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短杆菌肽A在脂质膜中形成孔道。

Pore formation in lipid membranes by alamethicin.

作者信息

Fringeli U P, Fringeli M

出版信息

Proc Natl Acad Sci U S A. 1979 Aug;76(8):3852-6. doi: 10.1073/pnas.76.8.3852.

Abstract

The conformation of the linear peptide antibiotic alamethicin in dipalmitoyl phosphatidylcholine multilayers was investigated in the absence of an electric field by means of infrared attenuated total reflection spectroscopy. Alamethicin was found to be incorporated into the lipid membrane not only in the dry state but also in an aqueous environment. Its molecular conformation, however, changed from a helix when dry to an extended chain when aqueous. The extended chain aggregated to di- and multimers spanning the lipid bilayer. The equilibrium concentration of alamethicin in the surrounding water was 90 nM, which is in the range of concentrations used in black film experiments. The corresponding molar ratio of lipid to peptide was 80:1. Concerning the molecular mechanism of electric field-induced pore formation, one has to conclude that the dipole model proposed by several authors is very unlikely because it is based on the assumption that the major part of alamethicin is adsorbed on the membrane surface, from which small amounts flip into the membrane under the influence of an electric field. An alternative mechanism is proposed, based on a field-induced conformational change of the peptide from the extended state to a helix. This transition is favored by the resulting dipole moment of the alamethicin helix.

摘要

利用红外衰减全反射光谱法,在无电场条件下研究了线性肽抗生素阿拉米辛在二棕榈酰磷脂酰胆碱多层膜中的构象。研究发现,阿拉米辛不仅能以干燥状态掺入脂质膜,在水环境中也能掺入。然而,其分子构象在干燥时为螺旋结构,在水环境中则变为伸展链结构。伸展链聚集成跨越脂质双层的二聚体和多聚体。阿拉米辛在周围水中的平衡浓度为90 nM,这处于黑膜实验所用的浓度范围内。脂质与肽的相应摩尔比为80:1。关于电场诱导孔形成的分子机制,不得不推断几位作者提出的偶极子模型极不可能,因为该模型基于这样的假设:阿拉米辛的主要部分吸附在膜表面,在电场影响下少量翻转进入膜内。基于肽从伸展状态到螺旋结构的场诱导构象变化,提出了一种替代机制。阿拉米辛螺旋产生的偶极矩有利于这种转变。

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Pore formation in lipid membranes by alamethicin.短杆菌肽A在脂质膜中形成孔道。
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