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In vivo multiplex molecular imaging of vascular inflammation using surface-enhanced Raman spectroscopy

机译:使用表面增强拉曼光谱对血管炎症进行体内多重分子成像

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Vascular immune-inflammatory responses play a crucial role in the progression and outcome of atherosclerosis. The ability to assess localized inflammation through detection of specific vascular inflammatory biomarkers would significantly improve cardiovascular risk assessment and management; however, no multi-parameter molecular imaging technologies have been established to date. Here, we report the targeted in vivo imaging of multiple vascular biomarkers using antibody-functionalized nanoparticles and surface-enhanced Raman scattering (SERS). Methods: A series of antibody-functionalized gold nanoprobes (BFNP) were designed containing unique Raman signals in order to detect intercellular adhesion molecule 1 (ICAM-1), vascular cell adhesion molecule 1 (VCAM-1) and P-selectin using SERS. Results: SERS and BFNP were utilized to detect, discriminate and quantify ICAM-1, VCAM-1 and P-selectin in vitro on human endothelial cells and ex vivo in human coronary arteries. Ultimately, non-invasive multiplex imaging of adhesion molecules in a humanized mouse model was demonstrated in vivo following intravenous injection of the nanoprobes. Conclusion: This study demonstrates that multiplexed SERS-based molecular imaging can indicate the status of vascular inflammation in vivo and gives promise for SERS as a clinical imaging technique for cardiovascular disease in the future.
机译:血管免疫炎症反应在动脉粥样硬化的进展和结果中起关键作用。通过检测特定的血管炎性生物标志物评估局部炎症的能力将显着改善心血管风险的评估和管理;但是,迄今为止尚未建立多参数分子成像技术。在这里,我们报告使用抗体功能化的纳米粒子和表面增强拉曼散射(SERS)的多个血管生物标记物的靶向体内成像。方法:设计了一系列包含独特拉曼信号的抗体功能化金纳米探针(BFNP),以便使用SERS检测细胞间粘附分子1(ICAM-1),血管细胞粘附分子1(VCAM-1)和P-选择素。结果:SERS和BFNP用于体外,人内皮细胞和离体人冠状动脉中的ICAM-1,VCAM-1和P-选择素的检测,区分和定量。最终,在静脉注射纳米探针后,在体内证明了人源化小鼠模型中粘附分子的非侵入性多重成像。结论:这项研究表明,基于SERS的多重分子成像可指示体内血管炎症的状态,并有望将SERS用作未来心血管疾病的临床成像技术。

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