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基于 HALO 标签技术的新型 MAS 相关 G 蛋白偶联受体 X2 细胞膜色谱分析模型及其应用。

A new MAS-related G protein-coupled receptor X2 cell membrane chromatography analysis model based on HALO-tag technology and its applications.

机构信息

School of Pharmacy, Xi'an Jiaotong University, 76# Yanta West Road, Xi'an, 710061, China; Institute of Pharmaceutical Science and Technology, Western China Science &Technology Innovation Harbour, Xi'an, 710115, China.

School of Pharmacy, Xi'an Jiaotong University, 76# Yanta West Road, Xi'an, 710061, China; Institute of Pharmaceutical Science and Technology, Western China Science &Technology Innovation Harbour, Xi'an, 710115, China.

出版信息

Talanta. 2024 Feb 1;268(Pt 1):125317. doi: 10.1016/j.talanta.2023.125317. Epub 2023 Oct 18.

Abstract

Cell membrane chromatography (CMC) is an effective method for studying receptors with multiple transmembrane structure such as MAS-related G protein-coupled receptor X2 (MrgX2). CMC relies on the maintenance of the complete biological structure of a membrane receptor; however, it needs to be further improved to obtain a more convenient and stable CMC model. In the present study, the haloalkane dehalogenase protein tag (HALO-tag) technology was used to construct a new MrgX2/CMC model. The fusion receptors of MrgX2 with HALO-tag at the C terminus were expressed in HEK293 cells. The silica gel was modified with a substrate of HALO-tag (chloroalkanes) via one-step acylation for the rapid capture of fusion receptors. The new CMC model (MrgX2-HALO-tag/CMC model) was not only quicker to prepare but also more stable and had a longer lifespan than a previous MrgX2-SNAP-tag/CMC model. In combination with the high-performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS) system, the MrgX2-HALO-tag/CMC model was used to screen and identify bioactive components in traditional Chinese medicine. Using this combination, sanggenon C and morusin were identified from Mori Cortex as anti-pseudo-allergic components. The MrgX2-HALO-tag/CMC model alone was also applied to analyze ligand-receptor interaction. The affinity order of four ligands to MrgX2 was as follows: desipramine < imipramine < amitriptyline < clomipramine. This was consistent with the results obtained using the MrgX2-SNAP-tag/CMC model. The MrgX2-HALO-tag/CMC model provides ideas and application prospects for the immobilization of cell membrane that contains receptors with more transmembrane structures.

摘要

细胞膜色谱法(CMC)是一种有效的方法,用于研究具有多个跨膜结构的受体,如 MAS 相关 G 蛋白偶联受体 X2(MrgX2)。CMC 依赖于膜受体完整生物结构的维持;然而,它需要进一步改进,以获得更方便和稳定的 CMC 模型。在本研究中,使用卤代烷烃脱卤酶蛋白标签(HALO-tag)技术构建了一种新的 MrgX2/CMC 模型。MrgX2 与 HALO-tag 在 C 末端融合受体在 HEK293 细胞中表达。硅胶通过一步酰化用 HALO-tag 的底物(卤代烷烃)修饰,用于快速捕获融合受体。新的 CMC 模型(MrgX2-HALO-tag/CMC 模型)不仅制备更快,而且更稳定,寿命也比以前的 MrgX2-SNAP-tag/CMC 模型更长。结合高效液相色谱-串联质谱(HPLC-MS/MS)系统,MrgX2-HALO-tag/CMC 模型用于筛选和鉴定中药中的生物活性成分。使用这种组合,从桑白皮中鉴定出桑根酮 C 和桑皮苷作为抗伪过敏成分。MrgX2-HALO-tag/CMC 模型也单独应用于分析配体-受体相互作用。四种配体与 MrgX2 的亲和力顺序如下:去甲丙咪嗪 < 丙咪嗪 < 阿米替林 < 氯米帕明。这与使用 MrgX2-SNAP-tag/CMC 模型得到的结果一致。MrgX2-HALO-tag/CMC 模型为含有更多跨膜结构受体的细胞膜固定化提供了思路和应用前景。

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