A Comparative Study of Ultrasmall Calcium Carbonate Nanoparticles for Targeting and Imaging Atherosclerotic Plaque

磁共振成像 离体 体内 材料科学 临床前影像学 医学影像学 医学 纳米技术 生物医学工程 放射科 生物 生物技术
作者
Lydia Martínez-Parra,Marina Piñol-Cancer,Carlos Sanchez‐Cano,A.B. Miguel-Coello,Desirè Di Silvio,Ana M. Gómez,Clara Uriel,Sandra Plaza-García,Marta Gallego,Raquel Pazos,Hugo Groult,Marc Jeannin,Kalotina Geraki,Laura Fernández‐Méndez,Ainhize Urkola-Arsuaga,María Jesús Sánchez-Guisado,Juliana Carrillo-Romero,Wolfgang J. Parak,Maurizio Prato,Fernando Herranz,Jesús Ruíz‐Cabello,Susana Carregal‐Romero
出处
期刊:ACS Nano [American Chemical Society]
卷期号:17 (14): 13811-13825 被引量:5
标识
DOI:10.1021/acsnano.3c03523
摘要

Atherosclerosis is a complex disease that can lead to life-threatening events, such as myocardial infarction and ischemic stroke. Despite the severity of this disease, diagnosing plaque vulnerability remains challenging due to the lack of effective diagnostic tools. Conventional diagnostic protocols lack specificity and fail to predict the type of atherosclerotic lesion and the risk of plaque rupture. To address this issue, technologies are emerging, such as noninvasive medical imaging of atherosclerotic plaque with customized nanotechnological solutions. Modulating the biological interactions and contrast of nanoparticles in various imaging techniques, including magnetic resonance imaging, is possible through the careful design of their physicochemical properties. However, few examples of comparative studies between nanoparticles targeting different hallmarks of atherosclerosis exist to provide information about the plaque development stage. Our work demonstrates that Gd (III)-doped amorphous calcium carbonate nanoparticles are an effective tool for these comparative studies due to their high magnetic resonance contrast and physicochemical properties. In an animal model of atherosclerosis, we compare the imaging performance of three types of nanoparticles: bare amorphous calcium carbonate and those functionalized with the ligands alendronate (for microcalcification targeting) and trimannose (for inflammation targeting). Our study provides useful insights into ligand-mediated targeted imaging of atherosclerosis through a combination of in vivo imaging, ex vivo tissue analysis, and in vitro targeting experiments.
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