基于生物打印水凝胶张力的非破坏性宏观测量的细胞收缩行为的量化。

S. Pragnère, Naima El Kholti, Leslie Gudimard, Lucie Essayan, C. Marquette, E. Petiot, C. Pailler-Mattéi
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引用次数: 3

摘要

基于表面测量的收缩测定法已被广泛用于评估3D模型中的细胞收缩性。这种方法很简单,不需要特定的设备,但它不能提供关于细胞产生的收缩力的定量数据。我们基于功能定理,用一个新的生物力学模型扩展了这种方法,以提供三维细胞产生的收缩力的无损纵向监测。我们将这种方法应用于接种有成纤维细胞或成骨细胞的水凝胶。调节水凝胶力学特性以增强(条件HCAHigh:水凝胶收缩测定-高收缩)或限制(条件HCALow:水凝胶收缩试验-低收缩)细胞收缩行为。宏观测量与细胞收缩行为以及对不同机械环境下细胞生理学的描述性分析进一步相关。成纤维细胞和成骨细胞的基质收缩率分别高达47%和77%。收缩应力在第5天达到峰值,成纤维细胞为1.1 10-14 Pa,成骨细胞为3.5 10-14 Pa。这与细胞附着和扩散有关。HCALow出现可忽略的收缩。成纤维细胞和成骨细胞在HCAHigh和HCALow中均表达α-SMA收缩纤维。HCALow的收缩失败归因于水凝胶的交联增加和对蛋白水解降解的抵抗力。
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Quantification of cell contractile behavior based on non-destructive macroscopic measurement of tension forces on bioprinted hydrogel.
Contraction assay based on surface measurement have been widely used to evaluate cell contractility in 3D models. This method is straightforward and requires no specific equipment, but it does not provide quantitative data about contraction forces generated by cells. We expanded this method with a new biomechanical model, based on the work-energy theorem, to provide non-destructive longitudinal monitoring of contraction forces generated by cells in 3D. We applied this method on hydrogels seeded with either fibroblasts or osteoblasts. Hydrogel mechanical characteristics were modulated to enhance (condition HCAHigh: hydrogel contraction assay high contraction) or limit (condition HCALow: hydrogel contraction assay low contraction) cell contractile behaviors. Macroscopic measures were further correlated with cell contractile behavior and descriptive analysis of their physiology in response to different mechanical environments. Fibroblasts and osteoblasts contracted their matrix up to 47% and 77% respectively. Contraction stress peaked at day 5 with 1.1 10-14 Pa for fibroblasts and 3.5 10-14 Pa for osteoblasts, which correlated with cell attachment and spreading. Negligible contraction was seen in HCALow. Both fibroblasts and osteoblasts expressed α-SMA contractile fibers in HCAHigh and HCALow. Failure to contract HCALow was attributed to increased cross-linking and resistance to proteolytic degradation of the hydrogel.
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