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通过碰撞诱导亲合选择质谱法推进 Kir4.2 通道配体鉴定。

Advancing Kir4.2 Channel Ligand Identification through Collision-Induced Affinity Selection Mass Spectrometry.

机构信息

Griffith Institute for Drug Discovery, Griffith University, Brisbane, Queensland 4111, Australia.

School of Environment and Science, Griffith University, Brisbane, Queensland 4111, Australia.

出版信息

ACS Chem Biol. 2024 Mar 15;19(3):763-773. doi: 10.1021/acschembio.3c00781. Epub 2024 Mar 7.

Abstract

The inwardly rectifying potassium Kir4.2 channel plays a crucial role in regulating membrane potentials and maintaining potassium homeostasis. Kir4.2 has been implicated in various physiological processes, including insulin secretion, gastric acid regulation, and the pathogenesis of central nervous system diseases. Despite its significance, the number of identified ligands for Kir4.2 remains limited. In this study, we established a method to directly observe ligands avoiding a requirement to observe the high-mass ligand-membrane protein-detergent complexes. This method used collision-induced affinity selection mass spectrometry (CIAS-MS) to identify ligands dissociated from the Kir4.2 channel-detergent complex. The CIAS-MS approach integrated all stages of affinity selection within the mass spectrometer, offering advantages in terms of time efficiency and cost-effectiveness. Additionally, we explored the effect of collisional voltage ramps on the dissociation behavior of the ligand and the ligand at different concentrations, demonstrating dose dependency.

摘要

内向整流钾通道 Kir4.2 在调节膜电位和维持钾离子稳态方面发挥着关键作用。Kir4.2 参与了多种生理过程,包括胰岛素分泌、胃酸调节以及中枢神经系统疾病的发病机制。尽管其意义重大,但已鉴定的 Kir4.2 配体数量仍然有限。在本研究中,我们建立了一种直接观察配体的方法,避免了观察大质量配体-膜蛋白-去污剂复合物的需要。该方法使用碰撞诱导亲和选择质谱(CIAS-MS)来鉴定从 Kir4.2 通道-去污剂复合物中解离的配体。CIAS-MS 方法将亲和选择的所有阶段集成在质谱仪内,在时间效率和成本效益方面具有优势。此外,我们还探讨了碰撞电压斜坡对配体和不同浓度下配体解离行为的影响,证明了剂量依赖性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9316/10949200/340d122b723c/cb3c00781_0001.jpg

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