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Configuration of influenza hemagglutinin fusion peptide monomers and oligomers in membranes

机译:膜中流感血凝素融合肽单体和寡聚体的构型

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摘要

The 20 N-terminal residues of the HA2 subunit of influenza hemagglutinin (HA), known as the fusion peptide, play a crucial role in membrane fusion. Molecular dynamics simulations with implicit solvation are employed here to study the structure and orientation of the fusion peptide in membranes. As a monomer the alpha-helical peptide adopts a shallow, slightly tilted orientation along the lipid tail-head group interface. The average angle of the peptide with respect to membrane plane is 12.4 degrees. We find that the kinked structure proposed on the basis of NMR data is not stable in our model because of the high energy cost related to the membrane insertion of polar groups. Because hemagglutinin-mediated membrane fusion is promoted by low pH, we examined the effect of protonation of the Glu and Asp residues. The configurations of the protonated peptides were slightly deeper in the membrane but at similar angles. Finally, because HA is a trimer, we modeled helical fusion peptide trimers. We find that oligomerization affects the insertion depth of the peptide and its orientation with respect to the membrane: a trimer exhibits equally favorable configurations in which some or all of the helices in the bundle insert obliquely deep into the membrane. (c) 2006 Elsevier B.V. All rights reserved.
机译:流感血凝素(HA)的HA2亚基的20个N末端残基(称为融合肽)在膜融合中起关键作用。此处使用具有隐性溶剂化的分子动力学模拟来研究融合​​肽在膜中的结构和方向。作为单体,α-螺旋肽沿脂质尾-头基团界面采用浅的,略微倾斜的取向。肽相对于膜平面的平均角度为12.4度。我们发现基于NMR数据提出的纽结结构在我们的模型中不稳定,因为与极性基团的膜插入相关的能源成本很高。由于低pH值可促进血凝素介导的膜融合,因此我们研究了Glu和Asp残基质子化的影响。质子化肽的构型在膜中稍深,但角度相似。最后,由于HA是三聚体,因此我们对螺旋融合肽三聚体进行了建模。我们发现低聚影响肽的插入深度及其相对于膜的取向:三聚体表现出同样有利的构型,其中束中的一些或全部螺旋斜向深深地插入膜中。 (c)2006 Elsevier B.V.保留所有权利。

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