidence in bioactive molecules (guanidine) guided the design of a library of amphipatic compounds, which allowed the discovery of novel TRPV1 ion channel blockers. The library was synthesized by parallel solid-phase synthesis from an orthogonally protected resin-bound Lys-Lys skeleton. Key steps of the synthetic procedure were the construction of the hydantoin ring, by reaction of the N-terminal amino group with N,N-disuccinimidyl carbonate (DSC) and subsequent base-induced cyclization, and the guanidinylation of the C-terminal Lys side-chain after removal of the Alloc protecting-group. The preliminary biological studies have allowed the identification of some of the key structural features directing the blockage of capsaicin-induced Ca(2+) influx through TRPV1 channels, particularly, the strong preference showed for highly lipophilic acyl groups and substituted guanidine moieties. Active compounds based on this new pharmacophoric scaffold that display in vitro and in vivo inhibitory activity.

Published

2011

34. Multiple inhibitory actions of lidocaine on Torpedo nicotinic acetylcholine receptors transplanted to Xenopus oocytes.

Author

Alberola-Die A, Martinez-Pinna J, González-Ros JM, Ivorra I, and Morales A

Subjects

Acetylcholine pharmacology, Animals, Benzenaminium, 4,4'-(3-oxo-1,5-pentanediyl)bis(N,N-dimethyl-N-2-propenyl-), Dibromide pharmacology, Dose-Response Relationship, Drug, Drug Synergism, Edrophonium pharmacology, Female, In Vitro Techniques, Ion Channel Gating, Lidocaine analogs & derivatives, Membrane Potentials drug effects, Oocytes physiology, Torpedo, Xenopus laevis, Anesthetics, Local pharmacology, Lidocaine pharmacology, Nicotinic Antagonists pharmacology, Oocytes drug effects, Receptors, Nicotinic physiology

Abstract

Lidocaine is a local anaesthetic that blocks sodium channels, but also inhibits several ligand-gated ion-channels. The aim of this work was to unravel the mechanisms by which lidocaine blocks Torpedo nicotinic receptors transplanted to Xenopus oocytes. Acetylcholine-elicited currents were reversibly blocked by lidocaine, in a concentration dependent manner. At doses lower than the IC(50) , lidocaine blocked nicotinic receptors only at negative potentials, indicating an open-channel blockade; the binding site within the channel was at about 30% of the way through the electrical field across the membrane. In the presence of higher lidocaine doses, nicotinic receptors were blocked both at positive and negative potentials, acetylcholine dose-response curve shifted to the right and lidocaine pre-application, before its co-application with acetylcholine, enhanced the current inhibition, indicating all together that lidocaine also blocked resting receptors; besides, it increased the current decay rate. When lidocaine, at low doses, was co-applied with 2-(triethylammonio)-N-(2,6-dimethylphenyl) acetamide bromide, edrophonium or 1,5-bis(4-allyldimethylammoniumphenyl)pentan-3-one dibromide, which are quaternary-ammonium molecules that also blocked nicotinic receptors, there was an additive inhibitory effect, indicating that these molecules bound to different sites within the channel pore. These results prove that lidocaine blocks nicotinic receptors by several independent mechanisms and evidence the diverse and complex modulation of this receptor by structurally related molecules., (© 2011 The Authors. Journal of Neurochemistry © 2011 International Society for Neurochemistry.)

Published

2011

35. Membrane-tethered peptides patterned after the TRP domain (TRPducins) selectively inhibit TRPV1 channel activity.

Author

Valente P, Fernández-Carvajal A, Camprubí-Robles M, Gomis A, Quirce S, Viana F, Fernández-Ballester G, González-Ros JM, Belmonte C, Planells-Cases R, and Ferrer-Montiel A

Subjects

Animals, Animals, Newborn, Capsaicin pharmacology, Cell Line, Cells, Cultured, Electrophysiology, HEK293 Cells, Humans, Immunohistochemistry, Peptides chemistry, Rats, TRPV Cation Channels chemistry, Peptides pharmacology, TRPV Cation Channels antagonists & inhibitors, TRPV Cation Channels metabolism

Abstract

The transient receptor potential vanilloid 1 (TRPV1) channel is a thermosensory receptor implicated in diverse physiological and pathological processes. The TRP domain, a highly conserved region in the C terminus adjacent to the internal channel gate, is critical for subunit tetramerization and channel gating. Here, we show that cell-penetrating, membrane-anchored peptides patterned after this protein domain are moderate and selective TRPV1 antagonists both in vitro and in vivo, blocking receptor activity in intact rat primary sensory neurons and their peripheral axons with mean decline time of 30 min. The most potent lipopeptide, TRP-p5, blocked all modes of TRPV1 gating with micromolar efficacy (IC(50)<10 μM), without significantly affecting other thermoTRP channels. In contrast, its retrosequence or the corresponding sequences of other TRPV channels did not alter TRPV1 channel activity (IC(50)>100 μM). TRP-p5 did not affect the capsaicin sensitivity of the vanilloid receptor. Our data suggest that TRP-p5 interferes with protein-protein interactions at the level of the TRP domain that are essential for the "conformational" change that leads to gate opening. Therefore, these palmitoylated peptides, which we termed TRPducins, are noncompetitive, voltage-independent, sequence-specific TRPV1 blockers. Our findings indicate that TRPducin-like peptides may embody a novel molecular strategy that can be exploited to generate a selective pharmacological arsenal for the TRP superfamily of ion channels.

Published

2011

36. Ion binding to KcsA: implications in ion selectivity and channel gating.

Author

Renart ML, Triano I, Poveda JA, Encinar JA, Fernández AM, Ferrer-Montiel AV, Gómez J, and González Ros JM

Subjects

Bacterial Proteins chemistry, Bacterial Proteins genetics, Binding Sites, Models, Molecular, Mutation, Potassium Channels chemistry, Potassium Channels genetics, Protein Binding, Protein Denaturation, Protein Structure, Tertiary, Streptomyces lividans chemistry, Streptomyces lividans genetics, Temperature, Tryptophan genetics, Bacterial Proteins metabolism, Potassium metabolism, Potassium Channels metabolism, Sodium metabolism, Streptomyces lividans metabolism

Abstract

Binding of K+ and Na+ to the potassium channel KcsA has been characterized from the stabilization observed in the heat-induced denaturation of the protein as the ion concentration is increased. KcsA thermal denaturation is known to include (i) dissociation of the homotetrameric channel into its constituent subunits and (ii) protein unfolding. The ion concentration-dependent changes in the thermal stability of the protein, evaluated as the Tm value for thermal-induced denaturation of the protein, may suggest the existence of both high- and low-affinity K+ binding sites of KcsA, which lend support to the tenet that channel gating may be governed by K+ concentration-dependent transitions between different affinity states of the channel selectivity filter. We also found that Na+ binds to KcsA with a KD similar to that estimated electrophysiologically from channel blockade. Therefore, our findings on ion binding to KcsA partly account for K+ over Na+ selectivity and Na+ blockade and argue against the strict “snug fit” hypothesis used initially to explain ion selectivity from the X-ray channel structure. Furthermore, the remarkable effects of increasing the ion concentration, K+ in particular, on the Tm of the denaturation process evidence that synergistic effects of the metal-mediated intersubunit interactions at the channel selectivity filter are a major contributor to the stability of the tetrameric protein. This observation substantiates the notion of a role for ions as structural “effectors” of ion channels.

Published

2010

37. Occupancy of nonannular lipid binding sites on KcsA greatly increases the stability of the tetrameric protein.

Author

Triano I, Barrera FN, Renart ML, Molina ML, Fernández-Ballester G, Poveda JA, Fernández AM, Encinar JA, Ferrer-Montiel AV, Otzen D, and González-Ros JM

Subjects

Bacterial Proteins chemistry, Binding Sites, Crystallography, X-Ray, Electrophoresis, Polyacrylamide Gel, Models, Molecular, Potassium Channels chemistry, Protein Conformation, Protein Denaturation, Spectrometry, Fluorescence, Bacterial Proteins metabolism, Lipid Metabolism, Potassium Channels metabolism

Abstract

KcsA, a homotetrameric potassium channel from prokaryotes, contains noncovalently bound lipids appearing in the X-ray crystallographic structure of the protein. The binding sites for such high-affinity lipids are referred to as "nonannular" sites, correspond to intersubunit protein domains, and bind preferentially anionic phospholipids. Here we used a thermal denaturation assay and detergent-phospholipid mixed micelles containing KcsA to study the effects of different phospholipids on protein stability. We found that anionic phospholipids stabilize greatly the tetrameric protein against irreversible, heat-induced unfolding and dissociation into subunits. This occurs in a phospholipid concentration-dependent manner, and phosphatidic acid species with acyl chain lengths ranging 14 to 18 carbon atoms are more efficient than similar phosphatidylglycerols in protecting the protein. A docking model of the KcsA-phospholipid complex suggests that the increased protein stability originates from the intersubunit nature of the binding sites and, thus, interaction of the phospholipid with such sites holds together adjacent subunits within the tetrameric protein. We also found that simpler amphiphiles, such as alkyl sulfates longer than 10 carbon atoms, also increase the protein stability to the same extent as anionic phospholipids, although at higher concentrations than the latter. Modeling the interaction of these simpler amphiphiles with KcsA and comparing it with that of anionic phospholipids serve to delineate the features of a hydrophobic pocket in the nonannular sites. Such pocket is predicted to comprise residues from the M2 transmembrane segment of a subunit and from the pore helix of the adjacent subunit and seems most relevant to protein stabilization.

Published

2010

38. Interaction of transmembrane-spanning segments of the alpha2-adrenergic receptor with model membranes.

Author

Prades J, Encinar JA, Funari SS, González-Ros JM, Escribá PV, and Barceló F

Subjects

Calorimetry, Differential Scanning, Cell Membrane chemistry, Fluorescence, Humans, Lipid Bilayers chemistry, Lipid Bilayers metabolism, Peptide Fragments metabolism, Phospholipids chemistry, Phospholipids metabolism, Protein Interaction Domains and Motifs, Protein Structure, Secondary, Protein Structure, Tertiary, Spectroscopy, Fourier Transform Infrared, Temperature, Tryptophan metabolism, Cell Membrane metabolism, Peptide Fragments chemistry, Receptors, Adrenergic, alpha-2 chemistry, Receptors, Adrenergic, alpha-2 metabolism

Abstract

Adrenergic receptors are integral membrane proteins involved in cellular signalling that belong to the G protein-coupled receptors. Synthetic peptides resembling the putative transmembrane (TM) segments TM4, TM6 and TM7, of the human alpha2-adrenergic receptor subtype C10 (P08913) and defined lipid vesicles were used to assess protein-lipid interactions that might be relevant to receptor structure/function. P6 peptide contains the hydrophobic core of TM6 plus the N-terminal hydrophilic motif REKR, while peptides P4 and P7 contained just the hydrophobic stretches of TM4 and TM7, respectively. All the peptides increase their helical tendency at moderate concentrations of TFE (30-50%) and in presence of 1,2-dielaidoyl-sn-glycero-3-phosphatidylethanolamine (DEPE) lipids. However, only P6 displays up to 19% of alpha-helix in the presence of just the DEPE lipids, evidences a transmembrane orientation and stabilizes the Lalpha lipid phase. Conversely, P4 and P7 peptides form only stable beta-sheet structures in DEPE and favour the non-lamellar, inverted hexagonal (H(II)) phase of DEPE by lowering its phase transition temperature. This study highlights the potential of using synthetic peptides derived from the amino acid sequence in the native proteins as templates to understand the behaviour of the transmembrane segments and underline the importance of interfacial anchoring interactions to meet hydrophobic matching requirements and define membrane organization.

Published

2009

39. Protein-promoted membrane domains.

Author

Poveda JA, Fernández AM, Encinar JA, and González-Ros JM

Subjects

Animals, Biophysical Phenomena, Biophysics, Electron Spin Resonance Spectroscopy, Membrane Glycoproteins metabolism, Membrane Lipids chemistry, Membrane Lipids metabolism, Membrane Microdomains metabolism, Membrane Proteins metabolism, Phosphatidic Acids chemistry, Phosphatidic Acids metabolism, Receptors, Nicotinic chemistry, Receptors, Nicotinic metabolism, Viral Envelope Proteins metabolism, Membrane Glycoproteins chemistry, Membrane Microdomains chemistry, Membrane Proteins chemistry, Viral Envelope Proteins chemistry

Abstract

The current notion of biological membranes encompasses a very complex structure, made of dynamically changing compartments or domains where different membrane components partition. These domains have been related to important cellular functions such as membrane sorting, signal transduction, membrane fusion, neuronal maturation, and protein activation. Many reviews have dealt with membrane domains where lipid-lipid interactions direct their formation, especially in the case of raft domains, so in this review we considered domains induced by integral membrane proteins. The nature of the interactions involved and the different mechanisms through which membrane proteins segregate lipid domains are presented, in particular with regard to those induced by the nAChR. It may be concluded that coupling of favourable lipid-lipid and lipid-protein interactions is a general condition for this phenomenon to occur.

Published

2008

40. N-type inactivation of the potassium channel KcsA by the Shaker B "ball" peptide: mapping the inactivating peptide-binding epitope.

Author

Molina ML, Barrera FN, Encinar JA, Renart ML, Fernández AM, Poveda JA, Santoro J, Bruix M, Gavilanes F, Fernández-Ballester G, Neira JL, and González-Ros JM

Subjects

Amino Acid Sequence, Amino Acids chemistry, Electrophysiology, Escherichia coli Proteins chemistry, Lysine chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Conformation, Molecular Sequence Data, Mutation, Peptides chemistry, Potassium Channels, Voltage-Gated, Protein Binding, Spectroscopy, Fourier Transform Infrared, Bacterial Proteins chemistry, Epitopes chemistry, Potassium Channels chemistry

Abstract

The effects of the inactivating peptide from the eukaryotic Shaker BK(+) channel (the ShB peptide) on the prokaryotic KcsA channel have been studied using patch clamp methods. The data show that the peptide induces rapid, N-type inactivation in KcsA through a process that includes functional uncoupling of channel gating. We have also employed saturation transfer difference (STD) NMR methods to map the molecular interactions between the inactivating peptide and its channel target. The results indicate that binding of the ShB peptide to KcsA involves the ortho and meta protons of Tyr(8), which exhibit the strongest STD effects; the C4H in the imidazole ring of His(16); the methyl protons of Val(4), Leu(7), and Leu(10) and the side chain amine protons of one, if not both, the Lys(18) and Lys(19) residues. When a noninactivating ShB-L7E mutant is used in the studies, binding to KcsA is still observed but involves different amino acids. Thus, the strongest STD effects are now seen on the methyl protons of Val(4) and Leu(10), whereas His(16) seems similarly affected as before. Conversely, STD effects on Tyr(8) are strongly diminished, and those on Lys(18) and/or Lys(19) are abolished. Additionally, Fourier transform infrared spectroscopy of KcsA in presence of (13)C-labeled peptide derivatives suggests that the ShB peptide, but not the ShB-L7E mutant, adopts a beta-hairpin structure when bound to the KcsA channel. Indeed, docking such a beta-hairpin structure into an open pore model for K(+) channels to simulate the inactivating peptide/channel complex predicts interactions well in agreement with the experimental observations.

Published

2008

41. Membranes: a meeting point for lipids, proteins and therapies.

Author

Escribá PV, González-Ros JM, Goñi FM, Kinnunen PK, Vigh L, Sánchez-Magraner L, Fernández AM, Busquets X, Horváth I, and Barceló-Coblijn G

Subjects

Animals, Drug Therapy, Humans, Models, Biological, Molecular Structure, Membrane Lipids chemistry, Membrane Lipids metabolism, Membrane Proteins chemistry, Membrane Proteins metabolism

Abstract

Membranes constitute a meeting point for lipids and proteins. Not only do they define the entity of cells and cytosolic organelles but they also display a wide variety of important functions previously ascribed to the activity of proteins alone. Indeed, lipids have commonly been considered a mere support for the transient or permanent association of membrane proteins, while acting as a selective cell/organelle barrier. However, mounting evidence demonstrates that lipids themselves regulate the location and activity of many membrane proteins, as well as defining membrane microdomains that serve as spatio-temporal platforms for interacting signalling proteins. Membrane lipids are crucial in the fission and fusion of lipid bilayers and they also act as sensors to control environmental or physiological conditions. Lipids and lipid structures participate directly as messengers or regulators of signal transduction. Moreover, their alteration has been associated with the development of numerous diseases. Proteins can interact with membranes through lipid co-/post-translational modifications, and electrostatic and hydrophobic interactions, van der Waals forces and hydrogen bonding are all involved in the associations among membrane proteins and lipids. The present study reviews these interactions from the molecular and biomedical point of view, and the effects of their modulation on the physiological activity of cells, the aetiology of human diseases and the design of clinical drugs. In fact, the influence of lipids on protein function is reflected in the possibility to use these molecular species as targets for therapies against cancer, obesity, neurodegenerative disorders, cardiovascular pathologies and other diseases, using a new approach called membrane-lipid therapy.

Published

2008

42. Protein self-assembly and lipid binding in the folding of the potassium channel KcsA.

Author

Barrera FN, Renart ML, Poveda JA, de Kruijff B, Killian JA, and González-Ros JM

Subjects

Bacterial Proteins, Electrophoresis, Polyacrylamide Gel, Escherichia coli Proteins chemistry, Potassium Channels chemistry, Potassium Channels, Voltage-Gated, Spectrometry, Fluorescence, Thermodynamics, Trifluoroethanol chemistry, Escherichia coli Proteins metabolism, Lipid Metabolism, Potassium Channels metabolism

Abstract

Moderate concentrations of the alcohol 2,2,2-trifluoroethanol (TFE) cause the coupled unfolding and dissociation into subunits of the homotetrameric potassium channel KcsA, in a process that is partially irreversible when the protein is solubilized in plain dodecyl beta-d-maltoside (DDM) micelles [Barrera et al. (2005) Biochemistry 44, 14344-52]. Here we report that the transition from the folded tetramer to the unfolded monomer becomes completely reversible when KcsA is solubilized in mixed micelles composed of the detergent DDM and the lipids DOPE (1,2-dioleoyl-sn-glycero-3-phosphoethanolamine) and DOPG (1,2-dioleoyl-sn-glycero-3-[phospho-rac-(1-glycerol)]). This result suggests that lipids may act as effectors in the tetramerization of KcsA. The observed reversibility allowed the determination of the standard free energy of the folding reaction of KcsA: DeltaG = 30.5 +/- 3.1 kcal x mol-1. We also observed that, prior to the unfolding of the tetramer, the presence of lower TFE concentrations causes the disassembly of supramolecular clusters of KcsA into the individual tetrameric molecules. Within the limits of experimental resolution, this is also a reversible process, but unlike the tetramer to monomer transition from above, the level of clustering is not influenced by the presence of solubilized lipids. These observations suggest a distinct role of the lipids in the different in vitro assembly steps (folding/tetramerization and clustering) of KcsA.

Published

2008

43. Interaction of the C-terminal region of the Ggamma protein with model membranes.

Author

Barceló F, Prades J, Encinar JA, Funari SS, Vögler O, González-Ros JM, and Escribá PV

Subjects

Animals, Calorimetry, Differential Scanning, Cattle, Cell Membrane metabolism, GTP-Binding Protein gamma Subunits physiology, Lipids chemistry, Peptides chemistry, Phospholipids chemistry, Protein Binding, Protein Structure, Tertiary, Spectrometry, Fluorescence, Spectroscopy, Fourier Transform Infrared, X-Ray Diffraction, GTP-Binding Protein gamma Subunits chemistry

Abstract

Heterotrimeric G-proteins interact with membranes. They accumulate around membrane receptors and propagate messages to effectors localized in different cellular compartments. G-protein-lipid interactions regulate G-protein cellular localization and activity. Although we recently found that the Gbetagamma dimer drives the interaction of G-proteins with nonlamellar-prone membranes, little is known about the molecular basis of this interaction. Here, we investigated the interaction of the C-terminus of the Ggamma(2) protein (P(gamma)-FN) with model membranes and those of its peptide (P(gamma)) and farnesyl (FN) moieties alone. X-ray diffraction and differential scanning calorimetry demonstrated that P(gamma)-FN, segregated into P(gamma)-FN-poor and -rich domains in phosphatidylethanolamine (PE) and phosphatidylserine (PS) membranes. In PE membranes, FN increased the nonlamellar phase propensity. Fourier transform infrared spectroscopy experiments showed that P(gamma) and P(gamma)-FN interact with the polar and interfacial regions of PE and PS bilayers. The binding of P(gamma)-FN to model membranes is due to the FN group and positively charged amino acids near this lipid. On the other hand, membrane lipids partially altered P(gamma)-FN structure, in turn increasing the fluidity of PS membranes. These data highlight the relevance of the interaction of the C-terminal region of the Ggamma protein with the cell membrane and its effect on membrane structure.

Published

2007

44. Effects of conducting and blocking ions on the structure and stability of the potassium channel KcsA.

Author

Renart ML, Barrera FN, Molina ML, Encinar JA, Poveda JA, Fernández AM, Gómez J, and González-Ros JM

Subjects

Bacterial Proteins, Cations, Monovalent, Escherichia coli Proteins chemistry, Potassium metabolism, Potassium Channels chemistry, Potassium Channels, Voltage-Gated, Sodium metabolism, Spectrometry, Fluorescence, Streptomyces lividans chemistry, Streptomyces lividans metabolism, Structure-Activity Relationship, Thermodynamics, Escherichia coli Proteins antagonists & inhibitors, Escherichia coli Proteins metabolism, Potassium physiology, Potassium Channels metabolism, Sodium physiology

Abstract

This article reports on the interaction of conducting (K(+)) and blocking (Na(+)) monovalent metal ions with detergent-solubilized and lipid-reconstituted forms of the K(+) channel KcsA. Monitoring of the protein intrinsic fluorescence reveals that the two ions bind competitively to KcsA with distinct affinities (dissociation constants for the KcsA.K(+) and KcsA.Na(+) complexes of approximately 8 and 190 mm, respectively) and induce different conformations of the ion-bound protein. The differences in binding affinity as well as the higher K(+) concentration bathing the intracellular mouth of the channel, through which the cations gain access to the protein binding sites, should favor that only KcsA.K(+) complexes are formed under physiological-like conditions. Nevertheless, despite such prediction, it was also found that concentrations of Na(+) well below its dissociation constant and even in the presence of higher K(+) concentrations, cause a remarkable decrease in the protein thermal stability and facilitate thermal dissociation into subunits of the tetrameric KcsA, as concluded from the temperature dependence of the protein infrared spectra and from gel electrophoresis, respectively. These latter observations cannot be explained based on the occupancy of the binding sites from above and suggest that there must be additional ion binding sites, whose occupancy could not be detected by fluorescence and in which the affinity for Na(+) must be higher or at least similar to that of K(+). Moreover, cation binding as reported by means of fluorescence does not suffice to explain the large differences in free energy of stabilization involved in the formation of the KcsA.Na(+) and KcsA.K(+) complexes, which for the most part should arise from synergistic effects of the ion-mediated intersubunit interactions.

Published

2006

45. Clustering and coupled gating modulate the activity in KcsA, a potassium channel model.

Author

Molina ML, Barrera FN, Fernández AM, Poveda JA, Renart ML, Encinar JA, Riquelme G, and González-Ros JM

Subjects

Cell Membrane chemistry, Cell Membrane metabolism, Cell Membrane ultrastructure, Liposomes, Microscopy, Confocal, Patch-Clamp Techniques, Streptomyces lividans, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Ion Channel Gating, Models, Biological, Potassium Channels chemistry, Potassium Channels metabolism

Abstract

Different patterns of channel activity have been detected by patch clamping excised membrane patches from reconstituted giant liposomes containing purified KcsA, a potassium channel from prokaryotes. The more frequent pattern has a characteristic low channel opening probability and exhibits many other features reported for KcsA reconstituted into planar lipid bilayers, including a moderate voltage dependence, blockade by Na(+), and a strict dependence on acidic pH for channel opening. The predominant gating event in this low channel opening probability pattern corresponds to the positive coupling of two KcsA channels. However, other activity patterns have been detected as well, which are characterized by a high channel opening probability (HOP patterns), positive coupling of mostly five concerted channels, and profound changes in other KcsA features, including a different voltage dependence, channel opening at neutral pH, and lack of Na(+) blockade. The above functional diversity occurs correlatively to the heterogeneous supramolecular assembly of KcsA into clusters. Clustering of KcsA depends on protein concentration and occurs both in detergent solution and more markedly in reconstituted membranes, including giant liposomes, where some of the clusters are large enough (up to micrometer size) to be observed by confocal microscopy. As in the allosteric conformational spread responses observed in receptor clustering (Bray, D. and Duke, T. (2004) Annu. Rev. Biophys. Biomol. Struct. 33, 53-73) our tenet is that physical clustering of KcsA channels is behind the observed multiple coupled gating and diverse functional responses.

Published

2006

46. Nicotinic acetylcholine receptor properties are modulated by surrounding lipids: an in vivo study.

Author

Morales A, de Juan E, Fernández-Carvajal AM, Martinez-Pinna J, Poveda JA, Encinar JA, Ivorra I, and González-Ros JM

Subjects

Acetylcholine pharmacology, Animals, Cell Membrane physiology, Cholesterol pharmacology, Patch-Clamp Techniques, Phosphatidylcholines pharmacology, Receptors, Nicotinic drug effects, Torpedo, Lipids pharmacology, Receptors, Nicotinic physiology

Abstract

In vitro studies carried out on liposomes of defined composition showed that nicotinic acetylcholine receptors (nAChRs) are fully functional when they are reconstituted in a heterogeneous lipid matrix, such as that provided by crude soybean (asolectin [R-Aso]) lipids. However, when they are reconstituted in plain phosphatidylcholine (R-PC) lipids, their functional activity is completely lost (Fong and McNamee, 1986). This kind of study also pointed out that phosphatidic acid (PA) and cholesterol (Chol) play an important role in preserving the ability of this protein to exhibit an optimal channel activity (Fong and McNamee, 1986). Furthermore, it has been shown recently that nAChR, itself, induces the formation of specific PA-rich lipid domains (Poveda et al., 2002). Because Xenopus oocytes incorporate functionally into their plasma membrane nAChRs after intracellular injection of liposomes bearing this protein (Morales et al., 1995), the aim of this work was to determine the effect of the reconstitution lipid matrix on the functional properties of the transplanted nAChRs.

Published

2006

47. Antifungal effects and mechanism of action of viscotoxin A3.

Author

Giudici M, Poveda JA, Molina ML, de la Canal L, González-Ros JM, Pfüller K, Pfüller U, and Villalaín J

Subjects

Amino Acid Sequence, Cell Death drug effects, Cell Membrane drug effects, Cell Membrane metabolism, Dose-Response Relationship, Drug, Egtazic Acid analogs & derivatives, Egtazic Acid metabolism, Egtazic Acid pharmacology, Fusarium drug effects, Fusarium metabolism, Lipid Bilayers chemistry, Microscopy, Confocal, Mistletoe metabolism, Mistletoe physiology, Molecular Sequence Data, Plant Leaves enzymology, Plant Preparations metabolism, Plant Preparations pharmacology, Plant Proteins metabolism, Plant Stems enzymology, Protein Binding drug effects, Spores, Fungal drug effects, Spores, Fungal metabolism, Fungi drug effects, Plant Proteins pharmacology

Abstract

Viscotoxins are cationic proteins, isolated from different mistletoe species, that belong to the group of thionins, a group of basic cysteine-rich peptides of approximately 5 kDa. They have been shown to be cytotoxic to different types of cell, including animal, bacterial and fungal. The aim of this study was to obtain information on the cell targets and the mechanism of action of viscotoxin isoform A3 (VtA3). We describe a detailed study of viscotoxin interaction with fungal-derived model membranes, its location inside spores of Fusarium solani, as well as their induced spore death. We show that VtA3 induces the appearance of ion-channel-like activity, the generation of H2O2, and an increase in cytoplasmic free Ca2+. Moreover, we show that Ca2+ is involved in VtA3-induced spore death and increased H2O2 concentration. The data presented here strongly support the notion that the antifungal activity of VtA3 is due to membrane binding and channel formation, leading to destabilization and disruption of the plasma membrane, thereby supporting a direct role for viscotoxins in the plant defence mechanism.

Published

2006

48. Structural and functional changes induced in the nicotinic acetylcholine receptor by membrane phospholipids.

Author

Fernández-Carvajal AM, Encinar JA, Poveda JA, de Juan E, Martínez-Pinna J, Ivorra I, Ferragut JA, Morales A, and González-Ros JM

Subjects

Animals, Cholesterol pharmacology, Kinetics, Membrane Lipids pharmacology, Receptors, Nicotinic drug effects, Spectroscopy, Fourier Transform Infrared, Torpedo, Phospholipids pharmacology, Receptors, Nicotinic chemistry, Receptors, Nicotinic physiology

Abstract

Ligand-gated ion channels (LGICs) constitute an important family of complex membrane proteins acting as receptors for neurotransmitters (Barnard, 1992; Ortells and Lunt, 1995). The nicotinic acetylcholine receptor (nAChR) from Torpedo is the most extensively studied member of the LGIC family and consists of a pentameric transmembrane glycoprotein composed of four different polypeptide subunits (alpha, beta, gamma, and delta) in a 2:1:1:1 stoichiometry (Galzi and Changeux, 1995; Hucho et al., 1996) that are arranged pseudosymmetrically around a central cation-selective ion channel. Conformational transitions, from the closed (nonconducting), to agonist-induced open (ion-conducting), to desensitized (nonconducting) states, are critical for functioning of the nAChR (Karlin, 2002). The ability of the nAChR to undergo these transitions is profoundly influenced by the lipid composition of the bilayer (Barrantes, 2004). Despite existing information on lipid dependence of AChR function, no satisfactory explanation has been given on the molecular events by which specific lipids exert such effects on the activity of an integral membrane protein. To date, several hypotheses have been entertained, including (1) indirect effects of lipids through the alteration of properties of the bilayer, such as fluidity (an optimal fluidity hypothesis [Fong and McNamee, 1986]) or membrane curvature and lateral pressure (Cantor, 1997; de Kruijff, 1997), or (2) direct effects through binding of lipids to defined sites on the transmembrane portion of the protein (Jones and McNamee, 1988; Blanton and Wang, 1990; Fernández et al., 1993; Fernández-Ballester et al., 1994), which has led to the postulation of a possible role of certain lipids as peculiar allosteric ligands of the protein. In this paper we have reconstituted purified AChRs from Torpedo into complex multicomponent lipid vesicles in which the phospholipid composition has been systematically altered. Stopped-flow rapid kinetics of cation translocation and Fourier transform-infrared (FT-IR) spectroscopy studies have been used to illustrate the lipid dependence of both AChR function and AChR secondary structure, respectively.

Published

2006

49. Unfolding and refolding in vitro of a tetrameric, alpha-helical membrane protein: the prokaryotic potassium channel KcsA.

Author

Barrera FN, Renart ML, Molina ML, Poveda JA, Encinar JA, Fernández AM, Neira JL, and González-Ros JM

Subjects

Circular Dichroism, Electrophoresis, Polyacrylamide Gel, Electrophysiology, Protein Denaturation, Sodium Dodecyl Sulfate chemistry, Spectrometry, Fluorescence, Tryptophan chemistry, Bacterial Proteins chemistry, Membrane Proteins chemistry, Potassium Channels chemistry, Protein Folding, Trifluoroethanol chemistry

Abstract

2,2,2-Trifluoroethanol (TFE) effectively destabilizes the otherwise highly stable tetrameric structure of the potassium channel KcsA, a predominantly alpha-helical membrane protein [Valiyaveetil, F. I., Zhou, Y., and MacKinnon, R. (2002) Biochemistry 41, 10771-10777]. Here, we report that the effects on the protein structure of increasing concentrations of TFE in detergent solution include two successive protein concentration-dependent, cooperative transitions. In the first of such transitions, occurring at lower TFE concentrations, the tetrameric KcsA simultaneously increases the exposure of tryptophan residues to the solvent, partly loses its secondary structure, and dissociates into its constituent subunits. Under these conditions, simple dilution of the TFE permits a highly efficient refolding and tetramerization of the protein in the detergent solution. Moreover, following reconstitution into asolectin giant liposomes, the refolded protein exhibits nativelike potassium channel activity, as assessed by patch-clamp methods. Conversely, the second cooperative transition occurring at higher TFE concentrations results in the irreversible denaturation of the protein. These results are interpreted in terms of a protein and TFE concentration-dependent reversible equilibrium between the folded tetrameric protein and partly unfolded monomeric subunits, in which folding and oligomerization (or unfolding and dissociation in the other direction of the equilibrium process) are seemingly coupled processes. At higher TFE concentrations this is followed by the irreversible conversion of the unfolded monomers into a denatured protein form.

Published

2005

50. Proteomic analysis of apical microvillous membranes of syncytiotrophoblast cells reveals a high degree of similarity with lipid rafts.

Author

Paradela A, Bravo SB, Henríquez M, Riquelme G, Gavilanes F, González-Ros JM, and Albar JP

Subjects

Blotting, Western, Cations, Cholesterol chemistry, Chromatography methods, Chromatography, Ion Exchange, Databases, Protein, Humans, Mass Spectrometry, Placenta metabolism, Proteome, Spectrometry, Mass, Electrospray Ionization, Sphingolipids chemistry, Time Factors, Trypsin pharmacology, Membrane Microdomains chemistry, Microvilli metabolism, Proteomics methods, Trophoblasts cytology

Abstract

Brush borders (microvilli) are cell membrane specialized structures that function mainly as high-throughput absortive/secretory areas. It has been well-established that brush borders are particularly rich in membrane lipids characteristic to lipid rafts. Here, we report 57 proteins identified from microvillous membranes (MVM) isolated from human syncytiotrophoblast cells using an experimental method that avoids the use of nonionic detergents. About 60% of the proteins reported here have been described previously as lipid-raft specific. Well-known lipid raft-markers such as Annexin A2 and alkaline phosphatase were identified. Cytoskeleton structural constituents and proteins related with the control and modulation of the cytoskeletal architecture as well as the regulation of the interaction of cytoskeletal constituents with the cell membrane and particularly with lipid raft domains were found (Ezrin, IQGAP1 and 2, EBP50). Other proteins identified include signal transduction molecules, such as Ras-related protein Rab-1B and Rab-7, and ADP-ribosylation factor 1. Several proteins harbor putative post-translational modifications that favor its localization in the lipid-raft environment, such as GPI (alkaline phosphatase and 5'-nucleotidase) and myristoylation (BASP1 and MARCKS). On the whole, this extensive description demonstrates from the protein composition point of view that brush border membranes are indeed highly enriched in lipid raft microdomains.

Published

2005