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首页> 外文期刊>Scientific reports. >Extracellular Matrix Rigidity-dependent Sphingosine-1-phosphate Secretion Regulates Metastatic Cancer Cell Invasion and Adhesion
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Extracellular Matrix Rigidity-dependent Sphingosine-1-phosphate Secretion Regulates Metastatic Cancer Cell Invasion and Adhesion

机译:细胞外基质刚性依赖性鞘氨酸-1-磷酸盐分泌调节转移性癌细胞侵袭和粘附性

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Dynamic interaction between cancer cells and the surrounding microenvironment is critical for cancer progression via changes in cellular behavior including alteration of secreted molecules. However, the molecular mechanisms underlying the influence exerted by the cancer microenvironment on secretion of molecules during cancer progression remain largely unknown. In this study, we report that secretion of spingsine-1-phosphate (S1P) and its regulator, SphK1 expression is dependent of the substrate rigidity, which is critical for the balance between cancer cell invasion and adhesion. Conditioned media (CM) of MDA-MB-231, an aggressive breast cancer cell obtained from soft substrate (~0.5?kPa) induced chemo-attractive invasion, while CM obtained from stiff substrate (~2.5?kPa) increased cell adhesion instead. We found that the expression of SphK1 is upregulated in the stiff substrate, resulting in an increase in S1P levels in the CM. We also found that upregulation of SphK1 expression in the stiff substrate is dominant in metastatic cancer cells but not in primary cancer cells. These results suggest that alterations in the mechanical environment of the ECM surrounding the tumor cells actively regulate cellular properties such as secretion, which in turn, may contribute to cancer progression.
机译:癌细胞与周围微环境之间的动态相互作用对于癌细胞行为的变化,包括细胞行为的变化对癌症进展至关重要,包括改变分子分子。然而,癌细胞微环境对癌症进展期间分子分泌施加的影响的分子机制仍然很大程度上是未知的。在这项研究中,我们认为Sppings-1-磷酸盐(S1P)及其调节剂的分泌,SPHK1表达依赖于基板刚性,这对于癌细胞侵袭和粘附之间的平衡至关重要。调节介质(CM)MDA-MB-231,一种从软质衬底(〜0.5μkPA)诱导的化学 - 有吸引力的侵袭,而来自刚性底物(〜2.5μKPA)获得的CM,而不是粘附。我们发现SPHK1的表达在硬质基板中上调,导致CM中的S1P水平增加。我们还发现,刚性底物中SPHK1表达的上调在转移性癌细胞中占优势,但不在原发性癌细胞中。这些结果表明,围绕肿瘤细胞周围的ECM的机械环境的改变主动调节细胞性质,例如分泌,这反过来可能有助于癌症进展。

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