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Microfluidic Cardiac Cell Culture Model ((mu)CCCM)

机译:微流控心肌细胞培养模型(μCCCM)

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Physiological heart development and cardiac function rely on the response of cardiac cells to mechanical stress during hemodynamic loading and unloading. These stresses, especially if sustained, can induce changes in cell structure, contractile function, and gene expression. Current cell culture techniques commonly fail to adequately replicate physical loading observed in the native heart. Therefore, there is a need for physiologically relevant in vitro models that recreate mechanical loading conditions seen in both normal and pathological conditions. To fulfill this need, we have developed a microfluidic cardiac cell culture model ((mu)CCCM) that for the first time allows in vitro hemodynamic stimulation of cardiomyocytes by directly coupling cell structure and function with fluid induced loading. Cells are cultured in a small (1 cm diameter) cell culture chamber on a thin flexible silicone membrane. Integrating the cell culture chamber with a pump, collapsible pulsatile valve and an adjustable resistance element (hemostatic valve) in series allow replication of various loading conditions experienced in the heart. This paper details the design, modeling, fabrication and characterization of fluid flow, pressure and stretch generated at various frequencies to mimic hemodynamic conditions associated with the normal and failing heart. Proof-of-concept studies demonstrate successful culture of an embryonic cardiomyoblast line (H9c2 cells) and establishment of an in vivo like phenotype within this system.
机译:生理心脏的发育和心脏功能依赖于血液动力学加载和卸载过程中心肌细胞对机械应力的反应。这些压力,尤其是持续存在的压力,可以诱导细胞结构,收缩功能和基因表达的变化。当前的细胞培养技术通常不能充分复制在天然心脏中观察到的物理负荷。因此,需要在生理上和生理上相关的体外模型,以重现在正常和病理条件下均可见的机械负荷条件。为了满足这一需求,我们开发了一种微流控心肌细胞培养模型(μCCCM),该模型首次通过将细胞的结构和功能与液体诱导的负荷直接结合,允许体外对心肌细胞进行血液动力学刺激。细胞在薄的柔性有机硅膜上的小(1厘米直径)细胞培养室中培养。将细胞培养室与泵,可折叠脉动阀和可调电阻元件(止血阀)串联集成在一起,可以复制心脏中经历的各种负荷条件。本文详细介绍了在各种频率下产生的流体流动,压力和拉伸的设计,建模,制造和特性,以模拟与正常心脏和衰竭心脏相关的血液动力学状况。概念验证研究表明,成功培养了胚胎心肌母细胞系(H9c2细胞),并在该系统内建立了类似体内的表型。

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