期刊
NANOSCALE
卷 13, 期 13, 页码 6461-6474出版社
ROYAL SOC CHEMISTRY
DOI: 10.1039/d0nr08039j
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资金
- Key Research and Development Program of Zhejiang Province [2017C03042]
- National Natural Science Foundation of China [32025021, 51873225]
- Public Welfare Technology Application Research Project of Zhejiang Province [2017C35003]
- Major Medical and Health Program of Zhejiang Province [WKJ-ZJ-1807]
- Natural Science Foundation of Zhejiang Province [LY18H180011, LQ19H180002, LQ19H180004, LQ20H180002]
- Key Laboratory of Diagnosis and Treatment of Digestive System Tumors of Zhejiang Province [2019E10020]
- Ningbo Clinical Research Center for Digestive System Tumors [2019A21003]
- Key Scientific and Technological Special Project of Ningbo City [2015C50004, 2017C110022]
- Ningbo Natural Science Foundation for Young Scholar [2019A610202]
- HwaMei Research Foundation of Ningbo No.2 Hospital [2018HMKY40]
The study proposes a macrophage-targeted and in situ stimuli-triggered T-1-T-2 switchable magnetic resonance imaging (MRI) nanoprobe for non-invasive diagnosis of vulnerable plaques, which can help identify vulnerable plaques at early stages. By modifying and transforming iron oxide nanoparticles, the nanoprobe achieves a substantial non-invasive diagnosis of vulnerable plaques, contributing significantly to the application of materials science in solving clinical problems.
Unlike stable atherosclerotic plaques, vulnerable plaques are very likely to cause serious cardio-cerebrovascular diseases. Meanwhile, how to non-invasively identify vulnerable plaques at early stages has been an urgent but challenging problem in clinical practices. Here, we propose a macrophage-targeted and in situ stimuli-triggered T-1-T-2 switchable magnetic resonance imaging (MRI) nanoprobe for the non-invasive diagnosis of vulnerable plaques. Precisely, single-dispersed iron oxide nanoparticles (IONPs) modified with hyaluronic acid (HA), denoted as IONP-HP, show macrophage targetability and T-1 MRI enhancement (r(2)/r(1) = 3.415). Triggered by the low pH environment of macrophage lysosomes, the single-dispersed IONP-HP transforms into a cluster analogue, which exhibits T-2 MRI enhancement (r(2)/r(1) = 13.326). Furthermore, an in vivo switch of T-1-T-2 enhancement modes shows that the vulnerable plaques exhibit strong T-1 enhancement after intravenous administration of the nanoprobe, followed by a switch to T-2 enhancement after 9 h. In contrast, stable plaques show only slight T-1 enhancement but without T-2 enhancement. It is therefore imperative that the intelligent and novel nanoplatform proposed in this study achieves a substantial non-invasive diagnosis of vulnerable plaques by means of a facile but effective T-1-T-2 switchable process, which will significantly contribute to the application of materials science in solving clinical problems.
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