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Identification of topographical architectures supporting the phenotype of rat tenocytes

机译:识别支持大鼠胞胎型表型的地形架构

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摘要

Tenocytes, the main cell type of the tendon, require mechanical stimuli for their proper function. When the tenocyte environment changes due to tissue damage or by transferring tenocytes from their native environment into cell culture, the signals from the tenocyte niche are lost, leading towards a decline of phenotypic markers. It is known that micro-topographies can influence cell fate by the physical cues they provide. To identify the optimal topography-induced biomechanical niche in vitro, we seeded tenocytes on the TopoChip, a micro-topographical screening platform, and measured expression of the tendon transcription factor Scleraxis. Through machine learning algorithms, we associated elevated Scleraxis levels with topological design parameters. Fabricating micro-topographies with optimal surface characteristics on larger surfaces allowed finding an improved expression of multiple tenogenic markers. However, long-term confluent culture conditions coincided with osteogenic marker expression and the loss of morphological characteristics. In contrast, passaging tenocytes which migrated from the tendon directly on the topography resulted in prolonged elongated morphology and elevated Scleraxis levels. This research provides new insights into how micro-topographies influence tenocyte cell fate, and supports the notion that micro-topographical design can be implemented in a new generation of tissue culture platforms for supporting the phenotype of tenocytes. (C) 2018 Published by Elsevier Ltd on behalf of Acta Materialia Inc.
机译:腱鞘是肌腱的主要细胞类型,需要机械刺激适当的功能。当Tenocyte环境因组织损伤或将腱梗转移到细胞培养物中而变化时,来自腱尾e的信号丢失,导致表型标志物的下降。已知微观图形可以通过它们提供的物理提示影响细胞命运。为了在体外鉴定最佳地形诱导的生物力学性质,我们将替氏素,微地形筛查平台和肌腱转录因子稀释物的测量表达播种。通过机器学习算法,我们与拓扑设计参数相关联升高的危险液。在较大的表面上具有最佳表面特性的微观形状,允许发现多种遗传标记的改善表达。然而,长期汇合培养条件与成骨标志物表达吻合和形态特征的丧失。相反,直接从肌腱迁移到地形上的传代胞胎导致延长细长的形态和升高的患者水平。本研究提供了新的见解如何影响腱鞘细胞命运,并支持微地形设计可以在新一代组织培养平台中实现的观念,以支持胞胎细胞的表型。 (c)2018年由elsevier有限公司发布代表Acta Materialia Inc.

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