Studying the Synergistic Effect of Substrate Stiffness and Cyclic Stretch Level on Endothelial Cells Using an Elastomeric Cell Culture Chamber

内皮干细胞 刚度 材料科学 生物物理学 细胞骨架 弹性(物理) 基质(水族馆) 内皮 纤维连接蛋白 组织工程 细胞 解剖 生物医学工程 化学 体外 复合材料 生物 生物化学 医学 内科学 生态学
作者
Nadia Chandra Sekar,Sergio Aguilera Suarez,Ngan Nguyen,Austin Lai,Peter Thurgood,Ying Zhou,Chanly Chheang,Scott Needham,Elena Pirogova,Karlheinz Peter,Khashayar Khoshmanesh,Sara Baratchi
出处
期刊:ACS Applied Materials & Interfaces [American Chemical Society]
卷期号:15 (4): 4863-4872 被引量:6
标识
DOI:10.1021/acsami.2c15818
摘要

Endothelial cells lining blood vessels are continuously exposed to biophysical cues that regulate their function in health and disease. As we age, blood vessels lose their elasticity and become stiffer. Vessel stiffness alters the mechanical forces that endothelial cells experience. Despite ample evidence on the contribution of endothelial cells to vessel stiffness, less is known about how vessel stiffness affects endothelial cells. In this study, we developed a versatile model to study the cooperative effect of substrate stiffness and cyclic stretch on human aortic endothelial cells. We cultured endothelial cells on elastomeric wells covered with fibronectin-coated polyacrylamide gel. Varying the concentrations of acrylamide and bis-acrylamide enabled us to produce soft and stiff substrates with elastic modules of 40 and 200 kPa, respectively. Using a customized three-dimensional (3D) printed cam-driven system, the cells were exposed to 5 and 10% cyclic stretch levels. This enabled us to mimic the stiffness and stretch levels that endothelial cells experience in young and aged arteries. Using this model, we found that endothelial cells cultured on a soft substrate had minimal cytoskeletal alignment to the direction of the stretch compared to the ones cultured on the stiff substrate. We also observed an increase in the cellular area and aspect ratio in cells cultured on the stiff substrate, both of which are positively regulated by cyclic stretch. However, neither cyclic stretch nor substrate stiffness significantly affected the nuclear circularity. Additionally, we found that the accumulation of NF-κB in the nucleus, endothelial proliferation, tube formation, and expression of IL1β depends on the stretch level and substrate stiffness. Our model can be further used to investigate the complex signaling pathways associated with vessel stiffening that govern the endothelial responses to mechanical forces.
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