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一种可点击的氧化甾醇光标记物保留NMDA受体活性并在神经元中积累。

A Clickable Oxysterol Photolabel Retains NMDA Receptor Activity and Accumulates in Neurons.

作者信息

Chen Daniel M, Ziolkowski Luke, Benz Ann, Qian Mingxing, Zorumski Charles F, Covey Douglas F, Mennerick Steven

机构信息

Department of Psychiatry, Washington University, St. Louis, MO, United States.

Taylor Family Institute for Innovative Psychiatric Research, St. Louis, MO, United States.

出版信息

Front Neurosci. 2018 Dec 6;12:923. doi: 10.3389/fnins.2018.00923. eCollection 2018.

Abstract

Oxysterol analogs that modulate NMDA receptor function are candidates for therapeutic development to treat neuropsychiatric disorders. However, the cellular actions of these compounds are still unclear. For instance, how these compounds are compartmentalized or trafficked in neurons is unknown. In this study, we utilized a chemical biology approach combining photolabeling and click chemistry. We introduce a biologically active oxysterol analog that contains: (1) a diazirine group, allowing for the permanent labeling of cellular targets, and (2) an alkyne group, allowing for subsequent visualization using Cu catalyzed cycloaddition of an azide-conjugated fluorophore. The physiological properties of this analog at NMDA receptors resemble those of other oxysterols, including occlusion with other oxysterol-like compounds. Fluorescent imaging reveals that the analog accumulates diffusely in the cytoplasm of neurons through an energy-independent mechanism. Overall, this work introduces a novel chemical biology approach to investigate oxysterol actions and introduces a tool useful for further cell biological and biochemical studies of oxysterols.

摘要

调节NMDA受体功能的氧化甾醇类似物是治疗神经精神疾病的候选药物。然而,这些化合物的细胞作用仍不清楚。例如,这些化合物在神经元中如何进行区室化或运输尚不清楚。在本研究中,我们采用了一种结合光标记和点击化学的化学生物学方法。我们引入了一种具有生物活性的氧化甾醇类似物,它包含:(1)一个重氮丙啶基团,可对细胞靶点进行永久性标记;(2)一个炔基,可通过铜催化的叠氮共轭荧光团环加成反应进行后续可视化。该类似物在NMDA受体上的生理特性与其他氧化甾醇相似,包括与其他氧化甾醇样化合物的阻断作用。荧光成像显示,该类似物通过一种能量非依赖机制在神经元细胞质中弥漫性积累。总的来说,这项工作引入了一种新的化学生物学方法来研究氧化甾醇的作用,并引入了一种有助于进一步进行氧化甾醇细胞生物学和生物化学研究的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c58a/6291516/db064fa4f7c4/fnins-12-00923-g001.jpg

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