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地塞米松和去氢表雄酮可显著减轻机械通气相关的肺上皮细胞损伤。

Dexamethasone and transdehydroandrosterone significantly reduce pulmonary epithelial cell injuries associated with mechanical ventilation.

机构信息

Biomedical Research Centre, Qatar University, Doha, Qatar.

Department of Chemistry and Earth Sciences, Qatar University, Doha, Qatar.

出版信息

J Appl Physiol (1985). 2021 Apr 1;130(4):1143-1151. doi: 10.1152/japplphysiol.00574.2020. Epub 2021 Feb 18.

Abstract

Many patients who suffer from pulmonary diseases cannot inflate their lungs normally, as they need mechanical ventilation (MV) to assist them. The stress associated with MV can damage the delicate epithelium in small airways and alveoli, which can cause complications resulting in ventilation-induced lung injuries (VILIs) in many cases, especially in patients with acute respiratory distress syndrome (ARDS). Therefore, efforts were directed to develop safe modes for MV. In our work, we propose a different approach to decrease injuries of epithelial cells (EpCs) upon MV. We alter EpCs' cytoskeletal structure to increase their survival rate during airway reopening conditions associated with MV. We tested two anti-inflammatory drugs dexamethasone (DEX) and transdehydroandrosterone (DHEA) to alter the cytoskeleton. Cultured rat L2 alveolar EpCs were exposed to airway reopening conditions using a parallel-plate perfusion chamber. Cells were exposed to a single bubble propagation to simulate stresses associated with mechanical ventilation in both control and study groups. Cellular injury and cytoskeleton reorganization were assessed via fluorescence microscopy, whereas cell topography was studied via atomic force microscopy (AFM). Our results indicate that culturing cells in media, DEX solution, or DHEA solution did not lead to cell death (static cultures). Bubble flows caused significant cell injury. Preexposure to DEX or DHEA decreased cell death significantly. The AFM verified alteration of cell mechanics due to actin fiber depolymerization. These results suggest potential beneficial effects of DEX and DHEA for ARDS treatment for patients with COVID-19. They are also critical for VILIs and applicable to future clinical studies. Preexposure of cultured cells to either dexamethasone or transdehydroandrosterone significantly decreases cellular injuries associated with mechanical ventilation due to their ability to alter the cell mechanics. This is an alternative protective method against VILIs instead of common methods that rely on modification of mechanical ventilator modes.

摘要

许多患有肺部疾病的患者无法正常充气,因为他们需要机械通气 (MV) 来辅助呼吸。MV 带来的压力会损害小气道和肺泡中的脆弱上皮细胞,这可能导致许多情况下的并发症,进而导致通气引起的肺损伤 (VILI),尤其是在患有急性呼吸窘迫综合征 (ARDS) 的患者中。因此,人们努力开发安全的 MV 模式。在我们的工作中,我们提出了一种不同的方法来减少 MV 引起的上皮细胞 (EpC) 损伤。我们改变 EpC 的细胞骨架结构,以增加它们在与 MV 相关的气道再开放条件下的存活率。我们测试了两种抗炎药物地塞米松 (DEX) 和去氢表雄酮 (DHEA) 来改变细胞骨架。使用平行板灌注室使培养的大鼠 L2 肺泡 EpC 暴露于气道再开放条件下。在对照和研究组中,细胞都暴露于单个气泡传播以模拟与机械通气相关的应激。通过荧光显微镜评估细胞损伤和细胞骨架重组,通过原子力显微镜 (AFM) 研究细胞形貌。我们的结果表明,在培养基、DEX 溶液或 DHEA 溶液中培养细胞不会导致细胞死亡(静态培养)。气泡流动会导致明显的细胞损伤。预先暴露于 DEX 或 DHEA 可显著降低细胞死亡。AFM 验证了由于肌动蛋白纤维解聚导致的细胞力学变化。这些结果表明 DEX 和 DHEA 对 COVID-19 患者 ARDS 治疗具有潜在的有益作用。它们对于 VILI 也很关键,并且适用于未来的临床研究。培养细胞预先暴露于地塞米松或去氢表雄酮可显著降低与机械通气相关的细胞损伤,因为它们能够改变细胞力学。这是一种替代的 VILI 保护方法,而不是依赖于修改机械呼吸机模式的常见方法。

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