基底硬度对神经细胞生物学反应影响及其机制的探讨。

ty10086 提交于 周三, 08/25/2021 - 16:31
文章英文标题
Exploration of the Effects of Substrate Stiffness on Biological Responses of Neural Cells and Their Mechanisms.
正文
基质刚度作为一个重要的力学因素,已被证明是生物反应、细胞功能和疾病发生的重要调节因素。然而,基底刚度对神经细胞表型和药物反应的影响仍在很大程度上未知。本研究采用不同刚度的聚二甲基硅氧烷( PDMS )基片建立不同器官组织的力学微环境。我们研究了僵硬度对神经细胞表型的影响,包括细胞活力、细胞周期、细胞骨架结构、细胞僵硬度以及神经细胞对神经退行性疾病( NDD )的休眠和治疗效果的药物反应,结果显示,最大刺激反应范围越大,刺激剂量的宽度越大,生长在与大脑僵硬度相称的软基底上的神经细胞中激素化学物质的最大神经保护活性范围也越高,表明刚性基底上的神经细胞对激素化学物质的休眠和神经保护作用具有抵抗力,对抗6 -羟基多巴胺( 6 - OHDA )诱导的帕金森病( PD )模型。软基上神经细胞对药物反应的敏感性与细胞存活率增加、细胞周期进程加快、肌动蛋白应力纤维增多、局灶性粘连形成、细胞刚度降低有关。通过RNA-Seq和生物信息学分析,证实软基对PC12细胞的促进作用以及激素化学物质对软基的增强激素和神经保护作用是通过上调EGFR / PI3K / AKT信号通路介导的。本研究表明,神经微环境的生物力学性能在体外神经细胞表型和药物反应中发挥重要作用,提示在抗NDD药物设计和治疗中应考虑基底刚度。
文章内容(英文)
Substrate stiffness, as a critical mechanical factor, has been proven to be an important regulator of biological responses, cellular functions, and disease occurrence. However, the effects of substrate stiffness on the phenotypes and drug responses of neural cells remain largely unknown. In this study, polydimethylsiloxane (PDMS) substrates with different stiffnesses were employed to establish the mechanical microenvironment of tissues of different organs. We studied the influences of stiffness on neural cell phenotypes, including cell viability, cell cycle, cytoskeleton structures, cell stiffness, and drug responses of neural cells for hormesis and therapeutic efficacy in neurodegenerative disorders (NDD). The results showed that the greater the range of maximum stimulatory responses, the bigger the width of the stimulatory dosage and the higher the range of maximum neuroprotective activities of hormetic chemicals in neural cells grown on the soft substrate commensurable to the stiffness of the brain, indicating that neural cells on a rigid substrate are resistant to hormetic and neuroprotective effects of hormetic chemicals against 6-hydroxydopamine (6-OHDA)-induced Parkinson's disease (PD) model. The sensitivity of neural cells on the soft substrate to drug response was attributed to the increased cell viability rate, cell cycle progression, actin stress fibers, focal adhesion formation, and decreased cell stiffness. The promoting effect of the soft substrate and the enhanced hormetic and neuroprotective effect of hormetic chemicals on soft substrates in PC12 cells were confirmed to be mediated by the upregulated EGFR/PI3K/AKT signaling pathway by RNA-Seq and bioinformatics analysis. This study demonstrates that the biomechanical properties of the neural microenvironment play important roles in cell phenotypes and drug responses of neural cells in vitro and suggests that substrate stiffness should be considered in the anti-NDD drug design and treatment.
来源出处
Journal|[J]ACS OmegaVolume 5, Issue 48. 2020. PP 31115-31125
DOI
https://doi.org/10.1021/ACSOMEGA.0C04279

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