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首页> 外文期刊>Molecular biology of the cell >Cells activated for wound repair have the potential to direct collective invasion of an epithelium
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Cells activated for wound repair have the potential to direct collective invasion of an epithelium

机译:被激活用于伤口修复的细胞有可能指导上皮的集体侵袭

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摘要

Mechanisms regulating how groups of cells are signaled to move collectively from their original site and invade surrounding matrix are poorly understood. Here we develop a clinically relevant ex vivo injury invasion model to determine whether cells involved in directing wound healing have invasive function and whether they can act as leader cells to direct movement of a wounded epithelium through a three-dimensional (3D) extracellular matrix (ECM) environment. Similar to cancer invasion, we found that the injured cells invade into the ECM as cords, involving heterotypical cell–cell interactions. Mesenchymal cells with properties of activated repair cells that typically locate to a wound edge are present in leader positions at the front of ZO-1–rich invading cords of cells, where they extend vimentin intermediate filament–enriched protrusions into the 3D ECM. Injury-induced invasion depends on both vimentin cytoskeletal function and MMP-2/9 matrix remodeling, because inhibiting either of these suppressed invasion. Potential push and pull forces at the tips of the invading cords were revealed by time-lapse imaging, which showed cells actively extending and retracting protrusions into the ECM. This 3D injury invasion model can be used to investigate mechanisms of leader cell–directed invasion and understand how mechanisms of wound healing are hijacked to cause disease.
机译:人们尚不清楚调节细胞群信号如何从其原始部位集体移动并侵入周围基质的机制。在这里,我们开发临床相关的离体损伤侵袭模型,以确定参与指导伤口愈合的细胞是否具有侵袭功能,以及它们是否可以充当引导细胞通过三维(3D)细胞外基质(ECM)引导受伤上皮的运动) 环境。与癌症侵袭类似,我们发现受损细胞以绳索的形式侵入ECM,涉及异型细胞间相互作用。具有活化修复细胞特性的间充质细胞通常位于伤口边缘,位于富含ZO-1的侵入细胞前部的前导位置,在那里它们将波形蛋白中间丝富集的突起延伸到3D ECM中。损伤诱导的侵袭取决于波形蛋白的细胞骨架功能和MMP-2 / 9基质重塑,因为抑制了这些抑制的侵袭之一。延时成像显示了在侵犯的脐带末端的潜在推拉力,这表明细胞活跃地向ECM伸出和缩回突起。该3D损伤入侵模型可用于研究前导细胞定向侵袭的机制,并了解如何劫持伤口愈合的机制以引起疾病。

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