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Gastrointestinal bioavailability of 2.0 nm diameter gold nanoparticles

机译:直径为2.0 nm的金纳米颗粒的胃肠道生物利用度

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摘要

The use of gold nanoparticles as imaging agents and therapeutic delivery systems is growing rapidly. However, a significant limitation of gold nanoparticles currently is their low absorption efficiencies in the gastrointestinal (GI) tract following oral administration. In an attempt to identify ligands that facilitate gold nanoparticle absorption in the GI tract, we have studied the oral bioavailability of 2.0 nm diameter gold nanoparticles modified with the small molecules p-mercaptobenzoic acid and glutathione, and polyethylene glycols (PEG) of different lengths and charge (neutral and anionic). We show that GI absorption of gold nanoparticles modified with the small molecules tested was undetectable. However, the absorption of PEGs depended upon PEG length, with the shortest PEG studied yielding gold nanoparticle absorptions that are orders-of-magnitude larger than observed previously. As the oral route is the most convenient one for administering drugs and diagnostic reagents, these results suggest that short-chain PEGs may be useful in the design of gold nanoparticles for the diagnosis and treatment of disease.
机译:金纳米颗粒作为成像剂和治疗递送系统的使用正在迅速增长。然而,目前金纳米颗粒的显着限制是口服后它们在胃肠道(GI)中的吸收效率低。为了确定有助于金纳米颗粒在胃肠道中吸收的配体,我们研究了用小分子对巯基苯甲酸和谷胱甘肽以及不同长度的聚乙二醇(PEG)修饰的直径为2.0 nm的金纳米颗粒的口服生物利用度。电荷(中性和阴离子)。我们表明用检测到的小分子修饰的金纳米颗粒的GI吸收是不可检测的。但是,PEG的吸收取决于PEG的长度,研究的最短的PEG产生的金纳米颗粒吸收比以前观察到的大几个数量级。由于口服途径是给药药物和诊断试剂的最便捷途径,因此这些结果表明,短链PEG可能在设计金纳米颗粒以诊断和治疗疾病中有用。

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