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病毒融合肽在压缩脂质单分子层中的多态性与相互作用

Polymorphism and interactions of a viral fusion peptide in a compressed lipid monolayer.

作者信息

Schwarz G, Taylor S E

机构信息

Department of Biophysical Chemistry, Biocenter of the University, University of Basel, CH-4056 Basel, Switzerland.

出版信息

Biophys J. 1999 Jun;76(6):3167-75. doi: 10.1016/S0006-3495(99)77468-0.

Abstract

With a view toward possible new insights into viral fusion mechanisms, we have investigated the HIV-1 gp41 fusion peptide in a monomolecular film of the biomembrane lipid palmitoyloleoylphosphatidylcholine. Its surface activity at an air/water interface was measured under equilibrium conditions, using the conventional Langmuir trough technique. Through a novel thermodynamic analysis, the partial molecular area of the peptide in the lipid moiety could be determined as a function of the lateral pressure and the interfacial peptide/lipid ratio. This indicates an orientation of the peptide backbone parallel to the lipid hydrocarbon tails. The molecular area decreases significantly upon monolayer compression, suggesting a conformational transition from a somewhat compact configuration to a more extended, presumably beta-strand structure when a lipid packing density is approached that is generally believed to mimic the physical state of a biological membrane. Up to a lateral pressure of approximately 15 mN/m, practically all peptide inserts into the lipid monolayer. At higher compression a distinct partitioning into the aqueous subphase is observed. Under these conditions the data also reflect a strong aggregation of the lipid-associated peptide. Beyond a critical peptide/lipid ratio, the peptide's area requirement was found to become substantially enhanced, possibly because of the formation of water-filled pores.

摘要

为了对病毒融合机制有新的见解,我们研究了生物膜脂质棕榈油酰磷脂酰胆碱单分子膜中的HIV-1 gp41融合肽。使用传统的Langmuir槽技术,在平衡条件下测量了其在空气/水界面的表面活性。通过新颖的热力学分析,可以确定肽在脂质部分的部分分子面积与侧向压力和界面肽/脂质比的函数关系。这表明肽主链与脂质烃尾平行的取向。单层压缩时分子面积显著减小,这表明当接近通常认为模拟生物膜物理状态的脂质堆积密度时,肽从某种紧密构象转变为更伸展的、可能是β-链结构。在侧向压力约为15 mN/m之前,几乎所有肽都插入脂质单层中。在更高的压缩下,观察到明显地分配到水相亚相中。在这些条件下,数据还反映了脂质相关肽的强烈聚集。超过临界肽/脂质比时,发现肽的面积需求大幅增加,可能是由于形成了充满水的孔。

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Conformational transitions of membrane-bound HIV-1 fusion peptide.
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本文引用的文献

3
The molecular area characteristics of the HIV-1 gp41-fusion peptide at the air/water interface. Effect of pH.
Biochim Biophys Acta. 1997 Jun 12;1326(2):257-64. doi: 10.1016/s0005-2736(97)00029-1.
4
Lateral pressure in membranes.膜中的侧向压力。
Biochim Biophys Acta. 1996 Oct 29;1286(3):183-223. doi: 10.1016/s0304-4157(96)00009-3.
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Peptide models for membrane channels.膜通道的肽模型。
Biochem J. 1996 Apr 15;315 ( Pt 2)(Pt 2):345-61. doi: 10.1042/bj3150345.

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