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地塞米松在随机定位过程中选择性抑制转移性甲状腺癌细胞的脱离。

Dexamethasone Selectively Inhibits Detachment of Metastatic Thyroid Cancer Cells during Random Positioning.

作者信息

Melnik Daniela, Cortés-Sánchez José Luis, Sandt Viviann, Kahlert Stefan, Kopp Sascha, Grimm Daniela, Krüger Marcus

机构信息

Department of Microgravity and Translational Regenerative Medicine, Otto von Guericke University, 39106 Magdeburg, Germany.

Research Group "Magdeburger Arbeitsgemeinschaft für Forschung unter Raumfahrt- und Schwerelosigkeitsbedingungen" (MARS), Otto von Guericke University, 39106 Magdeburg, Germany.

出版信息

Cancers (Basel). 2023 Mar 7;15(6):1641. doi: 10.3390/cancers15061641.

Abstract

We recently reported that synthetic glucocorticoid dexamethasone (DEX) is able to suppress metastasis-like spheroid formation in a culture of follicular thyroid cancer (FTC)-133 cells cultured under random positioning. We now show that this inhibition was selective for two metastatic thyroid carcinoma cells, FTC-133 and WRO, whereas benign Nthy-ori 3-1 thyrocytes and recurrent ML-1 follicular thyroid cancer cells were not affected by DEX. We then compare Nthy-ori 3-1 and FTC-133 cells concerning their adhesion and mechanosignaling. We demonstrate that DEX disrupts random positioning-triggered p38 stress signaling in FTC-133 cells, thereby antagonizing a variety of biological functions. Thus, DEX treatment of FTC-133 cells is associated with increased adhesiveness, which is mainly caused by the restored, pronounced formation of a normal number of tight junctions. Moreover, we show that Nthy-ori 3-1 and ML-1 cells upregulate the anti-adhesion protein mucin-1 during random positioning, presumably as a protection against mechanical stress. In summary, mechanical stress seems to be an important component in this metastasis model system that is processed differently by metastatic and healthy cells. The balance between adhesion, anti-adhesion and cell-cell connections enables detachment of adherent human cells on the random positioning machine-or not, allowing selective inhibition of thyroid in vitro metastasis by DEX.

摘要

我们最近报道,合成糖皮质激素地塞米松(DEX)能够抑制在随机定位培养条件下的甲状腺滤泡癌(FTC)-133细胞培养物中类似转移的球体形成。我们现在表明,这种抑制作用对两种转移性甲状腺癌细胞FTC-133和WRO具有选择性,而良性Nthy-ori 3-1甲状腺细胞和复发性ML-1甲状腺滤泡癌细胞不受DEX影响。然后,我们比较了Nthy-ori 3-1细胞和FTC-133细胞的黏附及机械信号转导情况。我们证明,DEX破坏了FTC-133细胞中随机定位触发的p38应激信号,从而拮抗了多种生物学功能。因此,DEX处理FTC-133细胞会使其黏附性增加,这主要是由于紧密连接恢复并明显形成了正常数量所致。此外,我们表明,Nthy-ori 3-1细胞和ML-1细胞在随机定位过程中会上调抗黏附蛋白黏蛋白-1,可能是作为对机械应力的一种保护。总之,机械应力似乎是这个转移模型系统中的一个重要组成部分,转移性细胞和健康细胞对其处理方式不同。黏附、抗黏附与细胞间连接之间的平衡决定了在随机定位机器上贴壁的人类细胞是否会脱离,从而使得DEX能够选择性抑制甲状腺体外转移。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eb71/10046141/ea24f4754a36/cancers-15-01641-g001.jpg

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