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三种突变使一种蛋白质传感器对烟碱激动剂的选择性转化为 S-美沙酮,可用于细胞、细胞器和生物流体。

Three Mutations Convert the Selectivity of a Protein Sensor from Nicotinic Agonists to S-Methadone for Use in Cells, Organelles, and Biofluids.

机构信息

Division of Biology and Biological Engineering, California Institute of Technology, Pasadena, California 91106, United States.

Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, California 91106, United States.

出版信息

J Am Chem Soc. 2022 May 18;144(19):8480-8486. doi: 10.1021/jacs.2c02323. Epub 2022 Apr 21.

Abstract

We report a reagentless, intensity-based S-methadone fluorescent sensor, iS-methadoneSnFR, consisting of a circularly permuted GFP inserted within the sequence of a mutated bacterial periplasmic binding protein (PBP). We evolved a previously reported nicotine-binding PBP to become a selective S-methadone-binding sensor, via three mutations in the PBP's second shell and hinge regions. iS-methadoneSnFR displays the necessary sensitivity, kinetics, and selectivity─notably enantioselectivity against R-methadone─for biological applications. Robust iS-methadoneSnFR responses in human sweat and saliva and mouse serum enable diagnostic uses. Expression and imaging in mammalian cells demonstrate that S-methadone enters at least two organelles and undergoes acid trapping in the Golgi apparatus, where opioid receptors can signal. This work shows a straightforward strategy in adapting existing PBPs to serve real-time applications ranging from subcellular to personal pharmacokinetics.

摘要

我们报告了一种无试剂、基于强度的 S-美沙酮荧光传感器 iS-methadoneSnFR,它由一个环状排列的 GFP 插入到突变的细菌周质结合蛋白(PBP)序列中。我们通过在 PBP 的第二壳层和铰链区域的三个突变,将先前报道的尼古丁结合 PBP 进化为一种选择性的 S-美沙酮结合传感器。iS-methadoneSnFR 具有用于生物应用所需的灵敏度、动力学和选择性——特别是对 R-美沙酮的对映选择性。在人汗、唾液和鼠血清中的稳健 iS-methadoneSnFR 响应使其能够用于诊断。在哺乳动物细胞中的表达和成像表明 S-美沙酮进入至少两个细胞器,并在高尔基体内经历酸捕获,阿片受体可以在那里发出信号。这项工作展示了一种直接的策略,即将现有的 PBP 适应实时应用,从亚细胞到个人药代动力学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/95d3/9121368/c74337df6d82/ja2c02323_0001.jpg

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