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与伴侣分子共表达会影响蛋白质的 3D 结构,人类脯氨酰肽酶的失活变异体就是一个例子。

Co-expression with chaperones can affect protein 3D structure as exemplified by loss-of-function variants of human prolidase.

机构信息

Macromolecular Crystallography, Helmholtz-Zentrum Berlin für Materialien und Energie, Berlin, Germany.

出版信息

FEBS Lett. 2020 Sep;594(18):3045-3056. doi: 10.1002/1873-3468.13877. Epub 2020 Jul 14.

Abstract

Prolidase catalyzes the cleavage of dipeptides containing proline on their C terminus. The reduction in prolidase activity is the cause of a rare disease named 'Prolidase Deficiency'. Local structural disorder was indicated as one of the causes for diminished prolidase activity. Previous studies showed that heat shock proteins can partially recover prolidase activity in vivo. To analyze this mechanism of enzymatic activity rescue, we compared the crystal structures of selected prolidase mutants expressed in the absence and in the presence of chaperones. Our results confirm that protein chaperones facilitate the formation of more ordered structures by their substrate protein. These results also suggest that the protein expression system needs to be considered as an important parameter in structural studies. DATABASES: The reported crystal structures and their associated structure factor amplitudes were deposited in the Protein Data Bank under the accession codes 6SRE, 6SRF, and 6SRG, respectively.

摘要

脯肽酶催化 C 末端含有脯氨酸的二肽的裂解。脯肽酶活性的降低是一种名为“脯肽酶缺乏症”的罕见疾病的原因。局部结构无序被认为是脯肽酶活性降低的原因之一。先前的研究表明,热休克蛋白可以在体内部分恢复脯肽酶的活性。为了分析这种酶活性恢复的机制,我们比较了在缺乏和存在伴侣蛋白的情况下表达的选定脯肽酶突变体的晶体结构。我们的结果证实,伴侣蛋白通过其底物蛋白促进更有序结构的形成。这些结果还表明,蛋白质表达系统需要被视为结构研究中的一个重要参数。数据库:报道的晶体结构及其相关的结构因子振幅分别以 6SRE、6SRF 和 6SRG 的登录号存储在蛋白质数据库中。

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