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δ-溶血素在磷脂酰胆碱囊泡中诱导的染料外排和脂质翻转的动力学以及两亲性α-螺旋肽的分级释放机制。

Kinetics of dye efflux and lipid flip-flop induced by delta-lysin in phosphatidylcholine vesicles and the mechanism of graded release by amphipathic, alpha-helical peptides.

作者信息

Pokorny Antje, Almeida Paulo F F

机构信息

Department of Chemistry and Biochemistry, University of North Carolina, Wilmington, North Carolina 28403, USA.

出版信息

Biochemistry. 2004 Jul 13;43(27):8846-57. doi: 10.1021/bi0497087.

Abstract

Delta-lysin is a 26-residue, amphipathic, alpha-helical peptide of bacterial origin. Its specificity is to some extent complementary to that of antimicrobial peptides. Therefore, understanding its mechanism is important for the more general goal of understanding the interaction of amphipathic peptides with membranes. In this article, we show that delta-lysin induces graded efflux of the contents of phosphatidylcholine vesicles. In view of this finding, carboxyfluorescein efflux kinetics were re-examined. In addition, peptide-induced lipid flip-flop was directly measured using fluorescence energy transfer between two lipid fluorophores initially placed on opposite leaflets of the bilayer. Carboxyfluorescein efflux and lipid flip-flop occur with essentially identical rate constants. On the basis of a detailed, quantitative analysis of the kinetics of peptide-vesicle interactions, we conclude that the peptide translocates across the bilayer as a small, transient aggregate, most likely a trimer. Dye efflux and lipid flip-flop occur concomitantly with the transient peptide-induced perturbation of the membrane. The experimental data are interpreted by comparing the predictions of the available models for the mechanism of action of amphipathic alpha-helical peptides. We demonstrate how the combination of the quantitative kinetic analysis, graded efflux, and reversibility of the peptide-vesicle interaction can be used to reject several models for this particular peptide. Two models are compatible with the data, the toroidal pore model and the sinking raft model. On the basis of the small aggregate size, a trimer, the latter appears to be more plausible. Some significant modifications are introduced in the sinking raft model to take into account the new finding of graded dye release. Furthermore, we present an explanation for the phenomenon of graded release in general, which, contrary to all-or-none efflux, has not been well-understood.

摘要

δ-溶血素是一种由细菌产生的、含有26个氨基酸残基的两亲性α-螺旋肽。其特异性在一定程度上与抗菌肽互补。因此,了解其作用机制对于更全面地理解两亲性肽与膜的相互作用这一目标具有重要意义。在本文中,我们表明δ-溶血素可诱导磷脂酰胆碱囊泡内容物的分级外排。鉴于这一发现,我们重新研究了羧基荧光素的外排动力学。此外,利用最初位于双层膜相对小叶上的两种脂质荧光团之间的荧光能量转移,直接测量了肽诱导的脂质翻转。羧基荧光素外排和脂质翻转的速率常数基本相同。基于对肽-囊泡相互作用动力学的详细定量分析,我们得出结论,该肽以小的瞬时聚集体形式穿过双层膜,最有可能是三聚体。染料外排和脂质翻转与肽诱导的膜瞬时扰动同时发生。通过比较两亲性α-螺旋肽作用机制的现有模型的预测结果来解释实验数据。我们展示了如何利用定量动力学分析、分级外排以及肽-囊泡相互作用的可逆性来排除该特定肽的几种模型。有两种模型与数据相符,即环形孔模型和下沉筏模型。基于三聚体这种小聚集体的大小,后者似乎更合理。在下沉筏模型中引入了一些重大修改,以考虑分级染料释放这一新发现。此外,我们对分级释放现象给出了一般性解释,与全或无外排相反,分级释放现象尚未得到很好的理解。

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