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脂质不饱和度对幽门螺杆菌HP(2 - 20)抗菌肽类似物HPA3膜相互作用的影响。

The role played by lipids unsaturation upon the membrane interaction of the Helicobacter pylori HP(2-20) antimicrobial peptide analogue HPA3.

作者信息

Mereuta Loredana, Luchian Tudor, Park Yoonkynung, Hahm Kyung-Soo

机构信息

Faculty of Physices, Laboratory of Biophysics and Medical Physics, Alexandru I. Cuza' University, Blvd. King Carol I, No. 11, Iasi R-700506, Roumania.

出版信息

J Bioenerg Biomembr. 2009 Feb;41(1):79-84. doi: 10.1007/s10863-009-9204-z. Epub 2009 Mar 18.

DOI:10.1007/s10863-009-9204-z
PMID:19294495
Abstract

The HPA3 peptide is an analogue of the linear antimicrobial peptide, HP(2-20), isolated from the N-terminal region of the Helicobacter pylori ribosomal protein, able to interact with zwitterionic lipid membranes and generate pores. Herein we focused on the importance of the degree of unsaturation of lipid acyl chains on HPA3 peptide-membrane interactions. Electrophysiology experiments carried out in reconstituted lipid membranes formed from phosphatidylcholines with one (1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine - POPC) and two monounsaturated acyl chains (1,2-dioleoyl-sn-glycero-3-phosphocholine - DOPC) demonstrate that the lesser degree of the packing density of membrane lipids encountered in DOPC-based planar membranes greatly enhances the electric activity of pores created by the HPA3 peptide. Data derived from fluorescence spectroscopy experiments demonstrate that upon interaction with the bilayer, the HPA3 peptide translocates to the trans-side of the membrane. From the same experiments, we demonstrate that in the case of DOPC-based planar membranes, the net amount of HPA3 peptide which passes across the membrane and re-dissolves in the trans solution is almost 22% greater than POPC-based membranes. Such data further emphasize the modulatory role played by lipid acyl chain in determining antimicrobial peptides-lipids interactions, and demonstrate that small differences in unsaturation degree can impose a sizeable influence on HPA3 peptide activity.

摘要

HPA3肽是一种线性抗菌肽HP(2 - 20)的类似物,从幽门螺杆菌核糖体蛋白的N端区域分离得到,能够与两性离子脂质膜相互作用并形成孔道。在此,我们聚焦于脂质酰基链的不饱和度对HPA3肽与膜相互作用的重要性。在由含有一条单不饱和酰基链(1 - 棕榈酰 - 2 - 油酰 - sn - 甘油 - 3 - 磷酸胆碱 - POPC)和两条单不饱和酰基链(1,2 - 二油酰 - sn - 甘油 - 3 - 磷酸胆碱 - DOPC)的磷脂酰胆碱形成的重构脂质膜中进行的电生理学实验表明,基于DOPC的平面膜中膜脂的堆积密度较低,这极大地增强了HPA3肽形成的孔道的电活性。荧光光谱实验数据表明,与双层膜相互作用时,HPA3肽会转移到膜的反面。从相同实验中,我们证明,在基于DOPC的平面膜的情况下,穿过膜并重新溶解在反面溶液中的HPA3肽的净量比基于POPC的膜几乎大22%。这些数据进一步强调了脂质酰基链在确定抗菌肽与脂质相互作用中所起的调节作用,并表明不饱和度的微小差异会对HPA3肽的活性产生相当大的影响。

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