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Dynamic tensile forces drive collective cell migration through three-dimensional extracellular matrices

机译:动态张力通过三维细胞外基质驱动集体细胞迁移

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摘要

Collective cell migration drives tissue remodeling during development, wound repair, and metastatic invasion. The physical mechanisms by which cells move cohesively through dense three-dimensional (3D) extracellular matrix (ECM) remain incompletely understood. Here, we show directly that migration of multicellular cohorts through collagenous matrices occurs via a dynamic pulling mechanism, the nature of which had only been inferred previously in 3D. Tensile forces increase at the invasive front of cohorts, serving a physical, propelling role as well as a regulatory one by conditioning the cells and matrix for further extension. These forces elicit mechanosensitive signaling within the leading edge and align the ECM, creating microtracks conducive to further migration. Moreover, cell movements are highly correlated and in phase with ECM deformations. Migrating cohorts use spatially localized, long-range forces and consequent matrix alignment to navigate through the ECM. These results suggest biophysical forces are critical for 3D collective migration.
机译:集体细胞迁移在发育,伤口修复和转移性侵袭过程中驱动组织重塑。细胞黏性移动通过密集的三维(3D)细胞外基质(ECM)的物理机制仍未完全了解。在这里,我们直接显示了通过胶原蛋白基质通过胶原蛋白基质发生的多细胞队列迁移,该机制的性质此前仅在3D中被推断出来。通过调节细胞和基质以进一步延伸,拉伸力在队列的侵入性前沿增加,从而起到物理,推动作用以及调节作用。这些力在前缘引起机械敏感的信号传导,并使ECM对准,从而形成有助于进一步迁移的微径迹。而且,细胞运动与ECM变形高度相关且同相。迁移队列使用空间局部的远距离作用力和随后的矩阵对齐方式来导航ECM。这些结果表明生物物理力对于3D集体迁移至关重要。

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