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从准外消旋混合物中结晶对映体纯蛋白质:通过同位素标记的酯胰岛素和人胰岛素的X射线衍射进行结构测定

Crystallization of Enantiomerically Pure Proteins from Quasi-Racemic Mixtures: Structure Determination by X-Ray Diffraction of Isotope-Labeled Ester Insulin and Human Insulin.

作者信息

Mandal Kalyaneswar, Dhayalan Balamurugan, Avital-Shmilovici Michal, Tokmakoff Andrei, Kent Stephen B H

机构信息

Department of Chemistry, University of Chicago, 929 East 57th Street, Chicago, IL, 60637, USA.

出版信息

Chembiochem. 2016 Mar 2;17(5):421-5. doi: 10.1002/cbic.201500600. Epub 2016 Feb 10.

Abstract

As a part of a program aimed towards the study of the dynamics of human insulin-protein dimer formation using two-dimensional infrared spectroscopy, we used total chemical synthesis to prepare stable isotope labeled [(1-(13) C=(18) O)Phe(B24) )] human insulin, via [(1-(13) C=(18) O)Phe(B24) )] ester insulin as a key intermediate product that facilitates folding of the synthetic protein molecule (see preceding article). Here, we describe the crystal structure of the synthetic isotope-labeled ester insulin intermediate and the product synthetic human insulin. Additionally, we present our observations on hexamer formation with these two proteins in the absence of phenol derivatives and/or Zn metal ions. We also describe and discuss the fractional crystallization of quasi-racemic protein mixtures containing each of these two synthetic proteins.

摘要

作为利用二维红外光谱研究人胰岛素 - 蛋白质二聚体形成动力学的项目的一部分,我们采用全化学合成法,通过[(1-(13)C=(18)O)Phe(B24))]酯胰岛素作为促进合成蛋白质分子折叠的关键中间产物,制备稳定同位素标记的[(1-(13)C=(18)O)Phe(B24))]人胰岛素(见前文)。在此,我们描述了合成同位素标记的酯胰岛素中间体和产物合成人胰岛素的晶体结构。此外,我们展示了在不存在酚类衍生物和/或锌金属离子的情况下,这两种蛋白质形成六聚体的观察结果。我们还描述并讨论了包含这两种合成蛋白质的准外消旋蛋白质混合物的分步结晶。

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