组氨酸残基对病毒孔蛋白跨膜螺旋的影响。

Q3 Biochemistry, Genetics and Molecular Biology
Molecular Membrane Biology Pub Date : 2013-11-01 Epub Date: 2013-10-09 DOI:10.3109/09687688.2013.842657
Yan Wang, Sang Ho Park, Ye Tian, Stanley J Opella
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引用次数: 5

摘要

通过比较病毒蛋白“u”(Vpu)和M2质子通道的TM螺旋,探讨组氨酸在跨膜螺旋通道形成中的作用。这两种蛋白都是病毒孔蛋白家族的成员,这是一种具有离子通道活性的小膜蛋白,并且具有能够形成低聚物的单个TM螺旋。两种蛋白的TM螺旋在c端都有一个保守的色氨酸。以前,Vpu的丙氨酸18突变为组氨酸,以人工引入与M2相同的HXXXW基序,该基序对质子通道活性至关重要。有趣的是,与野生型Vpu TM相比,突变的Vpu TM导致脂质双层螺旋倾斜角度增加了11°。我们发现相反的情况,当M2中HXXXW基序的组氨酸37突变为丙氨酸时,它使螺旋倾角比野生型M2降低了10°。倾斜变化与螺旋长度和色氨酸的存在无关。此外,与野生型M2相比,H37A突变体对质子浓度的敏感性降低。我们还发现含组氨酸的M2比不含组氨酸的M2的溶剂可得性更大。这表明TM螺旋可能通过改变其倾斜角度来增加溶剂暴露,以便在疏水膜区域内容纳极性/带电残留物。M2、Vpu及其突变体的比较结果表明,组氨酸在跨膜螺旋结构中的重要性,以及单个氨基酸位点的变化对离子通道功能和结构的显著可塑性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Impact of histidine residues on the transmembrane helices of viroporins.

Impact of histidine residues on the transmembrane helices of viroporins.

Impact of histidine residues on the transmembrane helices of viroporins.

Abstract The role of histidine in channel-forming transmembrane (TM) helices was investigated by comparing the TM helices from Virus protein 'u' (Vpu) and the M2 proton channel. Both proteins are members of the viroporin family of small membrane proteins that exhibit ion channel activity, and have a single TM helix that is capable of forming oligomers. The TM helices from both proteins have a conserved tryptophan towards the C-terminus. Previously, alanine 18 of Vpu was mutated to histidine in order to artificially introduce the same HXXXW motif that is central to the proton channel activity of M2. Interestingly, the mutated Vpu TM resulted in an increase in helix tilt angle of 11° in lipid bilayers compared to the wild-type Vpu TM. Here, we find the reverse, when histidine 37 of the HXXXW motif in M2 was mutated to alanine, it decreased the helix tilt by 10° from that of wild-type M2. The tilt change is independent of both the helix length and the presence of tryptophan. In addition, compared to wild-type M2, the H37A mutant displayed lowered sensitivity to proton concentration. We also found that the solvent accessibility of histidine-containing M2 is greater than without histidine. This suggests that the TM helix may increase the solvent exposure by changing its tilt angle in order to accommodate a polar/charged residue within the hydrophobic membrane region. The comparative results of M2, Vpu and their mutants demonstrated the significance of histidine in a transmembrane helix and the remarkable plasticity of the function and structure of ion channels stemming from changes at a single amino acid site.

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来源期刊
Molecular Membrane Biology
Molecular Membrane Biology 生物-生化与分子生物学
CiteScore
4.80
自引率
0.00%
发文量
0
审稿时长
>12 weeks
期刊介绍: Cessation. Molecular Membrane Biology provides a forum for high quality research that serves to advance knowledge in molecular aspects of biological membrane structure and function. The journal welcomes submissions of original research papers and reviews in the following areas: • Membrane receptors and signalling • Membrane transporters, pores and channels • Synthesis and structure of membrane proteins • Membrane translocation and targeting • Lipid organisation and asymmetry • Model membranes • Membrane trafficking • Cytoskeletal and extracellular membrane interactions • Cell adhesion and intercellular interactions • Molecular dynamics and molecular modelling of membranes. • Antimicrobial peptides.
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