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赖氨酰肽酶通道对血管紧张素 II 的随机感应。

Stochastic sensing of Angiotensin II with lysenin channels.

机构信息

Department of Physics, Boise State University, Boise, ID, 83725, USA.

Biomolecular Sciences Graduate Program, Boise State University, Boise, ID, 83725, USA.

出版信息

Sci Rep. 2017 May 26;7(1):2448. doi: 10.1038/s41598-017-02438-0.

Abstract

The ability of pore-forming proteins to interact with various analytes has found vast applicability in single molecule sensing and characterization. In spite of their abundance in organisms from all kingdoms of life, only a few pore-forming proteins have been successfully reconstituted in artificial membrane systems for sensing purposes. Lysenin, a pore-forming toxin extracted from the earthworm E. fetida, inserts large conductance nanopores in lipid membranes containing sphingomyelin. Here we show that single lysenin channels may function as stochastic nanosensors by allowing the short cationic peptide angiotensin II to be electrophoretically driven through the conducting pathway. Long-term translocation experiments performed using large populations of lysenin channels allowed unequivocal identification of the unmodified analyte by Liquid Chromatography-Mass Spectrometry. However, application of reverse voltages or irreversible blockage of the macroscopic conductance of lysenin channels by chitosan addition prevented analyte translocation. This investigation demonstrates that lysenin channels have the potential to function as nano-sensing devices capable of single peptide molecule identification and characterization, which may be further extended to other macromolecular analytes.

摘要

孔形成蛋白与各种分析物相互作用的能力在单分子传感和特性描述中具有广泛的适用性。尽管它们在所有生命领域的生物体中都很丰富,但只有少数孔形成蛋白被成功地在用于传感的人工膜系统中重建。lysenin 是一种从蚯蚓 E. fetida 中提取的形成孔的毒素,它在含有神经鞘磷脂的脂质膜中插入大电导纳米孔。在这里,我们表明,单个 lysenin 通道可以通过允许短阳离子肽血管紧张素 II 通过导电途径电泳驱动来充当随机纳米传感器。使用大量 lysenin 通道进行的长期易位实验通过液相色谱-质谱法明确鉴定了未修饰的分析物。然而,施加反向电压或通过添加壳聚糖不可逆地阻断 lysenin 通道的宏观电导率会阻止分析物易位。这项研究表明,lysenin 通道有可能作为纳米传感装置,能够识别和描述单个肽分子,这可能进一步扩展到其他大分子分析物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f445/5446423/d3499a8a04a4/41598_2017_2438_Fig1_HTML.jpg

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