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单分子分辨率下血液中多种抗生素庆大霉素的直接和连续监测。

Direct and Continuous Monitoring of Multicomponent Antibiotic Gentamicin in Blood at Single-Molecule Resolution.

机构信息

Department of Laboratory Medicine, State Key Laboratory of Biotherapy and Clinical Laboratory Medicine Research Center, West China Hospital, Sichuan University, Chengdu, 610041, China.

Tianfu Jincheng Laboratory, City of Future Medicine, Chengdu 610500, China.

出版信息

ACS Nano. 2024 Mar 26;18(12):9137-9149. doi: 10.1021/acsnano.4c00302. Epub 2024 Mar 12.

DOI:10.1021/acsnano.4c00302
PMID:38470845
Abstract

Point-of-care monitoring of small molecules in biofluids is crucial for clinical diagnosis and treatment. However, the inherent low degree of recognition of small molecules and the complex composition of biofluids present significant obstacles for current detection technologies. Although nanopore sensing excels in the analysis of small molecules, the direct detection of small molecules in complex biofluids remains a challenge. In this study, we present a method for sensing the small molecule drug gentamicin in whole blood based on the mechanosensitive channel of small conductance in (MscS) nanopore. MscS can directly detect gentamicin and distinguish its main components with only a monomethyl difference. The 'molecular sieve' structure of MscS enables the direct measurement of gentamicin in human whole blood within 10 min. Furthermore, a continuous monitoring device constructed based on MscS achieved continuous monitoring of gentamicin in live rats for approximately 2.5 h without blood consumption, while the drug components can be analyzed in situ. This approach enables rapid and convenient drug monitoring with single-molecule level resolution, which can significantly lower the threshold for drug concentration monitoring and promote more efficient drug use. Moreover, this work also lays the foundation for the future development of continuous monitoring technology with single-molecule level resolution in the living body.

摘要

生物流体中小分子的即时检测对于临床诊断和治疗至关重要。然而,小分子固有的低度识别和生物流体复杂的组成对当前的检测技术构成了重大障碍。尽管纳米孔传感在小分子分析方面表现出色,但对复杂生物流体中小分子的直接检测仍然是一个挑战。在本研究中,我们提出了一种基于小电导机械敏感通道 (MscS) 纳米孔检测全血中小分子药物庆大霉素的方法。MscS 可以直接检测庆大霉素,并仅通过一个单甲基差异来区分其主要成分。MscS 的“分子筛”结构使我们能够在 10 分钟内直接测量人全血中的庆大霉素。此外,基于 MscS 构建的连续监测装置实现了对活鼠体内庆大霉素的连续监测,无需采血,同时可以原位分析药物成分。这种方法能够以单分子水平分辨率实现快速便捷的药物监测,显著降低药物浓度监测的门槛,促进更有效的药物使用。此外,这项工作还为未来在活体中开发具有单分子水平分辨率的连续监测技术奠定了基础。

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