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精氨酸-芳环相互作用及其对精氨酸诱导的芳族溶质增溶和抑制蛋白质聚集的影响。

Arginine-aromatic interactions and their effects on arginine-induced solubilization of aromatic solutes and suppression of protein aggregation.

机构信息

Chemical & Pharmaceutical Engineering Program, The Singapore-MIT Alliance, National University of Singapore, Singapore.

出版信息

Biotechnol Prog. 2012 Jan-Feb;28(1):223-31. doi: 10.1002/btpr.710. Epub 2011 Sep 21.

DOI:10.1002/btpr.710
PMID:21948347
Abstract

We examine the interaction of aromatic residues of proteins with arginine, an additive commonly used to suppress protein aggregation, using experiments and molecular dynamics simulations. An aromatic-rich peptide, FFYTP (a segment of insulin), and lysozyme and insulin are used as model systems. Mass spectrometry shows that arginine increases the solubility of FFYTP by binding to the peptide, with the simulations revealing the predominant association of arginine to be with the aromatic residues. The calculations further show a positive preferential interaction coefficient, Γ(XP), contrary to conventional thinking that positive Γ(XP)'s indicate aggregation rather than suppression of aggregation. Simulations with lysozyme and insulin also show arginine's preference for aromatic residues, in addition to acidic residues. We use these observations and earlier results reported by us and others to discuss the possible implications of arginine's interactions with aromatic residues on the solubilization of aromatic moieties and proteins. Our results also highlight the fact that explanations based purely on Γ(XP), which measures average affinity of an additive to a protein, could obscure or misinterpret the underlying molecular mechanisms behind additive-induced suppression of protein aggregation.

摘要

我们使用实验和分子动力学模拟研究了芳香族残基与精氨酸的相互作用,精氨酸是一种常用的添加剂,可抑制蛋白质聚集。我们使用富含芳香族残基的肽 FFYTP(胰岛素的一个片段)、溶菌酶和胰岛素作为模型系统。质谱分析表明,精氨酸通过与肽结合增加了 FFYTP 的溶解度,模拟结果显示精氨酸与芳香族残基的主要结合方式。计算进一步表明,正优先相互作用系数 Γ(XP)为正,与传统观点相反,传统观点认为正 Γ(XP)表明聚集而不是抑制聚集。溶菌酶和胰岛素的模拟也表明,除了酸性残基外,精氨酸还偏爱芳香族残基。我们利用这些观察结果以及我们和其他人之前的研究结果,讨论了精氨酸与芳香族残基相互作用对芳香族部分和蛋白质溶解的可能影响。我们的研究结果还强调了一个事实,即仅基于 Γ(XP)(衡量添加剂与蛋白质平均亲和力的指标)的解释可能会掩盖或误解添加剂诱导抑制蛋白质聚集的潜在分子机制。

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Arginine-aromatic interactions and their effects on arginine-induced solubilization of aromatic solutes and suppression of protein aggregation.精氨酸-芳环相互作用及其对精氨酸诱导的芳族溶质增溶和抑制蛋白质聚集的影响。
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