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An Early-Stage Atherosclerosis Research Model Based on Microfluidics

机译:基于微流控的早期动脉粥样硬化研究模型

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The arterial microenvironment plays a vital role in the pathology of atherosclerosis (AS). However, the interplay between the arterial microenvironment and atherogenesis remains unclear, partially due to the gap between cell culture and animal experiments. Addressing this problem, the present study reports a microfluidic AS model reconstituting early-stage AS. Physiological or AS-prone hemodynamic conditions are recapitulated on the model. The on-chip model recaptures the atherogenic responses of endothelial cells (ECs) in ways that the Petri dish could not. Significant cytotoxicity of a clinical anti-atherosclerotic drug probucol is discovered on the model, which does not appear on Petri dish but is supported by previous clinical evidence. Moreover, the anti-AS efficiency of platinum-nanoparticles (Pt-NPs) on the model shows excellent consistency with animal experiments. The early-stage AS model shows an excellent connection between Petri dish and animal experiments and highlights its promising role in bridging fundamental AS research, drug screening, and clinical trials.
机译:动脉微环境在动脉粥样硬化(AS)的病理中起着至关重要的作用。然而,动脉微环境与动脉粥样硬化之间的相互作用尚不清楚,部分原因是细胞培养与动物实验之间存在差距。针对此问题,本研究报告了一种重建早期AS的微流控AS模型。在模型上概括了生理或AS易发的血液动力学状况。芯片上模型以皮氏培养皿无法捕获的方式重新捕获了内皮细胞(EC)的动脉粥样硬化反应。在模型中发现了临床抗动脉粥样硬化药物普罗布考的显着细胞毒性,该蛋白未出现在皮氏培养皿中,但已有先前的临床证据支持。此外,铂-纳米颗粒(Pt-NPs)在模型上的抗AS效率与动物实验显示出极好的一致性。早期的AS模型显示出陪替氏培养皿和动物实验之间的良好联系,并突出了其在衔接基础AS研究,药物筛选和临床试验中的有希望的作用。

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