Protein engineering modulates the transport properties and ion selectivity of the pores formed by staphylococcal gamma-haemolysins in lipid membranes. - Wikidata - wikimedia - TriplyDB

Protein engineering modulates the transport properties and ion selectivity of the pores formed by staphylococcal gamma-haemolysins in lipid membranes.

Protein engineering modulates the transport properties and ion selectivity of the pores formed by staphylococcal gamma-haemolysins in lipid membranes.

http://www.wikidata.org/entity/Q42678423

about

Crystal structure of the octameric pore of staphylococcal γ-hemolysin reveals the β-barrel pore formation mechanism by two components Molecular Architecture and Functional Analysis of NetB, a Pore-forming Toxin from Clostridium perfringens Crystal structure of leucotoxin S component: new insight into the Staphylococcal beta-barrel pore-forming toxins Membrane damage by an α-helical pore-forming protein, Equinatoxin II, proceeds through a succession of ordered steps Distinction between pore assembly by staphylococcal alpha-toxin versus leukotoxins.Homologous versus heterologous interactions in the bicomponent staphylococcal gamma-haemolysin pore.Ion channels and bacterial infection: the case of beta-barrel pore-forming protein toxins of Staphylococcus aureus.The bicomponent pore-forming leucocidins of Staphylococcus aureus Effects of MACPF/CDC proteins on lipid membranes.Heavy chain-only antibodies and tetravalent bispecific antibody neutralizing Staphylococcus aureus leukotoxins Single-molecule imaging of cooperative assembly of gamma-hemolysin on erythrocyte membranes.Protein conducting channels-mechanisms, structures and applications.Engineered covalent leucotoxin heterodimers form functional pores: insights into S-F interactions.Internalization of staphylococcal leukotoxins that bind and divert the C5a receptor is required for intracellular Ca2+mobilization by human neutrophils p-Sulfonato-calix[n]arenes inhibit staphylococcal bicomponent leukotoxins by supramolecular interactions The equinatoxin N-terminus is transferred across planar lipid membranes and helps to stabilize the transmembrane pore

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P2860

Protein engineering modulates the transport properties and ion selectivity of the pores formed by staphylococcal gamma-haemolysins in lipid membranes.

http://www.wikidata.org/entity/Q42678423

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2002 nî lūn-bûn

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Protein engineering modulates ...... aemolysins in lipid membranes.

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Protein engineering modulates ...... aemolysins in lipid membranes.

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Protein engineering modulates ...... aemolysins in lipid membranes.

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P356

J.1365-2958.2002.02943.X

P1433

Molecular Microbiology

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Protein engineering modulates ...... aemolysins in lipid membranes.

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P2093

Didier A Colin

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Gianfranco Menestrina

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Gilles Prévost

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Henri Monteil

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Manuela Coraiola

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Massimiliano Comai

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Sandra Werner

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P2860

An Algorithm for Least-Squares Estimation of Nonlinear Parameters

The structure of a Staphylococcus aureus leucocidin component (LukF-PV) reveals the fold of the water-soluble species of a family of transmembrane pore-forming toxins

Crystal structure of staphylococcal LukF delineates conformational changes accompanying formation of a transmembrane channel

Structure of staphylococcal alpha-hemolysin, a heptameric transmembrane pore

STAPHYLOCOCCAL TOXIN.

Mode of action of beta-barrel pore-forming toxins of the staphylococcal alpha-hemolysin family.

A new cytotoxin from Bacillus cereus that may cause necrotic enteritis.

The interaction of Staphylococcus aureus bi-component gamma-hemolysins and leucocidins with cells and lipid membranes.

The use and misuse of FTIR spectroscopy in the determination of protein structure.

Infrared spectroscopy of proteins and peptides in lipid bilayers.

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1251-1267

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scholarly article

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10.1046/J.1365-2958.2002.02943.X

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5

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Mauro Dalla Serra

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2002-06-01T00:00:00Z

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229505148

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12068809

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