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通过具有高配对特异性的四半胱氨酸肽实现蛋白质的铰链型二聚化

Hinge-Type Dimerization of Proteins by a Tetracysteine Peptide of High Pairing Specificity.

作者信息

Schrimpf Andreas, Hempel Franziska, Li Aitao, Linne Uwe, Maier Uwe G, Reetz Manfred T, Geyer Armin

机构信息

Department of Chemistry , Philipps-Universität Marburg , Hans-Meerwein-Straße 4 , 35032 Marburg , Germany.

Department of Biology , Philipps-Universität Marburg , Karl-von-Frisch-Straße 8 , 35043 Marburg , Germany.

出版信息

Biochemistry. 2018 Jul 3;57(26):3658-3664. doi: 10.1021/acs.biochem.8b00475. Epub 2018 Jun 14.

Abstract

Dimeric disulfide-linked peptides are formed by the regioselective oxidative folding of thiol precursors containing the CXCXCXC tetracysteine motif. Here, we investigate the general applicability of this peptide as a dimerization motif for different proteins. By recombinant DNA technology, the peptide CHWECRGCRLVC was loaded with proteins, and functional homodimers were obtained upon oxidative folding. Attached to the N-terminus of the dodecapeptide, the prokaryotic enzyme limonene epoxide hydrolase (LEH) completely forms a covalent antiparallel dimer. In a diatom expression system, the monoclonal antibody CL4 mAb is released in its functional form when its natural CPPC central parallel hinge is exchanged for the designed tetra-Cys hinge motif. To improve our understanding of the regioselectivity of tetra-disulfide formation, we provoked the formation of heterodimeric hinge peptides by mixing two different tetra-Cys peptides and characterizing the heterodimer by mass spectrometry and nuclear magnetic resonance spectroscopy.

摘要

二聚体二硫键连接的肽是由含有CXCXCXC四半胱氨酸基序的硫醇前体的区域选择性氧化折叠形成的。在此,我们研究了这种肽作为不同蛋白质二聚化基序的普遍适用性。通过重组DNA技术,将肽CHWECRGCRLVC与蛋白质负载在一起,氧化折叠后获得了功能性同二聚体。连接到十二肽的N端,原核酶柠檬烯环氧水解酶(LEH)完全形成共价反平行二聚体。在硅藻表达系统中,当单克隆抗体CL4 mAb的天然CPPC中央平行铰链被设计的四半胱氨酸铰链基序替换时,它以功能形式释放。为了更好地理解四硫键形成的区域选择性,我们通过混合两种不同的四半胱氨酸肽并通过质谱和核磁共振光谱对异二聚体进行表征,从而引发异二聚体铰链肽的形成。

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