首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Toxicity of an α-Pore-forming Toxin Depends on the Assembly Mechanism on the Target Membrane as Revealed by Single Molecule Imaging
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Toxicity of an α-Pore-forming Toxin Depends on the Assembly Mechanism on the Target Membrane as Revealed by Single Molecule Imaging

机译:α-成孔毒素的毒性取决于单分子成像显示的目标膜的组装机制

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摘要

α-Pore-forming toxins (α-PFTs) are ubiquitous defense tools that kill cells by opening pores in the target cell membrane. Despite their relevance in host/pathogen interactions, very little is known about the pore stoichiometry and assembly pathway leading to membrane permeabilization. Equinatoxin II (EqtII) is a model α-PFT from sea anemone that oligomerizes and forms pores in sphingomyelin-containing membranes. Here, we determined the spatiotemporal organization of EqtII in living cells by single molecule imaging. Surprisingly, we found that on the cell surface EqtII did not organize into a unique oligomeric form. Instead, it existed as a mixture of oligomeric species mostly including monomers, dimers, tetramers, and hexamers. Mathematical modeling based on our data supported a new model in which toxin clustering happened in seconds and proceeded via condensation of EqtII dimer units formed upon monomer association. Furthermore, altering the pathway of EqtII assembly strongly affected its toxic activity, which highlights the relevance of the assembly mechanism on toxicity.
机译:α-孔形成毒素(α-PFT)是普遍存在的防御工具,可通过打开靶细胞膜上的孔来杀死细胞。尽管它们在宿主/病原体相互作用中具有相关性,但对于导致膜透化的孔化学计量和组装途径了解甚少。 Equinatoxin II(EqtII)是来自海葵的α-PFT模型,可在含鞘磷脂的膜中低聚并形成孔。在这里,我们通过单分子成像确定了活细胞中EqtII的时空组织。出乎意料的是,我们发现EqtII在细胞表面没有组织成独特的寡聚形式。相反,它以低聚物质的混合物形式存在,主要包括单体,二聚体,四聚体和六聚体。基于我们数据的数学模型支持了一种新模型,其中毒素聚集在几秒钟内发生,并通过单体缔合时形成的EqtII二聚体单元的缩合进行。此外,改变EqtII装配的途径强烈影响其毒性活性,这突出了装配机理与毒性的相关性。

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