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核-细胞骨架偶联在细胞拉伸过程中控制细胞内变形分配。

Nucleo-cytoskeletal coupling controls intracellular deformation partitioning during cell stretching.

作者信息

Chen Jerry, Sloan Iris, Bermudez Alexandra, Choi David, Tsai Ming-Heng, Jin Lihua, Hu Jimmy K, Lin Neil

机构信息

University of California Los Angeles, Los Angeles, CA, USA.

出版信息

R Soc Open Sci. 2025 Jul 30;12(7):250409. doi: 10.1098/rsos.250409. eCollection 2025 Jul.

Abstract

Cells sense and transduce mechanical forces to regulate diverse biological processes, yet the mechanical stimuli that initiate these processes remain poorly understood. In particular, how nuclear and cytoplasmic deformations respond to external forces is unclear. Here, we developed a microscopy-based technique to quantify the extensional uniaxial strains of the nucleus and cytoplasm during cell stretching, enabling direct measurement of their bulk mechanical responses. Using this approach, we identified a previously unrecognized inverse relationship between nuclear and cytoplasmic deformation in epithelial monolayers. We demonstrate that nucleo-cytoskeletal coupling, mediated by the Linker of Nucleoskeleton and Cytoskeleton (LINC) complex, regulates this anti-correlation (Pearson correlation coefficient approx. 0.3). Disrupting LINC abolished this relationship, revealing its fundamental role in intracellular deformation partitioning. Furthermore, we found that cytoplasmic deformation is directly correlated with stretch-induced nuclear shrinkage, suggesting a mechanotransduction pathway in which cytoplasmic mechanics influence nuclear responses. Lastly, multivariable analyses established that intracellular deformation can be inferred from cell morphology, providing a predictive framework for cellular mechanical behaviour. These findings refine our understanding of nucleo-cytoskeletal coupling in governing intracellular force transmission and mechanotransduction.

摘要

细胞感知并传导机械力以调节多种生物学过程,然而启动这些过程的机械刺激仍知之甚少。特别是,细胞核和细胞质变形如何响应外力尚不清楚。在此,我们开发了一种基于显微镜的技术,用于量化细胞拉伸过程中细胞核和细胞质的单轴拉伸应变,从而能够直接测量它们的整体力学响应。使用这种方法,我们在单层上皮细胞中发现了细胞核和细胞质变形之间以前未被认识到的反比关系。我们证明,由核骨架与细胞骨架连接体(LINC)复合物介导的核 - 细胞骨架偶联调节这种反相关关系(皮尔逊相关系数约为0.3)。破坏LINC消除了这种关系,揭示了其在细胞内变形分配中的基本作用。此外,我们发现细胞质变形与拉伸诱导的核收缩直接相关,这表明存在一种机械转导途径,其中细胞质力学影响核反应。最后,多变量分析表明,可以从细胞形态推断细胞内变形,为细胞力学行为提供了一个预测框架。这些发现深化了我们对核 - 细胞骨架偶联在控制细胞内力传递和机械转导方面的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a54/12308074/417961000caf/rsos.250409.f001.jpg

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