| Literature DB >> 26351738 |
Nejc Rojko1, Mauro Dalla Serra2, Peter Maček3, Gregor Anderluh4.
Abstract
Actinoporins (APs) from sea anemones are ~20 kDa pore forming toxins with a β-sandwich structure flanked by two α-helices. The molecular mechanism of APs pore formation is composed of several well-defined steps. APs bind to membrane by interfacial binding site composed of several aromatic amino acid residues that allow binding to phosphatidylcholine and specific recognition of sphingomyelin. Subsequently, the N-terminal α-helix from the β-sandwich has to be inserted into the lipid/water interphase in order to form a functional pore. Functional studies and single molecule imaging revealed that only several monomers, 3-4, oligomerise to form a functional pore. In this model the α-helices and surrounding lipid molecules build toroidal pore. In agreement, AP pores are transient and electrically heterogeneous. On the contrary, crystallized oligomers of actinoporin fragaceatoxin C were found to be composed of eight monomers with no lipids present between the adjacent α-helices. This article is part of a Special Issue entitled: Pore-Forming Toxins edited by Maur Dalla Serra and Franco Gambale.Entities:
Keywords: Actinoporin; Equinatoxin; Fragaceatoxin; Pore formation; Sphingomyelin; Sticholysin
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Year: 2015 PMID: 26351738 DOI: 10.1016/j.bbamem.2015.09.007
Source DB: PubMed Journal: Biochim Biophys Acta ISSN: 0006-3002