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Folding mechanism of the c(h)2 antibody domain.

机译:c(h)2抗体域的折叠机制。

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摘要

The immunoglobulin C(H)2 domain is a simple model system suitable for the study of the folding of all-beta-proteins. Its structure consists of two beta-sheets forming a greek-key beta-barrel, which is stabilized by an internal disulfide bridge located in the hydrophobic core. Crystal structures of various antibodies suggest that the C(H)2 domains of the two heavy chains interact with their sugar moieties and form a homodimer. Here, we show that the isolated, unglycosylated C(H)2 domain is a monomeric protein. Equilibrium unfolding was a two-state process, and the conformational stability is remarkably low compared to other antibody domains. Folding kinetics of C(H)2 were found to consist of several phases. The reactions could be mapped to three parallel pathways, two of which are generated by prolyl isomerizations in the unfolded state. The slowest folding reaction, which was observed only after long-term denaturation, could be catalyzed by a prolyl isomerase. The majority of the unfolded molecules, however, folded more rapidly, on a time-scale of minutes. Presumably, these molecules also have to undergo prolyl isomerization before reaching the native state. In addition, we detected a small number of fast-folding molecules in which all proline residues appear to be in the correct conformation. On both prolyl isomerization limited pathways, the formation of partly structured intermediates could be observed.
机译:免疫球蛋白C(H)2结构域是一个简单的模型系统,适合研究全β蛋白的折叠。它的结构由两个形成希腊式beta-barrel的beta-sheets组成,并由位于疏水核中的内部二硫键稳定。各种抗体的晶体结构表明两条重链的C(H)2域与它们的糖部分相互作用并形成同型二聚体。在这里,我们表明分离的,未糖基化的C(H)2域是一种单体蛋白。平衡展开是两个过程,与其他抗体结构域相比,构象稳定性非常低。发现C(H)2的折叠动力学包括几个阶段。该反应可以被映射到三个平行的途径,其中两个是由未折叠状态的脯氨酰异构化产生的。仅在长期变性后才观察到的最慢的折叠反应可以被脯氨酰异构酶催化。然而,大多数未折叠分子在几分钟的时间尺度上折叠得更快。据推测,这些分子在达到天然状态之前还必须进行脯氨酰异构化。此外,我们检测到少量快速折叠分子,其中所有脯氨酸残基似乎都具有正确的构象。在两个脯氨酰异构化受限的途径上,都可以观察到部分结构化中间体的形成。

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