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细胞内细菌的超分子识别与诊断指导治疗

Supramolecular discrimination and diagnosis-guided treatment of intracellular bacteria.

作者信息

Tian Jia-Hong, Huang Siyuan, Wang Ze-Han, Li Juan-Juan, Song Xianhui, Jiang Ze-Tao, Shi Bing-Sen, Zhao Ying-Ying, Zhang Hui-Yan, Wang Ke-Rang, Hu Xin-Yue, Zhang Xinge, Guo Dong-Sheng

机构信息

College of Chemistry, Nankai University, Tianjin, China.

State Key Laboratory of Elemento-Organic Chemistry, Nankai University, Tianjin, China.

出版信息

Nat Commun. 2025 Jan 25;16(1):1016. doi: 10.1038/s41467-025-56308-9.

Abstract

Pathogenic intracellular bacteria pose a significant threat to global public health due to the barriers presented by host cells hindering the timely detection of hidden bacteria and the effective delivery of therapeutic agents. To address these challenges, we propose a tandem diagnosis-guided treatment paradigm. A supramolecular sensor array is developed for simple, rapid, accurate, and high-throughput identification of intracellular bacteria. This diagnostic approach executes the significant guiding missions of screening a customized host-guest drug delivery system by disclosing the rationale behind the discrimination. We design eight azocalix[4]arenes with differential active targeting, cellular internalization, and hypoxia responsiveness to penetrate cells and interact with bacteria. Loaded with fluorescent indicators, these azocalix[4]arenes form a sensor array capable of discriminating eight intracellular bacterial species without cell lysis or separation. By fingerprinting specimens collected from bacteria-infected mice, the facilitated accurate diagnosis offers valuable guidance for selecting appropriate antibiotics. Moreover, mannose-modified azocalix[4]arene (ManAC4A) is screened as a drug carrier efficiently taken up by macrophages. Doxycycline loaded with ManAC4A exhibits improved efficacy against methicillin-resistant Staphylococcus aureus-infected peritonitis. This study introduces an emerging paradigm to intracellular bacterial diagnosis and treatment, offering broad potential in combating bacterial infectious diseases.

摘要

致病性细胞内细菌对全球公共卫生构成重大威胁,因为宿主细胞形成的屏障阻碍了对隐藏细菌的及时检测以及治疗药物的有效递送。为应对这些挑战,我们提出了一种串联诊断引导治疗模式。开发了一种超分子传感器阵列,用于简单、快速、准确和高通量地鉴定细胞内细菌。这种诊断方法通过揭示鉴别背后的原理,执行筛选定制的主客体药物递送系统的重要指导任务。我们设计了八种具有不同主动靶向、细胞内化和缺氧反应性的偶氮杯[4]芳烃,以穿透细胞并与细菌相互作用。这些偶氮杯[4]芳烃负载荧光指示剂后,形成一个能够在不进行细胞裂解或分离的情况下鉴别八种细胞内细菌种类的传感器阵列。通过对从感染细菌的小鼠身上采集的样本进行指纹识别,这种便捷的准确诊断为选择合适的抗生素提供了有价值的指导。此外,筛选出甘露糖修饰的偶氮杯[4]芳烃(ManAC4A)作为一种能被巨噬细胞有效摄取的药物载体。负载多西环素的ManAC4A对耐甲氧西林金黄色葡萄球菌感染的腹膜炎表现出更高的疗效。本研究为细胞内细菌的诊断和治疗引入了一种新兴模式,在对抗细菌感染性疾病方面具有广阔的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5037/11762306/c8fe9b0f9922/41467_2025_56308_Fig1_HTML.jpg

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