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聚氨酯培养底物可使人神经创伤模型实现长期神经元单培养。

Polyurethane Culture Substrates Enable Long-Term Neuron Monoculture in a Human Model of Neurotrauma.

作者信息

Mitevska Angela, Santacruz Citlally, Martin Eric J, Jones Ian E, Ghiacy Arian, Dixon Simon, Mostafazadeh Nima, Peng Zhangli, Kiskinis Evangelos, Finan John D

机构信息

Department of Biomedical Engineering, University of Illinois at Chicago, Chicago, Illinois, USA.

The Ken & Ruth Davee Department of Neurology, Feinberg School of Medicine, Northwestern University, Chicago, Illinois, USA.

出版信息

Neurotrauma Rep. 2023 Oct 16;4(1):682-692. doi: 10.1089/neur.2023.0060. eCollection 2023.

Abstract

Human induced pluripotent stem cell (hiPSC)-derived cells can reproduce human-specific pathophysiology, patient-specific vulnerability, and gene-environment interactions in neurological disease. Human models of neurotrauma therefore have great potential to advance the field. However, this potential cannot be realized until important biomaterials challenges are addressed. stretch injury models of neurotrauma culture cells on sheets of polydimethylsiloxane (PDMS) that are incompatible with long-term monoculture of hiPSC-derived neurons. Here, we overcame this challenge in an established human neurotrauma model by replacing PDMS with a highly biocompatible form of polyurethane (PU). This substitution allowed long-term monoculture of hiPSC-derived neurons. It also changed the biomechanics of stretch injury. We quantified these changes experimentally using high-speed videography and digital image correlation. We used finite element modeling to quantify the influence of the culture substrate's thickness, stiffness, and coefficient of friction on membrane stretch and concluded that the coefficient of friction explained most of the observed biomechanical changes. Despite these changes, we demonstrated that the modified model produced a robust, dose-dependent trauma phenotype in hiPSC-derived neuron monocultures. In summary, the introduction of this PU film makes it possible to maintain hiPSC-derived neurons in monoculture for long periods in a human neurotrauma model. In doing so, it opens new horizons in the field of neurotrauma by enabling the unique experimental paradigms (e.g., isogenic models) associated with hiPSC-derived neurons.

摘要

人诱导多能干细胞(hiPSC)衍生的细胞能够再现人类特有的病理生理学、患者特有的易损性以及神经疾病中的基因-环境相互作用。因此,人类神经创伤模型在推动该领域发展方面具有巨大潜力。然而,在解决重要的生物材料挑战之前,这种潜力无法实现。神经创伤的拉伸损伤模型在聚二甲基硅氧烷(PDMS)片上培养细胞,而PDMS与hiPSC衍生神经元的长期单培养不相容。在此,我们在一个已建立的人类神经创伤模型中克服了这一挑战,用一种具有高度生物相容性的聚氨酯(PU)形式取代了PDMS。这种替代使得hiPSC衍生神经元能够长期单培养。它还改变了拉伸损伤的生物力学。我们使用高速摄像和数字图像相关技术对这些变化进行了实验量化。我们使用有限元建模来量化培养底物的厚度、刚度和摩擦系数对膜拉伸的影响,并得出结论,摩擦系数解释了观察到的大部分生物力学变化。尽管有这些变化,我们证明改进后的模型在hiPSC衍生神经元单培养物中产生了强大的、剂量依赖性的创伤表型。总之,这种PU膜的引入使得在人类神经创伤模型中能够长期维持hiPSC衍生神经元的单培养。这样做,它通过启用与hiPSC衍生神经元相关的独特实验范式(如同基因模型),为神经创伤领域开辟了新的视野。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6d6c/10615064/a88c24c7eb9d/neur.2023.0060_figure1.jpg

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