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首页> 外文期刊>Cellular and Molecular Bioengineering >Substrates with Engineered Step Changes in Rigidity Induce Traction Force Polarity and Durotaxis
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Substrates with Engineered Step Changes in Rigidity Induce Traction Force Polarity and Durotaxis

机译:刚性变化具有工程阶跃的基板会导致牵引力极性和Durotaxis

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Rigidity sensing plays a fundamental role in multiple cell functions ranging from migration, to proliferation and differentiation (Engler et al., Cell 126:677-689, 2006; Lo et al., Biophys. J. 79:144-152, 2000; Wells, Hepatology 47:1394-1400, 2008; Zoldan et al., Biomaterials 32:9612-9621, 2011). During migration, single cells have been reported to preferentially move toward more rigid regions of a substrate in a process termed durotaxis. Durotaxis could contribute to cell migration in wound healing and gastrulation, where local gradients in tissue rigidity have been described. Despite the potential importance of this phenomenon to physiology and disease, it remains unclear how rigidity guides these behaviors and the underlying cellular and molecular mechanisms. To investigate the functional role of subcellular distribution and dynamics of cellular traction forces during durotaxis, we developed a unique microfabrication strategy to generate elastomeric micropost arrays patterned with regions exhibiting two different rigidities juxtaposed next to each other. After initial cell attachment on the rigidity boundary of the micropost array, NIH 3T3 fibroblasts were observed to preferentially migrate toward the rigid region of the micropost array, indicative of durotaxis. Additionally, cells bridging two rigidities across the rigidity boundary on the micropost array developed stronger traction forces on the more rigid side of the substrate indistinguishable from forces generated by cells exclusively seeded on rigid regions of the micropost array. Together, our results highlighted the utility of step-rigidity micropost arrays to investigate the functional role of traction forces in rigidity sensing and durotaxis, suggesting that cells could sense substrate rigidity locally to induce an asymmetrical intracellular traction force distribution to contribute to durotaxis.
机译:刚性感测在从迁移到增殖和分化的多种细胞功能中起着基本作用(Engler等人,Cell 126:677-689,2006; Lo等人,Biophys.J.79:144-152,2000;等。 Wells,Hepatology 47:1394-1400,2008; Zoldan等人,Biomaterials 32:9612-9621,2011)。在迁移过程中,据报道单个细胞在称为durotaxis的过程中优先向基材的刚性区域移动。 Durotaxis可能有助于伤口愈合和胃形成中的细胞迁移,在此已经描述了组织刚度的局部梯度。尽管该现象对生理学和疾病具有潜在的重要性,但仍不清楚刚性如何指导这些行为以及潜在的细胞和分子机制。为了研究durotaxis期间亚细胞分布的功能性作用和细胞牵引力的动态变化,我们开发了一种独特的微细加工策略,以生成具有图案的弹性体微柱阵列,该阵列具有两个彼此并列的不同刚度的区域。在微柱阵列的刚度边界上初始细胞附着后,观察到NIH 3T3成纤维细胞优先向微柱阵列的刚性区域迁移,这表明存在durotaxis。另外,在微柱阵列上跨过刚性边界的两个刚度的单元在基板的更刚性侧上产生了更强的牵引力,该牵引力与仅在微柱阵列的刚性区域上播种的单元所产生的力没有区别。在一起,我们的研究结果突出了步进刚度微柱阵列的实用性,以研究牵引力在刚度感测和durotaxis中的功能作用,表明细胞可以局部感测基质刚度,从而诱导不对称的细胞内牵引力分布,从而有助于durotaxis。

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