Literature DB >> 28000294

Disrupting a key hydrophobic pair in the oligomerization interface of the actinoporins impairs their pore-forming activity.

Haydeé Mesa-Galloso1, Karelia H Delgado-Magnero1,2, Sheila Cabezas1, Aracelys López-Castilla3, Jorge E Hernández-González1, Lohans Pedrera1, Carlos Alvarez1, D Peter Tieleman2, Ana J García-Sáez4, Maria E Lanio1, Uris Ros1,4, Pedro A Valiente1.   

Abstract

Crystallographic data of the dimeric and octameric forms of fragaceatoxin C (FraC) suggested the key role of a small hydrophobic protein-protein interaction surface for actinoporins oligomerization and pore formation in membranes. However, site-directed mutagenesis studies supporting this hypothesis for others actinoporins are still lacking. Here, we demonstrate that disrupting the key hydrophobic interaction between V60 and F163 (FraC numbering scheme) in the oligomerization interface of FraC, equinatoxin II (EqtII), and sticholysin II (StII) impairs the pore formation activity of these proteins. Our results allow for the extension of the importance of FraC protein-protein interactions in the stabilization of the oligomeric intermediates of StII and EqtII pointing out that all of these proteins follow a similar pathway of membrane disruption. These findings support the hybrid pore proposal as the universal model of actinoporins pore formation. Moreover, we reinforce the relevance of dimer formation, which appears to be a functional intermediate in the assembly pathway of some different pore-forming proteins.
© 2016 The Protein Society.

Entities:  

Keywords:  dimeric intermediate; molecular dynamic simulations; oligomerization in membranes; pore-forming toxins; protein-lipid pore

Mesh:

Substances:

Year:  2017        PMID: 28000294      PMCID: PMC5326555          DOI: 10.1002/pro.3104

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  72 in total

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4.  A self-consistent method for the analysis of protein secondary structure from circular dichroism.

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5.  Effects of lipid composition on membrane permeabilization by sticholysin I and II, two cytolysins of the sea anemone Stichodactyla helianthus.

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Journal:  Biophys J       Date:  2001-06       Impact factor: 4.033

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Authors:  J W Doyle; W R Kem; F A Vilallonga
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8.  Molecular determinants of sphingomyelin specificity of a eukaryotic pore-forming toxin.

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Journal:  J Biol Chem       Date:  2008-04-28       Impact factor: 5.157

9.  Incomplete pneumolysin oligomers form membrane pores.

Authors:  Andreas F-P Sonnen; Jürgen M Plitzko; Robert J C Gilbert
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Authors:  Valeria Antonini; Victor Pérez-Barzaga; Silvia Bampi; David Pentón; Diana Martínez; Mauro Dalla Serra; Mayra Tejuca
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  8 in total

1.  Membrane Remodeling by the Lytic Fragment of SticholysinII: Implications for the Toroidal Pore Model.

Authors:  Haydee Mesa-Galloso; Pedro A Valiente; Mario E Valdés-Tresanco; Raquel F Epand; Maria E Lanio; Richard M Epand; Carlos Alvarez; D Peter Tieleman; Uris Ros
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2.  Emerging Diversity in Lipid-Protein Interactions.

Authors:  Valentina Corradi; Besian I Sejdiu; Haydee Mesa-Galloso; Haleh Abdizadeh; Sergei Yu Noskov; Siewert J Marrink; D Peter Tieleman
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Review 3.  Biophysical and biochemical strategies to understand membrane binding and pore formation by sticholysins, pore-forming proteins from a sea anemone.

Authors:  Carlos Alvarez; Uris Ros; Aisel Valle; Lohans Pedrera; Carmen Soto; Yadira P Hervis; Sheila Cabezas; Pedro A Valiente; Fabiola Pazos; Maria E Lanio
Journal:  Biophys Rev       Date:  2017-08-29

4.  Self-homodimerization of an actinoporin by disulfide bridging reveals implications for their structure and pore formation.

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5.  Multigene Family of Pore-Forming Toxins from Sea Anemone Heteractis crispa.

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Review 7.  Panorama of the Intracellular Molecular Concert Orchestrated by Actinoporins, Pore-Forming Toxins from Sea Anemones.

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8.  Structural and functional analysis of Hydra Actinoporin-Like Toxin 1 (HALT-1).

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  8 in total

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