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折叠成β-发夹结构可以防止淀粉样纤维的形成。

Folding into a beta-hairpin can prevent amyloid fibril formation.

作者信息

Hosia Waltteri, Bark Niklas, Liepinsh Edvards, Tjernberg Agneta, Persson Bengt, Hallén Dan, Thyberg Johan, Johansson Jan, Tjernberg Lars

机构信息

Department of Medical Biochemistry and Biophysics, Karolinska Institutet, S-171 77 Stockholm, Sweden.

出版信息

Biochemistry. 2004 Apr 27;43(16):4655-61. doi: 10.1021/bi036248t.

Abstract

The tetrapeptide KFFE is one of the shortest amyloid fibril-forming peptides described. Herein, we have investigated how the structural environment of this motif affects polymerization. Using a turn motif (YNGK) or a less rigid sequence (AAAK) to fuse two KFFE tetrapeptides, we show by several biophysical methods that the amyloidogenic properties are strongly dependent on the structural environment. The dodecapeptide KFFEAAAKKFFE forms abundant thick fibril bundles. Freshly dissolved KFFEAAAKKFFE is monomeric and shows mainly disordered secondary structure, as evidenced by circular dichroism, NMR spectroscopy, hydrogen/deuterium exchange measurements, and molecular modeling studies. In sharp contrast, the dodecapeptide KFFEYNGKKFFE does not form fibrils but folds into a stable beta-hairpin. This structure can oligomerize into a stable 12-mer and multiples thereof, as shown by size exclusion chromatography, sedimentation analysis, and electrospray mass spectrometry. These data indicate that the structural context in which a potential fibril forming sequence is present can prevent fibril formation by favoring self-limiting oligomerization over polymerization.

摘要

四肽KFFE是所描述的最短的形成淀粉样纤维的肽之一。在此,我们研究了该基序的结构环境如何影响聚合反应。使用一个转角基序(YNGK)或一个刚性较小的序列(AAAK)连接两个KFFE四肽,我们通过多种生物物理方法表明,淀粉样生成特性强烈依赖于结构环境。十二肽KFFEAAAKKFFE形成大量粗大的纤维束。新溶解的KFFEAAAKKFFE是单体,主要呈现无序二级结构,这通过圆二色性、核磁共振光谱、氢/氘交换测量以及分子模拟研究得以证明。形成鲜明对比的是,十二肽KFFEYNGKKFFE不形成纤维,而是折叠成稳定的β-发夹结构。如尺寸排阻色谱、沉降分析和电喷雾质谱所示,这种结构可以寡聚成稳定的十二聚体及其倍数。这些数据表明,潜在的形成纤维序列所处的结构背景可以通过促进自我限制的寡聚化而非聚合反应来阻止纤维形成。

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