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Role of intercellular communications in breast cancer multicellular tumor spheroids after chemotherapy.

机译:细胞间通讯在化疗后乳腺癌多细胞肿瘤球中的作用。

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Tumor heterogeneity is an important feature that is especially involved in tumor aggressiveness. Multicellular tumor spheroids (MTS) may provide some benefits in different steps for investigation of the aggregation, organization, differentiation, and network formation of tumor cells in 3D space. This model offers a unique opportunity for improvements in the capability of a current strategy to detect the effect of an appropriate anticancer agent. The aim of this study was to investigate the cellular interactions and morphological changes following chemotherapy in a 3D breast cancer spheroid model. Distribution of the gap junction protein "connexin-43" and the tight junction protein "occludin" was investigated by immunohistochemistry. Cellular interactions were examined by using transmission and scanning electron microscopies as well as light microscopy with Giemsa staining after treating cells with doxorubicin, docetaxel, and doxorubicin/docetaxel combination. Statistical analyses showed significant changes and various alterations that were observed in all groups; however, the most prominent effect was detected in the doxorubicin/docetaxel combination group. Distinct composition as a vessel-like structure and a pseudoglandular pattern of control spheroids were detected in drug-administered groups. Immunohistochemical results were consistent with the ultrastructural changes. In conclusion, doxorubicin/docetaxel combination may be more effective than the single drug usage as shown in a 3D model. The MTS model has been found to be an appropriate and reliable method for the detection of the changes in the expression of cellular junction proteins as well as other cellular proteins occurring after chemotherapy. The MTS model can be used to validate the effects of various combinations or new chemotherapeutic agents as well as documentation of possible mechanisms of new drugs.
机译:肿瘤异质性是一个重要特征,尤其与肿瘤侵袭性有关。在研究3D空间中肿瘤细胞的聚集,组织,分化和网络形成的不同步骤中,多细胞肿瘤球体(MTS)可能会提供一些好处。该模型为改善当前策略检测适当抗癌药效果的能力提供了独特的机会。这项研究的目的是研究3D乳腺癌球体模型中化疗后的细胞相互作用和形态变化。通过免疫组织化学研究了间隙连接蛋白“连接蛋白43”和紧密连接蛋白“封闭蛋白”的分布。在用阿霉素,多西他赛和阿霉素/多西他赛组合处理细胞后,通过透射和扫描电子显微镜以及吉姆萨染色的光学显微镜检查细胞相互作用。统计分析表明,在所有组中均观察到了显着的变化和各种变化。然而,在阿霉素/多西他赛联合用药组中发现了最显着的作用。在给药组中检测到不同的组成为血管样结构和对照球体的假腺样。免疫组织化学结果与超微结构变化一致。总之,阿霉素/多西他赛组合可能比3D模型中显示的单一药物使用更为有效。已经发现,MTS模型是检测细胞连接蛋白以及化疗后发生的其他细胞蛋白表达变化的合适且可靠的方法。 MTS模型可用于验证各种组合或新化疗药物的作用,以及新药可能作用机理的文献记录。

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