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一种通过多光谱光声断层扫描和近红外二区荧光成象技术用于诊断间质性膀胱炎和肝脏缺血再灌注损伤的 HO 激活型纳米探针。

A HO-activatable nanoprobe for diagnosing interstitial cystitis and liver ischemia-reperfusion injury via multispectral optoacoustic tomography and NIR-II fluorescent imaging.

机构信息

Biomedical Division, State Key Laboratory of Luminescent Materials and Devices, Guangdong Provincial Key Laboratory of Luminescence from Molecular Aggregates, College of Materials Science and Engineering, South China University of Technology, Wushan Road 381, Guangzhou, 510640, China.

Division of Chemistry and Biological Chemistry, School of Physical and Mathematical Sciences, Nanyang Technological University, 21 Nanyang Link, Singapore, 637371, Singapore.

出版信息

Nat Commun. 2021 Nov 25;12(1):6870. doi: 10.1038/s41467-021-27233-4.

Abstract

Developing high-quality NIR-II fluorophores (emission in 1000-1700 nm) for in vivo imaging is of great significance. Benzothiadiazole-core fluorophores are an important class of NIR-II dyes, yet ongoing limitations such as aggregation-caused quenching in aqueous milieu and non-activatable response are still major obstacles for their biological applications. Here, we devise an activatable nanoprobe to address these limitations. A molecular probe named BTPE-NO is synthesized by linking a benzothiadiazole core with two tetraphenylene groups serving as hydrophobic molecular rotors, followed by incorporating two nitrophenyloxoacetamide units at both ends of the core as recognition moieties and fluorescence quenchers. An FDA-approved amphiphilic polymer Pluronic F127 is then employed to encapsulate the molecular BTPE-NO to render the nanoprobe BTPE-NO@F127. The pathological levels of HO in the disease sites cleave the nitrophenyloxoacetamide groups and activate the probe, thereby generating strong fluorescent emission (950~1200 nm) and ultrasound signal for multi-mode imaging of inflammatory diseases. The nanoprobe can therefore function as a robust tool for detecting and imaging the disease sites with NIR-II fluorescent and multispectral optoacoustic tomography (MSOT) imaging. Moreover, the three-dimensional MSOT images can be obtained for visualizing and locating the disease foci.

摘要

开发高质量的近红外二区荧光团(发射波长在 1000-1700nm)对于活体成像是非常重要的。苯并噻二唑核心荧光团是近红外二区染料的一个重要类别,但目前仍存在一些限制,如在水介质中聚集引起的猝灭以及非激活响应,这些仍然是其生物应用的主要障碍。在这里,我们设计了一种可激活的纳米探针来解决这些限制。通过将苯并噻二唑核心与两个作为疏水分子转子的四苯乙烯基团连接,合成了一种名为 BTPE-NO 的分子探针,然后在核心的两端分别引入两个硝基苯氧乙酰胺单元作为识别部分和荧光猝灭剂。然后,采用 FDA 批准的两亲性聚合物 Pluronic F127 来包裹分子 BTPE-NO,得到纳米探针 BTPE-NO@F127。疾病部位的病理水平的 HO 会切割硝基苯氧乙酰胺基团并激活探针,从而产生强荧光发射(950-1200nm)和超声信号,用于炎症性疾病的多模式成像。因此,该纳米探针可以作为一种强大的工具,用于检测和成像近红外二区荧光和多光谱光声断层扫描(MSOT)成像的疾病部位。此外,还可以获得三维 MSOT 图像,用于可视化和定位疾病焦点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f77/8617030/dbf4af5fa4a5/41467_2021_27233_Fig4_HTML.jpg

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