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载顺铂金纳米粒子具有增强的重现性、载药量和稳定性:更接近药物批准?

Cisplatin-tethered gold nanoparticles that exhibit enhanced reproducibility, drug loading, and stability: a step closer to pharmaceutical approval?

机构信息

Strathclyde Institute of Pharmacy and Biomedical Sciences, Arbuthnott Building, University of Strathclyde, 161 Cathedral Street, Glasgow G4 0RE, United Kingdom.

出版信息

Inorg Chem. 2012 Mar 19;51(6):3490-7. doi: 10.1021/ic202197g. Epub 2012 Mar 5.

DOI:10.1021/ic202197g
PMID:22390791
Abstract

Gold nanoparticles (AuNPs) can be used as delivery vehicles for platinum anticancer drugs, improving their targeting and uptake into cells. Here, we examine the appropriateness of different-sized AuNPs as components of platinum-based drug-delivery systems, investigating their controlled synthesis, reproducibility, consistency of drug loading, and stability. The active component of cisplatin was tethered to 25, 55, and 90 nm AuNPs, with the nanoparticles being almost spherical in nature and demonstrating good batch-to-batch reproducibility (24.37 ± 0.62, 55.2 ± 1.75, and 89.1 ± 2.32 nm). The size distribution of 25 nm AuNPs has been significantly improved, compared with a previous method that produces polydispersed nanoparticles. Attachment of platinum to the AuNP surface through a poly(ethylene glycol) (PEG) linker exhibits an increase in the drug loading with increasing particle size: 25 nm (815 ± 106 drug molecules per AuNP), 55 nm (14216 ± 880), and 90 nm (54487 ± 15996). The stability of the naked, PEGylated, and platinum-conjugated nanoparticles has been examined over time under various conditions. When stored at 4 °C, there is minimal variation in the diameter for all three AuNP sizes; variation after 28 days for the 25 nm AuNPs was 2.4%; 55 nm, 3.3%; and 90 nm, 3.6%. The 25 nm AuNPs also demonstrate minimal changes in UV-visible absorbance over the same time period.

摘要

金纳米粒子(AuNPs)可用作铂类抗癌药物的输送载体,提高其靶向性和细胞摄取率。在这里,我们研究了不同尺寸的 AuNPs 作为基于铂的药物输送系统成分的适宜性,研究了它们的可控合成、重现性、药物负载的一致性和稳定性。顺铂的活性成分被连接到 25、55 和 90nm 的 AuNPs 上,这些纳米粒子本质上几乎呈球形,表现出良好的批次间重现性(24.37±0.62、55.2±1.75 和 89.1±2.32nm)。与以前生产多分散纳米粒子的方法相比,25nmAuNP 的尺寸分布得到了显著改善。通过聚乙二醇(PEG)接头将铂连接到 AuNP 表面,随着颗粒尺寸的增加,药物负载量增加:25nm(每个 AuNP 有 815±106 个药物分子)、55nm(14216±880)和 90nm(54487±15996)。在不同条件下,随着时间的推移,对裸、PEG 化和铂缀合纳米粒子的稳定性进行了研究。在 4°C 下储存时,三种 AuNP 尺寸的直径都有最小的变化;25nmAuNP 在 28 天后的变化为 2.4%;55nm,3.3%;90nm,3.6%。在同一时间段内,25nmAuNP 的紫外可见吸收也有最小的变化。

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