无细胞合成膜受体制备NKG2A整体微亲和层析

IF 4 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS Journal of Chromatography A Pub Date : 2025-04-12 Epub Date: 2025-02-13 DOI:10.1016/j.chroma.2025.465775
Chun Chen , Xinyi Chai , Yanqiu Gu , Chengliang Wang , Yongfang Yuan , Yifeng Chai , Zhengjin Jiang , Xiaofei Chen
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引用次数: 0

摘要

膜受体亲和层析是筛选靶向膜受体的化合物并确定其结合亲和力的一种实用策略。这些方法的关键是为特定受体在色谱固定相上的固定创造一个仿生细胞膜环境。然而,它的大规模应用受到包括细胞培养、重组蛋白表达和柱包装等劳动密集型和耗时的程序的限制。此外,传统的亲和色谱柱容易存在固定相组成不均匀和渗透率低的缺点。本研究建立了一种基于无细胞蛋白合成(CFPS)和双(磺基琥珀酰亚基)亚基修饰整体固定相的膜受体生物亲和层析新方法,用于批量快速制备整体微亲和柱,实现了免疫检查点自然杀手2族受体a (NKG2A)定向可控的高效合成和固定化。将制备的NKG2A微亲和柱与离线- 2d - ulc - qtof /MS系统耦合,筛选到两种新的NKG2A抑制剂黄芩苷和乌根草苷,KD值分别为30.23 μM和13.01 μM,可显著上调NK细胞颗粒酶B、肿瘤坏死因子-α和干扰素-γ的基因表达和CD107a蛋白表达。此外,这两种化合物还能增强NK细胞对肿瘤细胞的细胞毒活性。本文提出的基于cfps的整体微亲和层析技术实现了跨膜受体在一天内快速合成和固定化,实现了均匀性、良好的通透性和取向控制的高表达。该方法可扩展到任何感兴趣的跨膜受体,用于快速筛选药物和亲和力测定。
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Cell-free synthesis of membrane receptors for preparation of NKG2A monolithic micro-affinity chromatography
Membrane receptor affinity chromatography is a practical strategy for screening compounds targeting membrane receptors and determining their binding affinity. The key of these methods is to create a biomimetic cell membrane environment for the immobilization of specific receptors on chromatographic stationary phase. However, its large-scale applications are limited by the labor-intensive and time-consuming procedures including cell culture, recombinant protein expression and column packing. Furthermore, traditional affinity chromatography columns are prone to drawbacks such as heterogeneous composition of the stationary phase and low permeability. In this study, a novel membrane receptor biological affinity chromatographic method based on cell-free protein synthesis (CFPS) and Bis(sulfosuccinimidyl)suberate modified monolithic stationary phase was developed for fast preparation of monolithic micro-affinity column in batches, which realized efficient synthesis and immobilization of immune checkpoint natural killer group 2 family of receptor A (NKG2A) with controlled orientation. Coupling the prepared NKG2A micro-affinity column with an offline-2D-UPLC-QTOF/MS system, two new NKG2A inhibitors, baicalin and wogonoside, were screened out with the KD values of 30.23 and 13.01 μM respectively, significantly upregulating the gene expression of granzyme B, tumor necrosis factor-α and interferon-γ and the protein expression of CD107a in natural killer (NK) cells. Moreover, the cytotoxic activity of NK cells against tumor cells was enhanced by these two compounds. The proposed CFPS-based monolithic micro-affinity chromatography realizes rapid synthesis and immobilization of transmembrane receptors within one day, achieving homogeneity, good permeability and orientation-controlled high expression. This approach could be extended to any interested transmembrane receptors for rapid drug screening and affinity determination.
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来源期刊
Journal of Chromatography A
Journal of Chromatography A 化学-分析化学
CiteScore
7.90
自引率
14.60%
发文量
742
审稿时长
45 days
期刊介绍: The Journal of Chromatography A provides a forum for the publication of original research and critical reviews on all aspects of fundamental and applied separation science. The scope of the journal includes chromatography and related techniques, electromigration techniques (e.g. electrophoresis, electrochromatography), hyphenated and other multi-dimensional techniques, sample preparation, and detection methods such as mass spectrometry. Contributions consist mainly of research papers dealing with the theory of separation methods, instrumental developments and analytical and preparative applications of general interest.
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