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Tuning surface coatings of optimized magnetite nanoparticle tracers for in vivo Magnetic Particle Imaging

机译:调整用于体内磁性粒子成像的优化磁铁矿纳米粒子示踪剂的表面涂层

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摘要

Surface coatings are important components of Magnetic Particle Imaging (MPI) tracers – they preserve their key properties responsible for optimum tracer performance in physiological environments. In vivo, surface coatings form a physical barrier between the hydrophobic SPION cores and the physiological environment, and their design dictates the blood half-life and biodistribution of MPI tracers. Here we show the effect of tuning poly(ethylene glycol) (PEG)-based surface coatings on both in vitro and in vivo (mouse model) MPI performance of SPIONs. Our results showed that varying PEG molecular weight had a profound impact on colloidal stability, characterized using Dynamic Light Scattering (DLS), and the m’(H) response of SPIONs, measured in a 25 kHz/20 mTμ0−1max Magnetic Particle Spectrometer (MPS). Increasing PEG molecular weight from 5 kDa to 20 kDa preserved colloidal stability and m’(H) response of ~25 nm SPIONs – the optimum core diameter for MPI – in serum-rich cell culture medium for up to 24 hours. Furthermore, we compared the in vivo circulation time of SPIONs as a function of hydrodynamic diameter and showed that clustered SPIONs can adversely affect blood half-life; critically, SPIONs with clusters had 5 times shorter blood half-life than individually coated SPIONs. We anticipate that the development of MPI SPION tracers with long blood half-lives have potential not only in vascular imaging applications, but also enable opportunities in molecular targeting and imaging – a critical step towards early cancer detection using the new MPI modality.
机译:表面涂层是磁性粒子成像(MPI)示踪剂的重要组成部分–它们保留了其关键特性,可在生理环境中实现最佳的示踪剂性能。在体内,表面涂层在疏水性SPION核与生理环境之间形成物理屏障,其设计决定了MPI示踪剂的血液半衰期和生物分布。在这里,我们展示了调节聚(乙二醇)(PEG)基表面涂层对SPIONs的体内和体外(小鼠模型)MPI性能的影响。我们的结果表明,变化的PEG分子量对胶体稳定性有深远的影响,使用动态光散射(DLS)和SPIONs的m'(H)响应进行表征,在25 kHz / 20mTμ0 < / sup> max磁性粒子光谱仪(MPS)。在富含血清的细胞培养基中,将PEG分子量从5 kDa增加到20 kDa,可保持胶体稳定性和〜25 nm SPIONs的m'(H)响应-MPI的最佳核心直径-长达24小时。此外,我们比较了SPIONs的体内循环时间与流体动力学直径的函数关系,并发现聚簇的SPIONs会对血液半衰期产生不利影响。至关重要的是,具有簇状的SPIONs的血液半衰期比单独涂覆的SPIONs短5倍。我们预计,具有长血液半衰期的MPI SPION示踪剂的开发不仅在血管成像应用方面具有潜力,而且在分子靶向和成像方面也带来了机遇-这是使用新的MPI模式进行早期癌症检测的关键一步。

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