Microtubule dynamics regulation contributes to endothelial morphogenesis.

Bioarchitecture Pub Date : 2012-11-01 DOI:10.4161/bioa.22335
Karen S Lyle, Jose A Corleto, Torsten Wittmann
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引用次数: 1

Abstract

Because little is known how microtubules contribute to cell migration in a physiological three-dimensional environment, we analyzed microtubule function and dynamics during in vitro angiogenesis in which endothelial cells form networks on a reconstituted basement membrane. Endothelial network formation resulted from distinct cell behaviors: matrix reorganization by myosin-mediated contractile forces, and active cell migration along reorganized, bundled matrix fibers. Inhibition of microtubule dynamics inhibited persistent cell migration, but not matrix reorganization. In addition, microtubule polymerization dynamics and CLASP2-binding to microtubules were spatially regulated to promote microtubule growth into endothelial cell protrusions along matrix tension tracks. We propose that microtubules counter-act contractile forces of the cortical actin cytoskeleton and are required to stabilize endothelial cell protrusions in a soft three-dimensional environment.

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微管动力学调控有助于内皮细胞的形态发生。
由于微管在生理三维环境中如何促进细胞迁移,我们分析了微管在体外血管生成过程中的功能和动力学,其中内皮细胞在重建的基膜上形成网络。内皮网络的形成源于不同的细胞行为:肌球蛋白介导的收缩力介导的基质重组,以及细胞沿着重组的、捆绑的基质纤维的活跃迁移。微管动力学的抑制抑制了持续的细胞迁移,但不抑制基质重组。此外,微管聚合动力学和clasp2与微管的结合在空间上受到调节,从而促进微管沿基质张力轨迹生长为内皮细胞突起。我们提出微管对抗皮层肌动蛋白细胞骨架的收缩力,并且需要在柔软的三维环境中稳定内皮细胞突起。
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Letter from the editors. The impact of tropomyosins on actin filament assembly is isoform specific. Geometric control and modeling of genome reprogramming. Post-polymerization crosstalk between the actin cytoskeleton and microtubule network. Where are the limits of the centrosome?
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