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HAX1 impact on collective cell migration, cell adhesion, and cell shape is linked to the regulation of actomyosin contractility

机译:hax1对集体细胞迁移,细胞粘附和细胞形状的影响与actomyosin收缩性的调节有关

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摘要

HAX1 protein is involved in the regulation of apoptosis, cell motility and calcium homeostasis. Its overexpression was reported in several tumors, including breast cancer. This study demonstrates that HAX1 has an impact on collective, but not single-cell migration, thus indicating the importance of cell-cell contacts for the HAX1-mediated effect. Accordingly, it was shown that HAX1 knockdown affects cell-cell junctions, substrate adhesion, and epithelial cell layer integrity. As demonstrated here, these effects can be attributed to the modulation of actomyosin contractility through changes in RhoA and septin signaling. Additionally, it was shown that HAX1 does not influence invasive potential in the breast cancer cell line, suggesting that its role in breast cancer progression may be linked instead to collective invasion of the epithelial cells but not single-cell dissemination.
机译:HAX1蛋白参与细胞凋亡,细胞运动和钙稳态的调节。 其过度表达在几种肿瘤中报告,包括乳腺癌。 本研究表明,Hax1对集体影响而不是单细胞迁移,因此表明细胞 - 细胞接触对HAX1介导的效果的重要性。 因此,显示HAX1敲低影响细胞 - 细胞结,底物粘附和上皮细胞层完整性。 如这里所示,这些效果可以归因于通过RhoA和静止信号传导的变化来调节Actomyosin收缩性。 另外,表明HAX1不会影响乳腺癌细胞中的侵袭性潜力,表明其在乳腺癌进展中的作用可以连接到上皮细胞的集体侵袭,但不是单细胞传播。

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