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三维呼吸式肺芯片中纳米颗粒的动力学

Dynamics of nanoparticles in a 3D breathing lung-on-a-chip.

作者信息

Sheidaei Zohreh, Akbarzadeh Pooria, Kashaninejad Navid

机构信息

Faculty of Mechanical Engineering, Shahrood University of Technology, Shahrood, Iran.

Environmental Engineering Institute, School of Architecture, Civil and Environmental Engineering, Ecole Polytechnique Fédérale de Lausanne (EPFL), 1015, Lausanne, Switzerland.

出版信息

Drug Deliv Transl Res. 2025 Apr 16. doi: 10.1007/s13346-025-01853-5.

Abstract

The"Breathing Lung-on-a-Chip,"a novel microfluidic device featuring a stretchable membrane, replicates the natural expansion and contraction of the human lung. It provides a more realistic in-vitro platform to study respiratory diseases, particle deposition, and drug delivery mechanisms. This device enables investigations into the effects of inhaled nanoparticles (NPs) on lung tissue and supports the development of advanced inhalation therapies. Uniform and optimal concentration delivery of NPs to cultured cells within the chip is critical, particularly as membrane stretching significantly influences particle dynamics. To address this, we developed a 3D numerical model that accurately simulates NP behavior under dynamic conditions, overcoming experimental limitations. The model, validated against experimental data, explores the effects of flow dynamics, particle size, membrane porosity, and stretching frequency/intensity on NP deposition in the air channel and transfer through the porous membrane into the medium channel. The results indicate that increased membrane stretch enhances the sedimentation rate of NPs in the air channel, thereby promoting their transfer to the medium channel, particularly in membranes with initially low porosity. Additionally, excessive stretching frequencies or intensities can introduce reverse flow and stagnation, leading to a longer residence time for NPs and altering their sedimentation patterns. These insights advance our understanding of NP transport in dynamic lung environments, paving the way for more effective applications of lung-on-a-chip technology in toxicological assessments and respiratory therapy innovations.

摘要

“呼吸肺芯片”是一种具有可拉伸膜的新型微流控装置,可复制人类肺部的自然扩张和收缩。它为研究呼吸系统疾病、颗粒沉积和药物输送机制提供了一个更逼真的体外平台。该装置能够研究吸入纳米颗粒(NP)对肺组织的影响,并支持先进吸入疗法的开发。将NP均匀且最佳浓度地输送到芯片内的培养细胞至关重要,尤其是因为膜的拉伸会显著影响颗粒动力学。为了解决这个问题,我们开发了一个三维数值模型,该模型能准确模拟动态条件下NP的行为,克服了实验限制。该模型经实验数据验证,探索了流动动力学、颗粒大小、膜孔隙率以及拉伸频率/强度对NP在空气通道中的沉积以及通过多孔膜转移到介质通道的影响。结果表明,增加膜的拉伸会提高NP在空气通道中的沉降速率,从而促进它们转移到介质通道,特别是在初始孔隙率较低的膜中。此外,过高的拉伸频率或强度会引入逆流和停滞,导致NP的停留时间延长并改变其沉降模式。这些见解增进了我们对动态肺部环境中NP传输的理解,为肺芯片技术在毒理学评估和呼吸治疗创新中的更有效应用铺平了道路。

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