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Quantitative analysis of 3D extracellular matrix remodelling by pancreatic stellate cells

机译:胰腺星状细胞对3D细胞外基质重塑的定量分析

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Extracellular matrix (ECM) remodelling is integral to numerous physiological and pathological processes in biology, such as embryogenesis, wound healing, fibrosis and cancer. Until recently, most cellular studies have been conducted on 2D environments where mechanical cues significantly differ from physiologically relevant 3D environments, impacting cellular behaviour and masking the interpretation of cellular function in health and disease. We present an integrated methodology where cell-ECM interactions can be investigated in 3D environments via ECM remodelling. Monitoring and quantification of collagen-I structure in remodelled matrices, through designated algorithms, show that 3D matrices can be used to correlate remodelling with increased ECM stiffness observed in fibrosis. Pancreatic stellate cells (PSCs) are the key effectors of the stromal fibrosis associated to pancreatic cancer. We use PSCs to implement our methodology and demonstrate that PSC matrix remodelling capabilities depend on their contractile machinery and β1 integrin-mediated cell-ECM attachment.
机译:细胞外基质(ECM)重塑是生物学中众多生理和病理过程(如胚胎发生,伤口愈合,纤维化和癌症)不可或缺的部分。直到最近,大多数细胞研究都是在机械提示与生理相关3D环境明显不同的2D环境中进行的,这影响了细胞行为并掩盖了健康和疾病中细胞功能的解释。我们提出了一种集成的方法,其中可以通过ECM重塑在3D环境中研究细胞-ECM相互作用。通过指定的算法对重构基质中的胶原蛋白I结构进行监测和定量,结果表明3D基质可用于将重构与纤维化中观察到的ECM硬度增加相关联。胰腺星状细胞(PSC)是与胰腺癌相关的基质纤维化的关键效应物。我们使用PSC来实施我们的方法,并证明PSC基质的重塑能力取决于其收缩机制和β1整合素介导的细胞ECM附着。

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