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首页> 外文期刊>Oncology letters >Analysis of radiation effects in two irradiated tumor spheroid models
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Analysis of radiation effects in two irradiated tumor spheroid models

机译:两种辐照肿瘤球状模型中辐射效应分析

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摘要

Multicellular spheroids have proven suitable as three-dimensional in vivo-like models of non-vascularized micrometastases. Unlike monolayer-based models, spheroids mirror the cellular milieu and the pathophysiological gradients inside tumor nodules. However, there is limited knowledge of the radiation effects at the molecular level in spheroids of human origin. The present study is a presentation of selected cell biological processes that may easily be analyzed with methods available at routine pathology laboratories. Using gamma irradiated pancreatic neuroendocrine BON1 and colonic adenocarcinoma HCT116 spheroids as model systems, the present study assessed the radiobiological response in these models. Spheroid growth after irradiation was followed over time and molecular responses were subsequently assessed with immunohistochemistry (IHC) staining for descriptive analyses and semi-automatic grading of apoptosis, G(2)-phase and senescence in thin sections of the spheroids. Growth studies demonstrated the BON1 spheroids were slower growing and less sensitive to radiation compared with the HCT116 spheroids. IHC staining for G2-phase was primarily observed in the outer viable P-cell layers of the spheroids, with the 6 Gy irradiated HCT116 spheroids demonstrating a very clear increase in staining intensity compared with unirradiated spheroids. Apoptosis staining results indicated increased apoptosis with increasing radiation doses. No clear association between senescence and radiation exposure in the spheroids were observed. The present results demonstrate the feasibility of the use of multicellular spheroids of human origin in combination with IHC analyses to unravel radiobiological responses at a molecular level. The present findings inspire further investigations, including other relevant IHC-detectable molecular processes in time-and radiation dose-dependent settings.
机译:多细胞球体已被证明适合于非血管化微转移的体内模型的三维。与基于单层的模型不同,Spheroids镜像细胞内部和肿瘤结节内的病理生理学梯度。然而,对人来源的球状体中的分子水平的辐射效应存在有限。本研究表明了所选择的细胞生物学过程,可以通过常规病理实验室的方法轻松分析。使用γ辐照的胰腺神经内分泌Con1和结肠腺癌HCT116球体作为模型系统,本研究评估了这些模型中的放射生物反应。辐照后的球形生长随后随着时间的推移,随后用免疫组织化学(IHC)染色来评估分子反应,用于在球状体的薄切片中的细胞凋亡,G(2) - 异种和衰老的描述性分析和半自动分级。增长研究表明,与HCT116球状体相比,Bon1球状体生长较慢,对辐射不太敏感。对于G2相的IHC染色主要在球状体的外部可活性p细胞层中观察到,6GY辐照的HCT116球体与未照射的球状体相比,染色强度的显着增加。细胞凋亡染色结果表明辐射剂量增加增加了凋亡。观察到衰老和辐射暴露在球状体中没有明确关联。目前的结果表明,使用人类来源的多细胞球体与IHC分析在分子水平下的解开放射生物反应的可行性。本研究结果激发了进一步的研究,包括在时间和放射剂量依赖性设置中的其他相关的IHC可检测分子过程。

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