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Enhanced retention and cellular uptake of nanoparticles in tumors by controlling their aggregation behavior

机译:通过控制纳米粒子的聚集行为,增强纳米粒子在肿瘤中的保留和细胞摄取

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Effective accumulation of nanoparticles (NPs) in tumors is crucial for NP-assisted cancer diagnosis and treatment. With the hypothesis that aggregation of NPs stimulated by tumor microenvironment can be utilized to enhance retention and cellular uptake of NPs in tumors, we designed a smart NP system to evaluate the effect of aggregation on NPs' accumulation in tumor tissue. Gold nanoparticles (AuNPs, ~16 nm) were facilely prepared by surface modification with mixed-charge zwitterionic self-assembled monolayers, which can be stable at the pH of blood and normal tissues but aggregate instantly in response to the acidic extracellular pH of solid tumors. The zwitterionic AuNPs exhibited fast, ultrasensitive, and reversible response to the pH change from pH 7.4 to pH 6.5, which enabled the AuNPs to be well dispersed at pH 7.4 with excellent stealth ability to resist uptake by macrophages, while quickly aggregating at pH 6.5, leading to greatly enhanced uptake by cancer cells. An in vivo study demonstrated that the zwitterionic AuNPs had a considerable blood half-life with much higher tumor accumulation, retention, and cellular internalization than nonsensitive PEGylated AuNPs. A preliminary photothermal tumor ablation evaluation suggested the aggregation of AuNPs can be applied to cancer NIR photothermal therapy. These results suggest that controlled aggregation of NPs sensitive to tumor microenvironment can serve as a universal strategy to enhance the retention and cellular uptake of inorganic NPs in tumors, and modifying NPs with a mixed-charge zwitterionic surface can provide an easy way to obtain stealth properties and pH-sensitivity at the same time.
机译:纳米颗粒(NPs)在肿瘤中的有效积累对于NP辅助的癌症诊断和治疗至关重要。假设可以利用肿瘤微环境刺激的NP聚集来增强NP在肿瘤中的保留和细胞摄取,我们设计了一个智能NP系统来评估聚集对NP在肿瘤组织中积累的影响。金纳米颗粒(AuNPs,〜16 nm)通过混合电荷两性离子自组装单层表面修饰而轻松制备,其在血液和正常组织的pH下可以稳定,但在实体瘤的酸性细胞外pH下可立即聚集。两性离子AuNP对pH值从7.4到pH 6.5的变化表现出快速,超灵敏和可逆的响应,这使AuNP可以在pH 7.4时很好地分散,具有出色的抵抗巨噬细胞摄取的隐形能力,而在pH 6.5时迅速聚集。导致癌细胞摄取大大增强。一项体内研究表明,两性离子AuNPs的血液半衰期比非敏感的PEG化AuNPs的血液半衰期长得多,而且肿瘤的蓄积,保留和细胞内化性也更高。初步的光热肿瘤消融评估表明,AuNP的聚集可用于癌症近红外光热疗法。这些结果表明,对肿瘤微环境敏感的NP的受控聚集可以作为提高无机NP在肿瘤中的保留和细胞摄取的通用策略,并且用混合电荷的两性离子表面修饰NP可以提供获得隐身特性的简便方法。同时具有pH敏感性。

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