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两亲性α-螺旋肽HP(2 - 20)及其源自幽门螺杆菌的类似物:在各种脂质组成中的成孔机制。

Amphipathic alpha-helical peptide, HP (2-20), and its analogues derived from Helicobacter pylori: pore formation mechanism in various lipid compositions.

作者信息

Park Seong-Cheol, Kim Mi-Hyun, Hossain Mohammed Akhter, Shin Song Yub, Kim Yangmee, Stella Lorenzo, Wade John D, Park Yoonkyung, Hahm Kyung-Soo

机构信息

Research Center for Proteineous Materials (RCPM), Chosun University, Gwangju, Korea.

出版信息

Biochim Biophys Acta. 2008 Jan;1778(1):229-41. doi: 10.1016/j.bbamem.2007.09.020. Epub 2007 Oct 2.

DOI:10.1016/j.bbamem.2007.09.020
PMID:17961502
Abstract

In a previous study, we determined that HP(2-20) (residues 2-20 of parental HP derived from the N-terminus of Helicobacter pylori Ribosomal Protein L1) and its analogue, HPA3, exhibit broad-spectrum antimicrobial activity. The primary objective of the present study was to gain insight into the relevant mechanisms of action using analogues of HP(2-20) together with model liposomes of various lipid compositions and electron microscopy. We determined that these analogues, HPA3 and HPA3NT3, exert potent antibacterial effects in low-salt buffer and antifungal activity against chitin-containing fungi, while having little or no hemolytic activity or cytotoxicity against mammalian cell lines. Our examination of the interaction of HP(2-20) and its analogues with liposomes showed that the peptides disturb both neutral and negatively-charged membranes, as demonstrated by the release of encapsulated fluorescent markers. The release of fluorescent markers induced by HP(2-20) and its analogues was inversely related to marker size. The pore created by HP(2-20) shows that the radius is approximately 1.8 nm, whereas HPA3, HPA3NT3, and melittin have apparent radii between 3.3 and 4.8 nm. Finally, as shown by electron microscopy, the liposomes and various microbial cells treated with HPA3 and HPA3NT3 showed oligomerization and blebbing similar to that seen with melittin, while HP(2-20) exhibited flabbiness. These results suggest that HP(2-20) may exert its antibiotic effects through a small pore (about 1.8 nm), whereas HPA3 and HPA3NT3 formed pores of a size consistent with those formed by melittin.

摘要

在之前的一项研究中,我们确定了HP(2 - 20)(源自幽门螺杆菌核糖体蛋白L1 N端的亲本HP的2 - 20位残基)及其类似物HPA3具有广谱抗菌活性。本研究的主要目的是通过使用HP(2 - 20)类似物以及各种脂质组成的模型脂质体和电子显微镜来深入了解相关作用机制。我们确定这些类似物HPA3和HPA3NT3在低盐缓冲液中发挥强大的抗菌作用,并对含几丁质的真菌具有抗真菌活性,而对哺乳动物细胞系几乎没有溶血活性或细胞毒性。我们对HP(2 - 20)及其类似物与脂质体相互作用的研究表明,这些肽会干扰中性和带负电荷的膜,这通过封装的荧光标记物的释放得以证明。HP(2 - 20)及其类似物诱导的荧光标记物释放与标记物大小呈负相关。由HP(2 - 20)形成的孔显示其半径约为1.8 nm,而HPA3、HPA3NT3和蜂毒肽的表观半径在3.3至4.8 nm之间。最后,如电子显微镜所示,用HPA3和HPA3NT3处理的脂质体和各种微生物细胞显示出与蜂毒肽相似的寡聚化和起泡现象,而HP(2 - 20)则表现出松弛现象。这些结果表明,HP(2 - 20)可能通过一个小孔(约1.8 nm)发挥其抗生素作用,而HPA3和HPA3NT3形成的孔大小与蜂毒肽形成的孔一致。

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