板层
刚度
纳米尺度
细胞迁移
癌症转移
纳米技术
GSM演进的增强数据速率
生物系统
前沿
模式(计算机接口)
原子力显微镜
动力学(音乐)
计算机科学
光学
材料科学
细胞
物理
癌细胞
生物
计算机视觉
机械
声学
癌症
人机交互
复合材料
遗传学
作者
Guillaume Lamour,Michel Malo,Raphaël Crépin,Juan Pelta,S. Labdi,Clément Campillo
标识
DOI:10.1021/acsbiomaterials.3c01254
摘要
Cell migration profoundly influences cellular function, often resulting in adverse effects in various pathologies including cancer metastasis. Directly assessing and quantifying the nanoscale dynamics of living cell structure and mechanics has remained a challenge. At the forefront of cell movement, the flat actin modules─the lamellipodium and the lamellum─interact to propel cell migration. The lamellipodium extends from the lamellum and undergoes rapid changes within seconds, making measurement of its stiffness a persistent hurdle. In this study, we introduce the fast-quantitative imaging (fast-QI) mode, demonstrating its capability to simultaneously map both the lamellipodium and the lamellum with enhanced spatiotemporal resolution compared with the classic quantitative imaging (QI) mode. Specifically, our findings reveal nanoscale stiffness gradients in the lamellipodium at the leading edge, where it appears to be slightly thinner and significantly softer than the lamellum. Additionally, we illustrate the fast-QI mode's accuracy in generating maps of height and effective stiffness through a streamlined and efficient processing of force–distance curves. These results underscore the potential of the fast-QI mode for investigating the role of motile cell structures in mechanosensing.
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