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活细胞中维生素K循环酶的功能研究

Functional Study of the Vitamin K Cycle Enzymes in Live Cells.

作者信息

Tie J-K, Stafford D W

机构信息

University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.

University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.

出版信息

Methods Enzymol. 2017;584:349-394. doi: 10.1016/bs.mie.2016.10.015. Epub 2016 Nov 22.

Abstract

Vitamin K-dependent carboxylation, an essential posttranslational modification catalyzed by gamma-glutamyl carboxylase, is required for the biological functions of proteins that control blood coagulation, vascular calcification, bone metabolism, and other important physiological processes. Concomitant with carboxylation, reduced vitamin K (KH) is oxidized to vitamin K epoxide (KO). KO must be recycled back to KH by the enzymes vitamin K epoxide reductase and vitamin K reductase in a pathway known as the vitamin K cycle. Our current knowledge about the enzymes of the vitamin K cycle is mainly based on in vitro studies of each individual enzymes under artificial conditions, which are of limited usefulness in understanding how the complex carboxylation process is carried out in the physiological environment. In this chapter, we review the current in vitro activity assays for vitamin K cycle enzymes. We describe the rationale, establishment, and application of cell-based assays for the functional study of these enzymes in the native cellular milieu. In these cell-based assays, different vitamin K-dependent proteins were designed and stably expressed in mammalian cells as reporter proteins to accommodate the readily used enzyme-linked immunosorbent assay for carboxylation efficiency evaluation. Additionally, recently emerged genome-editing techniques TALENs and CRISPR-Cas9 were used to knock out the endogenous enzymes in the reporter cell lines to eliminate the background. These cell-based assays are easy to scale up for high-throughput screening of inhibitors of vitamin K cycle enzymes and have been successfully used to clarify the genotypes and their clinical phenotypes of enzymes of the vitamin K cycle.

摘要

维生素K依赖的羧化作用是由γ-谷氨酰羧化酶催化的一种必需的翻译后修饰,对于控制血液凝固、血管钙化、骨代谢及其他重要生理过程的蛋白质的生物学功能而言必不可少。在羧化作用的同时,还原型维生素K(KH)被氧化为维生素K环氧化物(KO)。KO必须通过维生素K环氧化物还原酶和维生素K还原酶在一条被称为维生素K循环的途径中循环变回KH。我们目前关于维生素K循环中各酶的知识主要基于在人工条件下对每种酶的体外研究,这对于理解在生理环境中复杂的羧化过程如何进行的作用有限。在本章中,我们综述了目前用于维生素K循环酶的体外活性测定方法。我们描述了基于细胞的测定方法的原理、建立及应用,用于在天然细胞环境中对这些酶进行功能研究。在这些基于细胞的测定方法中,设计了不同的维生素K依赖蛋白并在哺乳动物细胞中稳定表达作为报告蛋白,以适应易于使用的酶联免疫吸附测定来评估羧化效率。此外,最近出现的基因组编辑技术转录激活样效应因子核酸酶(TALENs)和规律成簇间隔短回文重复序列-Cas9(CRISPR-Cas9)被用于敲除报告细胞系中的内源性酶以消除背景。这些基于细胞的测定方法易于扩大规模以进行维生素K循环酶抑制剂的高通量筛选,并已成功用于阐明维生素K循环中各酶的基因型及其临床表型。

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