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定制裂解肽引起的膜裂解动力学及肽在膜中的取向

Kinetics of membrane lysis by custom lytic peptides and peptide orientations in membrane.

作者信息

Chen H M, Clayton A H, Wang W, Sawyer W H

机构信息

Department of Biochemistry, Hong Kong University of Science and Technology, Kowloon, Hong Kong.

出版信息

Eur J Biochem. 2001 Mar;268(6):1659-69. doi: 10.1046/j.1432-1327.2001.02039.x.

Abstract

To aid the development of custom peptide antibiotics, a kinetic study of membrane lysis by cecropin B (CB) and its analogs, cecropin B1 (CB1) and cecropin B3 (CB3) was carried out to determine the mechanism by which these peptides disrupt the bilayer structure of liposomes of defined composition. Disruption of the phospholipid bilayer was determined by a fluorescence assay involving the use of dithionite to quench the fluorescence of lipids labeled with N-7-nitro-2,1,3-benzoxadiazol-4-yl. Lytic peptides caused the disruption of liposomes to occur in two kinetic steps. For liposomes composed of mixtures of phosphatidylcholine and phosphatidic acid, the time constants for each kinetic step were shorter for CB and CB1 than for CB3. Oriented circular dichroism experiments showed that the peptides could exist in at least two different membrane-associated states that differed primarily in the orientation of the helical segments with respect to the bilayer surface. The results are discussed in terms of kinetic mechanisms of membrane lysis. The mode of actions of these peptides used for the interpretation of their kinetic mechanisms were supported by surface plasmon resonance experiments including or excluding the pore-forming activities.

摘要

为了辅助定制肽类抗生素的研发,开展了一项关于天蚕素B(CB)及其类似物天蚕素B1(CB1)和天蚕素B3(CB3)对膜裂解的动力学研究,以确定这些肽破坏特定组成脂质体双层结构的机制。通过一种荧光测定法来确定磷脂双层的破坏情况,该测定法使用连二亚硫酸盐淬灭用N - 7 - 硝基 - 2,1,3 - 苯并恶二唑 - 4 - 基标记的脂质的荧光。裂解肽导致脂质体的破坏分两个动力学步骤发生。对于由磷脂酰胆碱和磷脂酸混合物组成的脂质体,CB和CB1每个动力学步骤的时间常数比CB3的短。取向圆二色性实验表明,这些肽可以以至少两种不同的膜相关状态存在,主要区别在于螺旋片段相对于双层表面的取向。根据膜裂解的动力学机制对结果进行了讨论。这些肽用于解释其动力学机制的作用模式得到了包括或排除成孔活性的表面等离子体共振实验的支持。

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