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石墨烯作为一种纳米载体,可诱导不同来源的转化癌细胞系发生细胞凋亡。

Graphene as a nanocarrier for tamoxifen induces apoptosis in transformed cancer cell lines of different origins.

机构信息

Department of Organic Chemistry, Indian Institute of Science, Bangalore 560 012, India.

出版信息

Small. 2012 Jan 9;8(1):131-43. doi: 10.1002/smll.201101640. Epub 2011 Nov 18.

Abstract

A cationic amphiphile, cholest-5en-3β-oxyethyl pyridinium bromide (PY(+) -Chol), is able to efficiently disperse exfoliated graphene (GR) in water by the physical adsorption of PY(+) -Chol on the surface of GR to form stable, dark aqueous suspensions at room temperature. The GR-PY(+) -Chol suspension can then be used to solubilize Tamoxifen Citrate (TmC), a breast cancer drug, in water. The resulting TmC-GR-PY(+) -Chol is stable for a long time without any precipitation. Fluorescence emission and UV absorption spectra indicate the existence of noncovalent interactions between TmC, GR, and PY(+) -Chol in these suspensions. Electron microscopy shows the existence of segregated GR sheets and TmC 'ribbons' in the composite suspensions. Atomic force microscopy indicates the presence of 'extended' structures of GR-PY(+) -Chol, which grows wider in the presence of TmC. The slow time-dependent release of TmC is noticed in a reconstituted cell culture medium, a property useful as a drug carrier. TmC-GR-PY(+) -Chol selectively enhanced the cell death (apoptosis) of the transformed cancer cells compared to normal cells. This potency is found to be true for a wide range of transformed cancer cells viz. HeLa, A549, ras oncogene-transformed NIH3T3, HepG2, MDA-MB231, MCF-7, and HEK293T compared to the normal cell HEK293 in vitro. Confocal microscopy confirmed the high efficiency of TmC-GR-PY(+) -Chol in delivering the drug to the cells, compared to the suspensions devoid of GR.

摘要

一种阳离子两亲化合物,胆甾-5-烯-3β-氧基乙基吡啶溴盐(PY(+) -Chol),能够通过 PY(+) -Chol 在 GR 表面的物理吸附有效地将剥离的石墨烯(GR)分散在水中,从而在室温下形成稳定的、深黑色的水悬浮液。GR-PY(+) -Chol 悬浮液可用于在水中溶解他莫昔芬柠檬酸酯(TmC),一种乳腺癌药物。所得的 TmC-GR-PY(+) -Chol 在长时间内稳定,没有任何沉淀。荧光发射和紫外吸收光谱表明,在这些悬浮液中,TmC、GR 和 PY(+) -Chol 之间存在非共价相互作用。电子显微镜显示在复合悬浮液中存在分层的 GR 片和 TmC '条带'。原子力显微镜表明存在 GR-PY(+) -Chol 的 '伸展'结构,在 TmC 的存在下变得更宽。在重建的细胞培养基中注意到 TmC 的缓慢时变释放,这是作为药物载体的有用性质。与正常细胞相比,TmC-GR-PY(+) -Chol 选择性地增强了转化癌细胞的细胞死亡(凋亡)。这种效力在广泛的转化癌细胞系中被发现是真实的,例如 HeLa、A549、ras 癌基因转化的 NIH3T3、HepG2、MDA-MB231、MCF-7 和 HEK293T,与体外正常细胞 HEK293 相比。共聚焦显微镜证实了 TmC-GR-PY(+) -Chol 与不含 GR 的悬浮液相比,将药物递送到细胞中的效率很高。

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