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Mapping the structure and biological functions within mesenchymal bodies using microfluidics

机译:使用微流体测绘间充质体内的结构和生物学功能

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Organoids that recapitulate the functional hallmarks of anatomic structures comprise cell populations able to self-organize cohesively in 3D. However, the rules underlying organoid formation in vitro remain poorly understood because a correlative analysis of individual cell fate and spatial organization has been challenging. Here, we use a novel microfluidics platform to investigate the mechanisms determining the formation of organoids by human mesenchymal stromal cells that recapitulate the early steps of condensation initiating bone repair in vivo. We find that heterogeneous mesenchymal stromal cells self-organize in 3D in a developmentally hierarchical manner. We demonstrate a link between structural organization and local regulation of specific molecular signaling pathways such as NF-κB and actin polymerization, which modulate osteo-endocrine functions. This study emphasizes the importance of resolving spatial heterogeneities within cellular aggregates to link organization and functional properties, enabling a better understanding of the mechanisms controlling organoid formation, relevant to organogenesis and tissue repair.
机译:重组解剖结构的功能标志的有机体包含能够在3D中自制卷入的细胞群。然而,体外有机体形成的规则仍然明确地理解,因为个体细胞命运和空间组织的相关性分析一直在具有挑战性。在这里,我们使用新的微流体平台来研究通过人间充质基质细胞确定有机体的形成的机制,该机制重新制备了在体内引发骨修复的缩合的早期步骤。我们发现异质间充质基质细胞以发育等级方式在3D中自组织。我们展示了结构组织和局部调节的特定分子信号传导途径(如NF-κB和肌动蛋白聚合)之间的联系,其调节骨内分泌功能。该研究强调了解决细胞聚集体内的空间异质性以链接组织和功能性质的重要性,使得能够更好地理解控制有机体形成的机制,与组织发生和组织修复相关。

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