Design and Biodistribution of PEGylated Core-Shell X-ray Fluorescent Nanoparticle Contrast Agents

被引:0
作者
Saladino, Giovanni M. [1 ,2 ]
Brodin, Bertha [1 ]
Ciobanu, Mihai [1 ]
Kilic, Nuzhet I. [3 ]
Toprak, Muhammet S. [1 ]
Hertz, Hans M. [1 ]
机构
[1] KTH Royal Inst Technol, Sch Engn Sci, Dept Appl Phys, SE-10691 Stockholm, Sweden
[2] Stanford Univ, Sch Med, Dept Radiol, Stanford, CA 94305 USA
[3] KTH Royal Inst Technol, Sch Engn Sci Chem Biotechnol & Hlth, Dept Fiber & Polymer Technol, SE-10044 Stockholm, Sweden
关键词
core-shell nanoparticles; surface functionalization; X-ray fluorescence; PEGylation; nanomedicine; biodistribution; contrast agents; POLYETHYLENE-GLYCOL; TOMOGRAPHY; SPHERES;
D O I
10.1021/acsami.5c01902
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
Nanoparticle (NP) uptake by macrophages and their accumulation in undesired organs such as the liver and spleen constitute a major barrier to the effective delivery of NPs to targeted tissues for bioimaging and therapeutics. Surface functionalization with polyethylene glycol (PEG) has been demonstrated to be a promising strategy to limit NP sequestration, although its longitudinal stability under physiological conditions and impact on the NP biodistribution have not been investigated with an in vivo quantitative approach. X-ray fluorescence (XRF) imaging has been employed to noninvasively map the in vivo biodistribution of purposely designed molybdenum-based contrast agents, leading to submillimeter resolution, elemental specificity, and high penetration depth. In the present work, we design a stepwise layering approach for NP synthesis to investigate the role of chemisorbed and physisorbed PEG on silica-coated molybdenum-based contrast agents in affecting their in vivo biodistribution, using whole-body XRF imaging. Comparative quantitative in vivo studies indicated that physisorbed PEG (1.5 kDa) did not substantially affect the biodistribution, while the chemisorption route with mPEG-Si (6-9 PEG units) led to significant macroscopic variations in the biodistribution, leading to a reduction in NP uptake by the liver. Furthermore, the results highlighted the major role of the spleen in compensating for the limited sequestration by the liver, microscopically validated with a multiscale imaging approach with fluorophore doping of the silica shell. These findings demonstrated the promising role of XRF imaging for the rapid assessment of surface-functionalized contrast agents with whole-body in vivo quantitative pharmacokinetic studies, establishing the groundwork for developing strategies to identify and bypass undesired NP uptake.
引用
收藏
页码:26338 / 26347
页数:10
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