Recombinant Kv Channels at the Membrane of Escherichia coli Bind Specifically Agitoxin2

Nekrasova, Oksana V.; Ignatova, Anastasia A.; Nazarova, Anna; Feofanov, Аlexey V.; Korolkova, Yuliya V.; Boldyreva, E. F.; Tagvei, Anna I.; Grishin, Eugene V.; Arseniev, Alexander S.; Kirpichnikov, Mikhaǐl P.

doi:10.1007/s11481-008-9116-4

Cited by 18 publications

(15 citation statements)

References 40 publications

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“…Kv1 channels were studied using flow cytometry (60), single molecule fluorescent microscopy (61), and the analysis of membrane potential changes using fluorescent dyes and fluorescence readers (62). Recently, a convenient fluorescent screening system based on KcsA-Kv1.3 hybrid receptors was developed and applied successfully to screen Orthochirus scrobiculosus venom for peptide toxins, which specifically target the pore region of Kv1.3 (36,38). This system, which represents an efficient, robust, and rapid binding assay, is a powerful alternative to radioligand and patch clamp techniques.…”

Section: Discussionmentioning

confidence: 99%

“…KcsA-Kv1.1 is readily expressed in E. coli and forms tetramers in the plasma membrane with the outer pore vestibule of the channel oriented extracellularly. Spheroplasts prepared from E. coli cells with membrane-embedded KcsA-Kv1.1 bind specifically fluorescently labeled agitoxin-2 (R-AgTx2) (38). Therefore, RAgTx2 and spheroplasts bearing KcsA-Kv1.1 can be used as components of a fluorescent system for investigation of Kv1.1 ligands just as it was realized recently for the KcsA-Kv1.3 system (36).…”

Section: P-loop (mentioning

confidence: 97%

“…coli BL21(DE3) cells that express KcsA-Kv1.1 proteins in the inner membrane were obtained as described earlier (37,38). Cell cultivation and preparation of spheroplasts were performed as described elsewhere (36).…”

Section: Poly(a)mentioning

confidence: 99%

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Variability of Potassium Channel Blockers in Mesobuthus eupeus Scorpion Venom with Focus on Kv1.1

Kuzmenkov

Vassilevski

Kudryashova

et al. 2015

Journal of Biological Chemistry

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Background: Scorpion venoms are an ample source of toxins targeting potassium channels. Results: A comprehensive search for new toxins was performed by combining transcriptomics and peptidomics with a fluorescent test system. Conclusion: We identified five new high affinity potassium channel blockers in the venom of Mesobuthus eupeus. Significance: The proposed integrated approach is of general utility for potassium channel pharmacology.

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Section: Discussionmentioning

confidence: 99%

Section: P-loop (mentioning

confidence: 97%

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Variability of Potassium Channel Blockers in Mesobuthus eupeus Scorpion Venom with Focus on Kv1.1

Kuzmenkov

Vassilevski

Kudryashova

et al. 2015

Journal of Biological Chemistry

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“…For this, we used a procedure for binding KcsA-Kv1.3 to a fluorescently labeled peptide toxin - agitoxin2, on the entire surface of E. coli cells [26]. Agitoxin (AgTx2), a 38-a.a. peptide from the venom of a scorpion, Leiurus quinquestriatus, is an effective blocker of the Kv1.3 channel [27].…”

Section: Resultsmentioning

confidence: 99%

Studying of Membrane Localization of Recombinant Potassium Channels in E.coli

et al. 2009

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The effective expression of recombinant membrane proteins in E.coli depends upon the targeting and insertion of proteins into the cellular membrane, as well as on those proteins adopting the correct spatial structure. A significant technological problem involves the design of approaches for detecting the location of target proteins within a host cell. Using a hybrid potassium channel KcsA-Kv1.3 as a model, we developed a technological scheme which is suitable for the study of membrane localization in E.coli cells of recombinant proteins containing voltage-gated eukaryotic potassium channels as the functional active site. The scheme involves both biochemical and fluorescent methods for detecting target proteins in the cytoplasmic membrane of E.coli, as well as the study of the ligand-binding activity of membrane-embedded proteins.

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“…The authors present the recent data about domain organization of eukaryotic potassium voltage-gated ion channels and discuss the interaction between the domains and the corresponding conformational changes upon activation of the channel. This theme is continued in a study by Nekrasova et al (2008), which reports on a new bacterial cell-based system, suitable for study of interactions between ligands and ligand-binding sites of eukaryotic Kv1.3 and Kv1.1 channels. This new system may be useful for screening of ligands to membrane-embedded pharmaceutical targets.…”

mentioning

confidence: 99%

Nanobiology for the Pharmacology of Cellular Ion Channels

Kabanov

Kirpichnikov

Хохлов

2009

J Neuroimmune Pharmacol

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Writing this editorial is especially pleasing. First, it provides us an opportunity to introduce new directives to the field of Neuroimmune Pharmacology and to explain why the field of nanomedicine is likely an important part of its future growth and development. Second, it is an opportunity to showcase research in this area currently operative in Russia that may not be readily accessible to the readership. Third, it is a platform to better explain why the Journal Editorial leadership was enthusiastic about the science and its relationship to the Society on NeuroImmune Pharmacology strategic goals. All are brought to bear in this issue of the Journal of Neuroimmune Pharmacology. The issue includes articles presented at a recent joint US-Russian workshop entitled, "Health in the 21st Century: Nanomedicine and Self-Organization of Biological Systems" held at M.V. Lomonosov Moscow State University (MSU), Moscow, Russia, December 10-11, 2007. The conjoint meeting was organized through the Departments of Biology, Chemistry, and Physics, MSU and by the Center for Drug Delivery and Nanomedicine and Department of Pharmacology and Experimental Neuroscience, University of Nebraska Medical Center (Omaha, NE). The speakers included established internationally regarded scientists from these institutions as well as graduate students and faculties at MSU. In addition to selected papers by workshop contributors, we have included several papers closely aligned to the theme of nanomedicine and nanopharmacology of the central nervous system in order to provide a biological anchor for this research. We understand that such works are new to many but hope that its organization and interdisciplinary approaches will appeal to this audience. All together, it is our hope that, by gathering basic and clinical scientists with the common interest of using nanotechnology in the delivery of therapeutic agents with a focus on nanopharmacology and complex supramolecular biological assembly, the papers included will provide a platform for thought, discussion, and future translational research.

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Recombinant Kv Channels at the Membrane of Escherichia coli Bind Specifically Agitoxin2

Cited by 18 publications

References 40 publications

Variability of Potassium Channel Blockers in Mesobuthus eupeus Scorpion Venom with Focus on Kv1.1

Variability of Potassium Channel Blockers in Mesobuthus eupeus Scorpion Venom with Focus on Kv1.1

Studying of Membrane Localization of Recombinant Potassium Channels in E.coli

Nanobiology for the Pharmacology of Cellular Ion Channels

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