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吉西他滨与碳酸磷灰石相互作用,同时降低粒径并增强对乳腺癌细胞的细胞毒性。

Gemcitabine interacts with carbonate apatite with concomitant reduction in particle diameter and enhancement of cytotoxicity in breast cancer cells.

作者信息

Mozar Fitya S, Chowdhury Ezharul H

机构信息

Advanced Engineering Platform and Jeffrey Cheah School of Medicine and Health Sciences, Monash University, Malaysia.

出版信息

Curr Drug Deliv. 2015;12(3):333-41. doi: 10.2174/1567201812666150120153809.

DOI:10.2174/1567201812666150120153809
PMID:25600981
Abstract

Substantial amount of research has been done in recent decades for the development of nanoparticle systems to selectively deliver drugs to cancer cells for concurrently enhancing and reducing anti-cancer and off-target effects, respectively. pH-sensitive carbonate apatite (CA) was originally developed for efficient and targeted delivery of DNA, siRNA and proteins to various cancer cell lines. Recently, the CA particles were employed to deliver anti-cancer drugs, cyclophosphamide, doxorubicin and methotrexate to cancer cells. Here, we report on the fabrication and characterization of gemcitabine- loaded CA particles, followed by the evaluation of their roles in enhancement of cytotoxicity in two human and one murine breast cancer cell lines. HPLC was performed to measure binding efficiency of the drug to the apatite particles whereas particle size and zeta potential were evaluated to characterize drug/apatite complex. Depending on the initial doses of the drug, its bind binding affinity towards the particles varied from 3.85% to 4.45%. The particle size was found to surprisingly decrease with an increase of the initial drug concentration. In vitro chemosensitivity assay revealed that apatite/drug nanoparticle complexes presented significantly higher cytotoxicity to breast cancer cells compared to free drugs, which could be correlated with the enhanced cellular uptake of the small size drug-loaded particles through endocytosis compared to the passive diffusion of the free drug.

摘要

近几十年来,为了开发纳米颗粒系统,以便将药物选择性地递送至癌细胞,从而分别同时增强抗癌作用并降低脱靶效应,人们开展了大量研究。pH敏感的碳酸磷灰石(CA)最初是为了将DNA、siRNA和蛋白质高效且靶向地递送至各种癌细胞系而开发的。最近,CA颗粒被用于将抗癌药物环磷酰胺、阿霉素和甲氨蝶呤递送至癌细胞。在此,我们报告了吉西他滨负载的CA颗粒的制备与表征,随后评估了它们在增强两种人源和一种鼠源乳腺癌细胞系细胞毒性方面的作用。采用高效液相色谱法测量药物与磷灰石颗粒的结合效率,同时评估粒径和zeta电位以表征药物/磷灰石复合物。根据药物的初始剂量,其与颗粒的结合亲和力在3.85%至4.45%之间变化。令人惊讶的是,发现粒径随着初始药物浓度的增加而减小。体外化学敏感性试验表明,与游离药物相比,磷灰石/药物纳米颗粒复合物对乳腺癌细胞具有显著更高的细胞毒性,这可能与通过内吞作用增强的小尺寸载药颗粒的细胞摄取有关(相比之下,游离药物是被动扩散)。

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