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人胱抑素C是一种淀粉样蛋白,通过三维结构域交换形成二聚体。

Human cystatin C, an amyloidogenic protein, dimerizes through three-dimensional domain swapping.

作者信息

Janowski R, Kozak M, Jankowska E, Grzonka Z, Grubb A, Abrahamson M, Jaskolski M

机构信息

Department of Crystallography, Faculty of Chemistry, A. Mickiewicz University, Grunwaldzka 6, 60-780 Poznan, Poland.

出版信息

Nat Struct Biol. 2001 Apr;8(4):316-20. doi: 10.1038/86188.

Abstract

The crystal structure of human cystatin C, a protein with amyloidogenic properties and a potent inhibitor of cysteine proteases, reveals how the protein refolds to produce very tight two-fold symmetric dimers while retaining the secondary structure of the monomeric form. The dimerization occurs through three-dimensional domain swapping, a mechanism for forming oligomeric proteins. The reconstituted monomer-like domains are similar to chicken cystatin except for one inhibitory loop that unfolds to form the 'open interface' of the dimer. The structure explains the tendency of human cystatin C to dimerize and suggests a mechanism for its aggregation in the brain arteries of elderly people with amyloid angiopathy. A more severe 'conformational disease' is associated with the L68Q mutant of human cystatin C, which causes massive amyloidosis, cerebral hemorrhage and death in young adults. The structure of the three-dimensional domain-swapped dimers shows how the L68Q mutation destabilizes the monomers and makes the partially unfolded intermediate less unstable. Higher aggregates may arise through the three-dimensional domain-swapping mechanism occurring in an open-ended fashion in which partially unfolded molecules are linked into infinite chains.

摘要

人胱抑素C是一种具有淀粉样变性特性的蛋白质,也是半胱氨酸蛋白酶的有效抑制剂,其晶体结构揭示了该蛋白质如何重新折叠以产生非常紧密的双轴对称二聚体,同时保留单体形式的二级结构。二聚化通过三维结构域交换发生,这是一种形成寡聚蛋白的机制。重组后的单体样结构域与鸡胱抑素相似,只是有一个抑制环展开形成二聚体的“开放界面”。该结构解释了人胱抑素C二聚化的倾向,并提示了其在患有淀粉样血管病的老年人脑动脉中聚集的机制。一种更严重的“构象疾病”与人类胱抑素C的L68Q突变体有关,该突变体在年轻人中会导致大量淀粉样变性、脑出血和死亡。三维结构域交换二聚体的结构显示了L68Q突变如何使单体不稳定,并使部分展开的中间体更不易稳定。更高的聚集体可能通过三维结构域交换机制以开放式方式产生,其中部分展开的分子连接成无限链。

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