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小鼠肺类器官对减少、增加和循环拉伸的反应。

Mouse lung organoid responses to reduced, increased, and cyclic stretch.

机构信息

Critical Care Medicine, Cincinnati Children's Hospital Medical Center, Cincinnati, Ohio.

Biomedical Engineering, Cincinnati Children's Hospital Medical Center, Cincinnati, Ohio.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2022 Jan 1;322(1):L162-L173. doi: 10.1152/ajplung.00310.2020. Epub 2021 Dec 1.

Abstract

Most lung development occurs in the context of cyclic stretch. Alteration of the mechanical microenvironment is a common feature of many pulmonary diseases, with congenital diaphragmatic hernia (CDH) and fetal tracheal occlusion (FETO, a therapy for CDH) being extreme examples with changes in lung structure, cell differentiation, and function. To address limitations in cell culture and in vivo mechanotransductive models, we developed two mouse lung organoid (mLO) mechanotransductive models using (PND5) mouse lung CD326-positive cells and fibroblasts subjected to increased, decreased, and cyclic strain. In the first model, mLOs were exposed to forskolin (FSK) and/or disrupted (DIS) and evaluated at 20 h. mLO cross-sectional area changed by +59%, +24%, and -68% in FSK, control, and DIS mLOs, respectively. FSK-treated organoids had twice as many proliferating cells as other organoids. In the second model, 20 h of 10.25% biaxial cyclic strain increased the mRNAs of lung mesenchymal cell lineages compared with static stretch and no stretch. Cyclic stretch increased TGF-β and integrin-mediated signaling, with upstream analysis indicating roles for histone deacetylases, microRNAs, and long noncoding RNAs. Cyclic stretch mLOs increased αSMA-positive and αSMA-PDGFRα-double-positive cells compared with no stretch and static stretch mLOs. In this PND5 mLO mechanotransductive model, cell proliferation is increased by static stretch, and cyclic stretch induces mesenchymal gene expression changes important in postnatal lung development.

摘要

大多数肺发育是在周期性拉伸的背景下发生的。机械微环境的改变是许多肺部疾病的共同特征,先天性膈疝 (CDH) 和胎儿气管阻塞 (FETO,一种治疗 CDH 的方法) 是结构、细胞分化和功能改变的极端例子。为了解决细胞培养和体内机械转导模型的局限性,我们使用 (PND5) 小鼠肺 CD326 阳性细胞和成纤维细胞开发了两种小鼠肺类器官 (mLO) 机械转导模型,使其受到增加、减少和周期性应变的影响。在第一个模型中,mLO 暴露于 forskolin (FSK) 和/或破坏 (DIS),并在 20 小时进行评估。FSK、对照和 DIS mLO 中 mLO 的横截面积分别增加了+59%、+24%和-68%。FSK 处理的类器官中增殖细胞数量是其他类器官的两倍。在第二个模型中,与静态拉伸和无拉伸相比,20 小时的 10.25%双轴循环应变增加了肺间质细胞谱系的 mRNAs。循环应变增加了 TGF-β 和整合素介导的信号转导,上游分析表明组蛋白去乙酰化酶、microRNAs 和长非编码 RNA 发挥作用。与无拉伸和静态拉伸 mLO 相比,循环拉伸 mLO 增加了 αSMA 阳性和 αSMA-PDGFRα 双阳性细胞。在这个 PND5 mLO 机械转导模型中,静态拉伸会增加细胞增殖,而循环拉伸会诱导出生后肺发育中重要的间充质基因表达变化。

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