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尿素促进β-乳球蛋白淀粉样纤维形成的动力学研究。

A kinetic study of beta-lactoglobulin amyloid fibril formation promoted by urea.

作者信息

Hamada Daizo, Dobson Christopher M

机构信息

Division of Physical Chemistry, Institute for Protein Research, Osaka University, 3-2 Yamadaoka, Suita, Japan.

出版信息

Protein Sci. 2002 Oct;11(10):2417-26. doi: 10.1110/ps.0217702.

Abstract

The formation of fibrillar aggregates by beta-lactoglobulin in the presence of urea has been monitored by using thioflavin T fluorescence and transmission electron microscopy (TEM). Large quantities of aggregated protein were formed by incubating beta-lactoglobulin in 3-5 M urea at 37 degrees C and pH 7.0 for 10-30 days. The TEM images of the aggregates in 3-5 M urea show the presence of fibrils with diameters of 8-10 nm, and increases in thioflavin T fluorescence are indicative of the formation of amyloid structures. The kinetics of spontaneous fibrillogenesis detected by thioflavin T fluorescence show sigmoidal behavior involving a clear lag phase. Moreover, addition of preformed fibrils into protein solutions containing urea shows that fibril formation can be accelerated by seeding processes that remove the lag phase. Both of these findings are indicative of nucleation-dependent fibril formation. The urea concentration where fibril formation is most rapid, both for seeded and unseeded solutions, is approximately 5.0 M, close to the concentration of urea corresponding to the midpoint of unfolding (5.3 M). This result indicates that efficient fibril formation involves a balance between the requirement of a significant population of unfolded or partially unfolded molecules and the need to avoid conditions that strongly destabilize intermolecular interactions.

摘要

通过硫黄素T荧光和透射电子显微镜(TEM)监测了β-乳球蛋白在尿素存在下形成纤维状聚集体的过程。将β-乳球蛋白在37℃、pH 7.0的3-5 M尿素中孵育10-30天,形成了大量聚集蛋白。3-5 M尿素中聚集体的TEM图像显示存在直径为8-10 nm的纤维,硫黄素T荧光的增加表明淀粉样结构的形成。通过硫黄素T荧光检测到的自发纤维形成动力学呈S形,包括明显的延迟期。此外,将预先形成的纤维添加到含有尿素的蛋白质溶液中表明,通过消除延迟期的接种过程可以加速纤维形成。这两个发现都表明纤维形成是依赖成核的。对于接种和未接种的溶液,纤维形成最快时的尿素浓度约为5.0 M,接近对应于解折叠中点(5.3 M)的尿素浓度。这一结果表明,有效的纤维形成涉及大量未折叠或部分未折叠分子的需求与避免强烈破坏分子间相互作用条件的需求之间的平衡。

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