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倾斜肽:历史

Tilted peptides: the history.

作者信息

Thomas Annick, Brasseur Robert

机构信息

Centre de Biophysique Moléculaire Numérique, FSAGx, Passage des déportés, 2, 5030 Belgium.

出版信息

Curr Protein Pept Sci. 2006 Dec;7(6):523-7. doi: 10.2174/138920306779025594.

Abstract

Nature has selected peptide motifs for protein functions. It is clear that specific sequence motifs can identify families of enzymes. These sequence motifs are one dimensional signatures and nature has also developed two dimension motifs which cannot be read in the one dimension of sequence language but can be detected in the three dimensional properties of a secondary structure. One of such motifs is tilted peptides. They do not correspond to any consensus of sequence but correspond to a consensus motif where hydrophobicity balance is used as a functional device. In the nineteen eighties, the first tilted peptide was deciphered from the sequence of a virus fusion protein by molecular modelling. It was described as a protein fragment hydrophobic enough to insert into a membrane but too short to span it. The fragment exhibited an asymmetric distribution of hydrophobicity along the helix long axis and hence, was unable to lie parallel or perpendicular to a membrane surface but adopted an orientation in between. Hydrophobicity motif was a very new and very challenging concept and tilted peptides were rapidly found to be involved in several mechanisms of virus fusion. They were also found to be involved in protein secretion and future studies could establish their involvement in the destabilization of 3D protein structures and in the alpha to beta transconformations, which drive the generation of amyloid deposits.

摘要

自然界为蛋白质功能选择了肽基序。显然,特定的序列基序可以识别酶家族。这些序列基序是一维特征,而且自然界还发展出了二维基序,它们无法从序列语言的一维中读取,但可以在二级结构的三维特性中检测到。其中一种基序就是倾斜肽。它们不对应任何序列共识,而是对应一种以疏水性平衡作为功能手段的共识基序。在20世纪80年代,通过分子建模从病毒融合蛋白的序列中解析出了首个倾斜肽。它被描述为一个疏水性足以插入膜中但又太短而无法跨越膜的蛋白质片段。该片段沿螺旋长轴呈现出不对称的疏水性分布,因此,它既不能与膜表面平行也不能垂直,而是采取介于两者之间的取向。疏水性基序是一个非常新颖且极具挑战性的概念,人们很快发现倾斜肽参与了病毒融合的多种机制。它们还被发现与蛋白质分泌有关,未来的研究可能会证实它们参与了三维蛋白质结构的不稳定以及α-螺旋向β-折叠的转变,而这种转变会促使淀粉样沉积物的形成。

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