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侵袭性阿米巴样肉瘤细胞的转移依赖于 Rho/ROCK/MLC 信号通路。

Metastasis of aggressive amoeboid sarcoma cells is dependent on Rho/ROCK/MLC signaling.

机构信息

Department of Cell Biology, Faculty of Science, Charles University in Prague, Viničná 7, 12843 Prague 2, Czech Republic.

出版信息

Cell Commun Signal. 2013 Jul 30;11:51. doi: 10.1186/1478-811X-11-51.

Abstract

BACKGROUND

Although there is extensive evidence for the amoeboid invasiveness of cancer cells in vitro, much less is known about the role of amoeboid invasiveness in metastasis and the importance of Rho/ROCK/MLC signaling in this process.

RESULTS

We analyzed the dependence of amoeboid invasiveness of rat and chicken sarcoma cells and the metastatic activity of chicken cells on individual elements of the Rho/ROCK/MLC pathway. In both animal models, inhibition of Rho, ROCK or MLC resulted in greatly decreased cell invasiveness in vitro, while inhibition of extracellular proteases using a broad spectrum inhibitor did not have a significant effect. The inhibition of both Rho activity and MLC phosphorylation by dominant negative mutants led to a decreased capability of chicken sarcoma cells to metastasize. Moreover, the overexpression of RhoA in non-metastatic chicken cells resulted in the rescue of both invasiveness and metastatic capability. Rho and ROCK, unlike MLC, appeared to be directly involved in the maintenance of the amoeboid phenotype, as their inhibition resulted in the amoeboid-mesenchymal transition in analyzed cell lines.

CONCLUSION

Taken together, these results suggest that protease-independent invasion controlled by elements of the Rho/ROCK/MLC pathway can be frequently exploited by metastatic sarcoma cells.

摘要

背景

尽管有大量证据表明癌细胞在体外具有变形虫样侵袭性,但对于变形虫样侵袭性在转移中的作用以及 Rho/ROCK/MLC 信号通路在这一过程中的重要性知之甚少。

结果

我们分析了大鼠和鸡肉瘤细胞的变形虫样侵袭性和鸡细胞的转移活性对 Rho/ROCK/MLC 通路各个元件的依赖性。在这两种动物模型中,抑制 Rho、ROCK 或 MLC 导致细胞体外侵袭性大大降低,而使用广谱抑制剂抑制细胞外蛋白酶则没有显著效果。显性负突变体抑制 Rho 活性和 MLC 磷酸化导致鸡肉瘤细胞转移能力降低。此外,在非转移性鸡细胞中过表达 RhoA 导致侵袭性和转移能力的恢复。与 MLC 不同,Rho 和 ROCK 似乎直接参与维持变形虫样表型,因为它们的抑制导致分析细胞系中的变形虫样-间充质转化。

结论

综上所述,这些结果表明,由 Rho/ROCK/MLC 通路元件控制的非依赖蛋白酶的侵袭可能经常被转移性肉瘤细胞利用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ad8/3735423/78b1d23067f3/1478-811X-11-51-1.jpg

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