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新型镧系涂层纳米载体的细胞内同步辐射纳米成像和 DNA 损伤/遗传毒性筛选。

Intracellular synchrotron nanoimaging and DNA damage/genotoxicity screening of novel lanthanide-coated nanovectors.

机构信息

School of Chemistry, University of Birmingham, Edgbaston, Birmingham, UK.

出版信息

Nanomedicine (Lond). 2010 Dec;5(10):1547-57. doi: 10.2217/nnm.10.96. Epub 2010 Sep 29.

Abstract

AIMS

In cancer therapy, research has focused on the development of nanocarriers that can aid diagnosis, deliver therapeutic agents and monitor treatment progress. This study introduces high-resolution synchrotron x-ray fluorescence microscopy (SR-XFM) to investigate intracellular localization of novel lanthanide-coated nanoparticles in human cells and their genotoxicity screening after internalization.

MATERIALS & METHODS: Noble metal nanoparticles coated with cerium and luminescent europium complexes have been developed as platforms for bioimaging and potential biodelivery applications. The intracellular distribution after internalization has been analyzed by ultrasensitive SR-XFM and genotoxicity evaluated using γ-H2AX DNA damage foci phosphorylation assay.

RESULTS

We demonstrate the unprecedented capability of SR-XFM for extremely sensitive nanoimaging and intracellular elemental distribution analysis of noble metal nanoparticles in cells. Furthermore, we show that, depending on the charge of the coating complex and the presence of the DNA cargo, the internalization of functionalized nanoparticles by human fibroblasts can cause elevated levels of DNA damage detected by histone H2AX phosphorylation.

CONCLUSION

The variable genotoxic impact of newly designed nanovectors emphasizes the need for careful and comprehensive testing of biological responses of all new nanoconstructs intended for future clinical applications. This can be greatly facilitated by SR-XFM nanoimaging of nanoparticles in cells at very low concentrations.

摘要

目的

在癌症治疗中,研究集中在开发纳米载体上,以帮助诊断、输送治疗剂和监测治疗进展。本研究采用高分辨率同步辐射 X 射线荧光显微镜(SR-XFM)研究新型镧系涂层纳米粒子在人细胞内的细胞内定位及其内化后的遗传毒性筛选。

材料与方法

用铈和发光铕配合物涂覆的贵金属纳米粒子已被开发为生物成像和潜在生物递药应用的平台。通过超灵敏的 SR-XFM 分析了内化后的细胞内分布,并通过γ-H2AX DNA 损伤焦点磷酸化测定评估了遗传毒性。

结果

我们证明了 SR-XFM 具有前所未有的能力,可对细胞内的贵金属纳米粒子进行极其灵敏的纳米成像和细胞内元素分布分析。此外,我们表明,根据涂层复合物的电荷和 DNA 货物的存在,人成纤维细胞内的功能化纳米粒子的内化可导致组蛋白 H2AX 磷酸化检测到的 DNA 损伤水平升高。

结论

新设计的纳米载体的遗传毒性影响具有可变性,强调需要对所有拟用于未来临床应用的新型纳米结构进行仔细和全面的生物反应测试。通过在非常低的浓度下对细胞内的纳米粒子进行 SR-XFM 纳米成像,可以极大地促进这一过程。

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