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细胞牵引场驱动的模式形成和体外管状发生的关键条件。

Critical conditions for pattern formation and in vitro tubulogenesis driven by cellular traction fields.

作者信息

Namy Patrick, Ohayon Jacques, Tracqui Philippe

机构信息

Equipe Dynacell, Laboratoire TIMC-IMAG, CNRS UMR 5525, Institut de l'Ingénierie et de l'Information de Santé (In3s), F-38706 La Tronche cedex, France.

出版信息

J Theor Biol. 2004 Mar 7;227(1):103-20. doi: 10.1016/j.jtbi.2003.10.015.

Abstract

In vitro angiogenesis assays have shown that tubulogenesis of endothelial cells within biogels, like collagen or fibrin gels, only appears for a critical range of experimental parameter values. These experiments have enabled us to develop and validate a theoretical model in which mechanical interactions of endothelial cells with extracellular matrix influence both active cell migration--haptotaxis--and cellular traction forces. Depending on the number of cells, cell motility and biogel rheological properties, various 2D endothelial patterns can be generated, from non-connected stripe patterns to fully connected networks, which mimic the spatial organization of capillary structures. The model quantitatively and qualitatively reproduces the range of critical values of cell densities and fibrin concentrations for which these cell networks are experimentally observed. We illustrate how cell motility is associated to the self-enhancement of the local traction fields exerted within the biogel in order to produce a pre-patterning of this matrix and subsequent formation of tubular structures, above critical thresholds corresponding to bifurcation points of the mathematical model. The dynamics of this morphogenetic process is discussed in the light of videomicroscopy time lapse sequences of endothelial cells (EAhy926 line) in fibrin gels. Our modeling approach also explains how the progressive appearance and morphology of the cellular networks are modified by gradients of extracellular matrix thickness.

摘要

体外血管生成实验表明,在内凝胶(如胶原蛋白或纤维蛋白凝胶)中,内皮细胞的管状形成仅在实验参数值的关键范围内出现。这些实验使我们能够开发并验证一个理论模型,其中内皮细胞与细胞外基质的机械相互作用会影响细胞的主动迁移——趋触性——以及细胞牵引力。根据细胞数量、细胞运动性和生物凝胶的流变特性,可以生成各种二维内皮模式,从非连接的条纹模式到完全连接的网络,这些模式模拟了毛细血管结构的空间组织。该模型定量和定性地再现了实验观察到这些细胞网络的细胞密度和纤维蛋白浓度的临界值范围。我们说明了细胞运动性如何与生物凝胶内局部牵引力场的自我增强相关联,以便在高于对应于数学模型分岔点的临界阈值时,对该基质进行预图案化并随后形成管状结构。根据纤维蛋白凝胶中内皮细胞(EAhy926系)的视频显微镜延时序列,讨论了这种形态发生过程的动力学。我们的建模方法还解释了细胞网络的逐渐出现和形态如何受到细胞外基质厚度梯度的影响。

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