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Multimodal imaging of the receptor for advanced glycation end-products with molecularly targeted nanoparticles

DOI:10.7150/thno.24791 期刊:Theranostics 出版年份:2018 更新时间:2025-09-23 15:21:01
摘要: The receptor for advanced glycation end-products (RAGE) is central to multiple disease states, including diabetes-related conditions such as peripheral arterial disease (PAD). Despite RAGE’s importance in these pathologies, there remains a need for a molecular imaging agent that can accurately assess RAGE levels in vivo. Therefore, we have developed a multimodal nanoparticle-based imaging agent targeted at RAGE with the well-characterized RAGE ligand, carboxymethyllysine (CML)-modified human serum albumin (HSA). Methods: A multimodal tracer (64Cu-Rho-G4-CML) was developed using a generation-4 (G4) polyamidoamine (PAMAM) dendrimer, conjugated with both rhodamine and copper-64 (64Cu) chelator (NOTA) for optical and PET imaging, respectively. First, 64Cu-Rho-G4-CML and its non-targeted analogue (64Cu-Rho-G4-HSA) were evaluated chemically using techniques such as dynamic light scattering (DLS), electron microscopy and nuclear magnetic resonance (NMR). The tracers’ binding capabilities were examined at the cellular level and optimized using live and fixed HUVEC cells grown in 5.5-30 mM glucose, followed by in vivo PET-CT imaging, where the probes’ kinetics, biodistribution, and RAGE targeting properties were examined in a murine model of hindlimb ischemia. Finally, histological assessment of RAGE levels in both ischemic and non-ischemic tissues was performed. Conclusions: Our RAGE-targeted probe demonstrated an average size of 450 nm, a Kd of 340-390 nM, rapid blood clearance, and a 3.4 times greater PET uptake in ischemic RAGE-expressing hindlimbs than their non-ischemic counterpart. We successfully demonstrated increased RAGE expression in a murine model of hindlimb ischemia and the feasibility for non-invasive examination of cellular, tissue, and whole-body RAGE levels with a molecularly targeted tracer.
作者: Christian J. Konopka,Marcin Wozniak,Jamila Hedhli,Agata Ploska,Aaron Schwartz-Duval,Anna Siekierzycka,Dipanjan Pan,Gnanasekar Munirathinam,Iwona T. Dobrucki,Leszek Kalinowski,Lawrence W. Dobrucki
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To develop a multimodal nanoparticle-based imaging agent targeted at RAGE for accurate assessment of RAGE levels in vivo, particularly in diabetes-related conditions such as peripheral arterial disease (PAD).

The study successfully demonstrated the utility of a multimodal nanoparticle-based imaging agent for non-invasive examination of RAGE levels in a murine model of hindlimb ischemia. The RAGE-targeted probe showed significant uptake in ischemic tissues, providing a potential tool for diagnosing and monitoring RAGE-related pathologies.

The size of 64Cu-Rho-G4-CML prevents it from crossing the blood-brain barrier, limiting its use for neurological assessments. Additionally, the use of CML as a targeting ligand may confer non-specific binding in conditions where other CML receptors are highly upregulated.

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