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金纳米球的细胞核靶向或细胞质靶向光热解的比较研究:连续波或脉冲激光。

Comparative study of photothermolysis of cancer cells with nuclear-targeted or cytoplasm-targeted gold nanospheres: continuous wave or pulsed lasers.

机构信息

Georgia Institute of Technology, School of Chemistry and Biochemistry, Laser Dynamics Laboratory, 901 Atlantic Drive, Atlanta, Georgia 30332, USA.

出版信息

J Biomed Opt. 2010 Sep-Oct;15(5):058002. doi: 10.1117/1.3486538.

DOI:10.1117/1.3486538
PMID:21054128
Abstract

We conduct a comparative study on the efficiency and cell death pathways of continuous wave (cw) and nanosecond pulsed laser photothermal cancer therapy using gold nanospheres delivered to either the cytoplasm or nucleus of cancer cells. Cytoplasm localization is achieved using arginine-glycine-aspartate peptide modified gold nanospheres, which target integrin receptors on the cell surface and are subsequently internalized by the cells. Nuclear delivery is achieved by conjugating the gold nanospheres with nuclear localization sequence peptides originating from the simian virus. Photothermal experiments show that cell death can be induced with a single pulse of a nanosecond laser more efficiently than with a cw laser. When the cw laser is applied, gold nanospheres localized in the cytoplasm are more effective in inducing cell destruction than gold nanospheres localized at the nucleus. The opposite effect is observed when the nanosecond pulsed laser is used, suggesting that plasmonic field enhancement of the nonlinear absorption processes occurs at high localization of gold nanospheres at the nucleus. Cell death pathways are further investigated via a standard apoptosis kit to show that the cell death mechanisms depend on the type of laser used. While the cw laser induces cell death via apoptosis, the nanosecond pulsed laser leads to cell necrosis. These studies add mechanistic insight to gold nanoparticle-based photothermal therapy of cancer.

摘要

我们使用递送到癌细胞细胞质或细胞核的金纳米球,对连续波 (cw) 和纳秒脉冲激光光热癌症治疗的效率和细胞死亡途径进行了比较研究。细胞质定位是通过使用精氨酸-甘氨酸-天冬氨酸肽修饰的金纳米球实现的,该肽靶向细胞表面的整合素受体,随后被细胞内化。核递送是通过将金纳米球与源自猴病毒的核定位序列肽缀合来实现的。光热实验表明,与连续波激光相比,纳秒激光的单次脉冲更有效地诱导细胞死亡。当应用连续波激光时,定位在细胞质中的金纳米球比定位在核中的金纳米球更有效地诱导细胞破坏。当使用纳秒脉冲激光时,观察到相反的效果,这表明在金纳米球高度定位在核时,等离子体场增强了非线性吸收过程。通过标准凋亡试剂盒进一步研究细胞死亡途径,以表明细胞死亡机制取决于所用激光的类型。虽然连续波激光通过细胞凋亡诱导细胞死亡,但纳秒脉冲激光导致细胞坏死。这些研究为基于金纳米粒子的癌症光热疗法提供了机制见解。

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