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脂膜介导的功能性淀粉样肽 Somatostatin-14 的组装。

Lipid membrane-mediated assembly of the functional amyloid-forming peptide Somatostatin-14.

机构信息

School of Science, STEM College, RMIT University, Melbourne, Australia.

ISA, Department of Physics and Astronomy, Aarhus University, DK-8000 Aarhus C, Denmark.

出版信息

Biophys Chem. 2022 Aug;287:106830. doi: 10.1016/j.bpc.2022.106830. Epub 2022 May 21.

DOI:10.1016/j.bpc.2022.106830
PMID:35635892
Abstract

Membrane-mediated assembly has been well characterised for toxic amyloid species such as the amyloid-β peptide implicated in Alzheimer's disease. However, little is known about the membrane-mediated assembly of functional-amyloid forming peptides, recently identified as a natural storage state for neuropeptide hormones in vivo. Here, we study the aggregation of somatostatin-14 (SST-14) co-incubated with model lipid membranes. Atomic force microscopy (AFM) studies confirmed that nanofibrils formed in the presence of various lipid membranes display reduced fibrillogenesis and promote the formation of non-fibrillar oligomers. Both circular dichroism (CD) and intrinsic tryptophan fluorescence studies confirmed interaction between the peptide and the lipid bilayer; this interaction appears to drive changes in membrane-mediated aggregation kinetics. We show that both the surface charge of the membrane and chain packing drive changes in the electrostatic and hydrophobic interactions between the peptide and the membrane, and hence the rate of assembly. The similarities in the effect of the lipid membrane on aggregation of functional amyloids and the more well studied toxic amyloids suggest strong aggregation modifying lipid bilayer interactions are a ubiquitous feature of all amyloid fibrils and highlight the need for further investigation as to why this leads to toxicity in some systems and not others.

摘要

膜介导的组装在毒性淀粉样物质中得到了很好的描述,例如与阿尔茨海默病相关的淀粉样-β肽。然而,对于功能性淀粉样形成肽的膜介导组装知之甚少,这些肽最近被确定为体内神经肽激素的天然储存状态。在这里,我们研究了生长抑素-14(SST-14)与模型脂质膜共孵育时的聚集。原子力显微镜(AFM)研究证实,在各种脂质膜存在的情况下形成的纳米原纤维显示出减少的纤维化并促进无纤维寡聚物的形成。圆二色性(CD)和本征色氨酸荧光研究均证实了肽与脂质双层之间的相互作用;这种相互作用似乎驱动了膜介导聚集动力学的变化。我们表明,膜的表面电荷和链堆积都驱动了肽与膜之间的静电和疏水性相互作用的变化,从而改变了组装的速度。脂质膜对功能性淀粉样聚集的影响与研究更为深入的毒性淀粉样物质相似,这表明强烈的聚集修饰脂质双层相互作用是所有淀粉样纤维的普遍特征,并强调需要进一步研究为什么这会导致一些系统而不是其他系统的毒性。

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