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Air-Blood-Barrier Translocation of Tracheally Instilled Gold Nanoparticles Inversely Depends on Particle Size

机译:气管滴注金纳米粒子的气血屏障易位与粒径成反比

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摘要

Gold nanoparticles (AuNP) provide many opportunities in imaging, diagnostics, and therapy in nanomedicine. For the assessment of AuNP biokinetics, we intratracheally instilled into rats a suite of 198Au-radio-labelled monodisperse, well-characterized, negatively-charged AuNP of five different sizes (1.4, 2.8, 5, 18, 80, 200 nm) and 2.8 nm AuNP with positive surface charges. At 1-h, 3-h, and 24-h the biodistribution of the AuNP was quantitatively measured by gamma-spectrometry to be used for comprehensive risk assessment. Our study shows, as AuNP get smaller, they are more likely to cross the air-blood-barrier (ABB) depending strongly on the inverse diameter d−1 of their gold core; i.e. their specific surface area (SSA). So, 1.4 nm AuNP (highest SSA) translocated most while 80 nm AuNP (lowest SSA) translocated least, but 200 nm particles did not follow the d−1 relation translocating significantly higher than 80 nm AuNP. However, relative to the AuNP which had crossed the ABB, their retention in most of the secondary organs and tissues was SSA-independent. Only renal filtration, retention in blood and excretion via urine further declined with d−1 of AuNP core. Translocation of 5, 18 and 80 nm AuNP is virtually complete after 1-h, while 1.4 nm AuNP continue to translocate until 3-h. Translocation of negatively charged 2.8 nm AuNP was significantly higher than for positively charged 2.8 nm AuNP. Our study shows that translocation across the ABB and accumulation and retention in secondary organs and tissues are two distinct processes, both depending specifically on particle characteristics such as SSA and surface charge.
机译:金纳米颗粒(AuNP)为纳米医学的成像,诊断和治疗提供了许多机会。为了评估AuNP的生物动力学,我们向大鼠气管内滴注了一组 198 Au放射性标记的单分散,特征明确的,带负电荷的5种不同大小的AuNP(1.4、2.8、5、18 ,80、200 nm)和2.8 nm AuNP带正表面电荷。在1小时,3小时和24小时,通过γ光谱法对AuNP的生物分布进行了定量测量,以用于全面的风险评估。我们的研究表明,随着AuNP变小,它们越有可能越过空气屏障(ABB),这在很大程度上取决于其金芯的反直径d -1 。即它们的比表面积(SSA)。因此,1.4 nm AuNP(最高SSA)易位最多,而80 nm AuNP(最低SSA)易位最少,但200 nm粒子未遵循明显高于80 nm AuNP的d -1 关系。但是,相对于穿过ABB的AuNP,它们在大多数次要器官和组织中的保留是非SSA依赖性的。 AuNP核心的d -1 仅使肾脏滤过,血液滞留和尿液排泄进一步降低。 5、18和80 nm AuNP的移位实际上在1小时后完成,而1.4 nm AuNP继续移位,直到3小时。带负电的2.8 nm AuNP的移位明显高于带正电的2.8 nm AuNP的移位。我们的研究表明,跨ABB的转运以及在次要器官和组织中的积累和保留是两个不同的过程,这两个过程都特别取决于颗粒特征,例如SSA和表面电荷。

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