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抗癌药物对 DNA 的影响 - 基于中子光谱学、同步辐射傅里叶变换红外光谱学和扩展 X 射线吸收精细结构的研究。

Anticancer drug impact on DNA - a study by neutron spectroscopy coupled with synchrotron-based FTIR and EXAFS.

机构信息

Química-Física Molecular, Department of Chemistry, University of Coimbra, 3004-535 Coimbra, Portugal.

ISIS Facility, STFC Rutherford Appleton Laboratory, Chilton, Didcot, Oxfordshire OX11 0QX, UK.

出版信息

Phys Chem Chem Phys. 2019 Feb 20;21(8):4162-4175. doi: 10.1039/c8cp05881d.

DOI:10.1039/c8cp05881d
PMID:30656331
Abstract

Complementary structural and dynamical information on drug-DNA interplay has been achieved at a molecular level, for Pt/Pd-drugs, allowing a better understanding of their pharmacodynamic profile which is crucial for the development of improved chemotherapeutic agents. The interaction of two cisplatin-like dinuclear Pt(ii) and Pd(ii) complexes with DNA was studied through a multidisciplinary experimental approach, using quasi-elastic neutron scattering (QENS) techniques coupled with synchrotron-based extended X-ray absorption fine structure (SR-EXAFS) and Fourier-Transform Infrared Spectroscopy-Attenuated Total Reflectance (SR-FTIR-ATR). DNA extracted from drug-exposed human triple negative breast cancer cells (MDA-MB-231) was used, with a view to evaluate the effect of the unconventional antineoplastic agents on this low prognosis type of cancer. The drug impact on DNA's dynamical profile, via its hydration layer, was provided by QENS, a drug-triggered enhanced mobility having been revealed. Additionally, an onset of anharmonicity was detected for dehydrated DNA, at room temperature. Far- and mid-infrared measurements allowed the first simultaneous detection of the drugs and their primary pharmacological target, as well as the drug-prompted changes in DNA's conformation that mediate cytotoxicity. The local environment of the absorbing Pd(ii) and Pt(ii) centers in the drugs' adducts with adenine, guanine and glutathione was attained by EXAFS.

摘要

已经在分子水平上获得了有关药物-DNA 相互作用的补充结构和动态信息,用于铂/钯药物,从而可以更好地了解其药效学特征,这对于开发改良的化疗药物至关重要。通过使用准弹性中子散射(QENS)技术与基于同步加速器的扩展 X 射线吸收精细结构(SR-EXAFS)和傅立叶变换红外光谱-衰减全反射(SR-FTIR-ATR)相结合的多学科实验方法,研究了两种顺铂类似的双核 Pt(ii)和 Pd(ii)配合物与 DNA 的相互作用。从暴露于药物的人三阴性乳腺癌细胞(MDA-MB-231)中提取的 DNA 被用于评估非常规抗肿瘤药物对这种低预后类型癌症的影响。通过 QENS 提供了药物对 DNA 动态特性的影响,通过其水合层揭示了药物触发的增强迁移。此外,在室温下检测到脱水 DNA 的非谐性开始。远-中和中红外测量允许首次同时检测药物及其主要药理靶标,以及介导细胞毒性的 DNA 构象变化。通过 EXAFS 获得了药物与腺嘌呤、鸟嘌呤和谷胱甘肽加合物中吸收的 Pd(ii)和 Pt(ii)中心的局部环境。

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