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通过核磁共振研究富含脯氨酸的蛋白质与黄烷-3-醇之间的相互作用:天然未折叠蛋白质中的残余结构为配体提供锚定点。

Study of the interactions between a proline-rich protein and a flavan-3-ol by NMR: residual structures in the natively unfolded protein provides anchorage points for the ligands.

作者信息

Pascal Christine, Paté Franck, Cheynier Véronique, Delsuc Marc-André

机构信息

INRA-UMR Sciences Pour l'Oenologie (SPO), 2 place Pierre Viala, Montpellier F34060, France.

出版信息

Biopolymers. 2009 Sep;91(9):745-56. doi: 10.1002/bip.21221.

Abstract

Astringency is one of the major organoleptic properties of food and beverages that are made from plants, such as tea, chocolate, beer, or red wine. This sensation is thought to be due to interactions between tannins and salivary proline-rich proteins, which are natively unfolded proteins. A human salivary proline-rich protein, namely IB-5, was produced by the recombinant method. Its interactions with a model tannin, epigallocatechin gallate (EGCG), the major flavan-3-ol in green tea, were studied here. Circular dichroism experiments showed that IB-5 presents residual structures (PPII helices) when the ionic strength is close to that in saliva. In the presence of these residual structures, IB-5 undergoes an increase in structural content upon binding to EGCG. NMR data corroborated the presence of preformed structural elements within the protein prior to binding and a partial assignment was proposed, showing partial structuration. TOCSY experiments showed that amino acids that are involved in PPII helices are more likely to interact with EGCG than those in random coil regions, as if they were anchorage points for the ligand. The signal from IB-5 in the DOSY NMR spectrum revealed an increase in polydispersity upon addition of EGCG while the mean hydrodynamic radius remained unchanged. This strongly suggests the formation of IB-5/EGCG aggregates.

摘要

涩味是由植物制成的食品和饮料(如茶、巧克力、啤酒或红酒)的主要感官特性之一。这种感觉被认为是由于单宁与富含唾液脯氨酸的蛋白质之间的相互作用所致,这些蛋白质是天然未折叠的蛋白质。通过重组方法制备了一种人类富含唾液脯氨酸的蛋白质,即IB-5。在此研究了它与模型单宁表没食子儿茶素没食子酸酯(EGCG,绿茶中的主要黄烷-3-醇)的相互作用。圆二色性实验表明,当离子强度接近唾液中的离子强度时,IB-5呈现出残余结构(II型聚脯氨酸螺旋)。在这些残余结构存在的情况下,IB-5与EGCG结合后结构含量增加。核磁共振数据证实了蛋白质在结合前存在预先形成的结构元件,并提出了部分归属,显示出部分结构化。全相关谱实验表明,与随机卷曲区域的氨基酸相比,参与II型聚脯氨酸螺旋的氨基酸更有可能与EGCG相互作用,就好像它们是配体的锚定点。扩散排序核磁共振谱中IB-5的信号显示,加入EGCG后多分散性增加,而平均流体动力学半径保持不变。这有力地表明形成了IB-5/EGCG聚集体。

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