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Three-dimensional domain swapping in the folded and molten-globule states of cystatins an amyloid-forming structural superfamily

机译:胱抑素的折叠态和熔融球态的三维域交换胱抑素是淀粉样蛋白形成的结构超家族

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摘要

Cystatins, an amyloid-forming structural superfamily, form highly stable, domain-swapped dimers at physiological protein concentrations. In chicken cystatin, the active monomer is a kinetic trap en route to dimerization, and any changes in solution conditions or mutations that destabilize the folded state shorten the lifetime of the monomeric form. In such circumstances, amyloidogenesis will start from conditions where a domain-swapped dimer is the most prevalent species. Domain swapping occurs by a rearrangement of loop I, generating the new intermonomer interface between strands 2 and 3. The transition state for dimerization has a high level of hydrophobic group exposure, indicating that gross conformational perturbation is required for domain swapping to occur. Dimerization also occurs when chicken cystatin is in its reduced, molten-globule state, implying that the organization of secondary structure in this state mirrors that in the folded state and that domain swapping is not limited to the folded states of proteins. Although the interface between cystatin-fold units is poorly defined for cystatin A, the dimers are the appropriate size to account for the electron-dense regions in amyloid protofilaments.
机译:胱抑素是淀粉样蛋白形成的结构超家族,在生理蛋白浓度下会形成高度稳定的结构域交换二聚体。在鸡肉半胱氨酸蛋白酶抑制剂中,活性单体是二聚化过程中的动力学陷阱,溶液条件的任何变化或使折叠状态不稳定的突变都会缩短单体形式的寿命。在这种情况下,淀粉样蛋白生成将从域交换二聚体为最普遍的物种开始。域交换是通过环I的重排而发生的,从而在链2和3之间生成新的单体界面。二聚化的过渡态具有高水平的疏水基团暴露,表明域交换发生需要总体构象扰动。当鸡半胱氨酸蛋白酶抑制剂处于其还原的熔融球状状态时,也会发生二聚化,这表明该状态下的二级结构的组织与折叠状态下的结构镜像相同,并且域交换不限于蛋白质的折叠状态。尽管对于半胱氨酸蛋白酶抑制剂A,半胱氨酸蛋白酶抑制剂-折叠单元之间的界面定义不明确,但是二聚体的大小合适,以解释淀粉样蛋白原丝中的电子致密区域。

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