ACE2 通过调节 Ang1-7/Mas 减轻呼吸机诱导的肺损伤中的内质网应激并防止细胞焦亡。
ACE2 Alleviates Endoplasmic Reticulum Stress and Protects against Pyroptosis by Regulating Ang1-7/Mas in Ventilator-Induced Lung Injury.
机构信息
Department of Intensive Care Unit, Fuzhou University Affiliated Provincial Hospital, 350001 Fuzhou, Fujian, China.
Department of Pulmonary Disease, Shanghai Municipal Hospital of Traditional Chinese Medicine, Shanghai University of Traditional Chinese Medicine, 200071 Shanghai, China.
出版信息
Front Biosci (Landmark Ed). 2024 Sep 24;29(9):334. doi: 10.31083/j.fbl2909334.
BACKGROUND
Ventilator-induced lung injury (VILI) is a consequence of inflammation and increased alveolar-capillary membrane permeability due to alveolar hyperdistention or elevated intrapulmonary pressure, but the precise mechanisms remain unclear. The aim of the study was to analyze the mechanism by which angiotensin converting enzyme 2 (ACE2) alleviates endoplasmic reticulum stress (ERS) and protects alveolar cells from pyroptosis in VILI by regulating angiotensin (Ang)1-7/Mas.
METHODS
VILI was induced in mice by mechanical ventilation by regulating the tidal volume. The alveolar cell line, A549, mimics VILI by cyclic stretch (CS). Ang (1-7) (100 nmol/L) was added to the medium. ERS was induced in cells by stimulating with tunicamycin (TM, 2 μg/mL). ERS was inhibited by tracheal instillation of 4-phenylbutyric acid (4-PBA) (1 mg/kg). ACE2's enzymatic function was activated or inhibited by subcutaneous injection of resorcinolnaphthalein (RES, 20 μg/kg) or MLN-4760 (20 μg/kg). pGLV-EF1a-GFP-ACE2 was instilled into the trachea to increase the protein expression of ACE2. The Ang (1-7) receptor, Mas, was antagonized by injecting A779 subcutaneously (80 μg/kg).
RESULTS
ACE2 protein levels decreased after modeling. Ang (1-7) level was decreased and Ang II was accumulated. ERS was significantly induced in VILI mice, and pyroptosis was observed in cells. When ERS was inhibited, pyroptosis under the VILI condition was significantly inhibited. Ang (1-7) alleviated ERS and pyroptosis under CS. When ERS was continuously activated, the function of Ang (1-7) in inhibiting pyroptosis was blocked. Resorcinolnaphthalein (RES) effectively promoted Ang II conversion, alleviated the Ang (1-7) level in VILI, ameliorated lung injury, and inhibited ERS and cell pyroptosis. Inhibiting ACE2's function in VILI hindered the production of Ang (1-7), promoted the accumulation of Ang II, and exacerbated ERS and pyroptosis, along with lung injury. The Mas antagonist significantly blocked the inhibitory effects of ACE2 on ERS and pyroptosis in VILI.
CONCLUSIONS
Reduced ACE2 expression in VILI is involved in ERS and pyroptosis-related injury. ACE2 can alleviate ERS in alveolar cells by catalyzing the production of Ang (1-7), thus inhibiting pyroptosis in VILI.
背景
呼吸机相关性肺损伤(VILI)是由于肺泡过度扩张或肺内压升高导致炎症和肺泡毛细血管膜通透性增加而引起的,但确切的机制仍不清楚。本研究旨在分析血管紧张素转换酶 2(ACE2)通过调节血管紧张素(Ang)1-7/ Mas 缓解内质网应激(ERS)并保护 VILI 中肺泡细胞发生细胞焦亡的机制。
方法
通过调节潮气量对小鼠进行机械通气以诱导 VILI。肺泡细胞系 A549 通过循环拉伸(CS)模拟 VILI。将 Ang(1-7)(100nmol/L)加入培养基中。用衣霉素(TM,2μg/ml)刺激细胞诱导 ERS。通过气管内滴注 4-苯丁酸(4-PBA)(1mg/kg)抑制 ERS。通过皮下注射间苯二酚萘酚(RES,20μg/kg)或 MLN-4760(20μg/kg)激活或抑制 ACE2 的酶活性。将 pGLV-EF1a-GFP-ACE2 注入气管以增加 ACE2 的蛋白表达。通过皮下注射 A779 拮抗 Ang(1-7)受体 Mas(80μg/kg)。
结果
建模后 ACE2 蛋白水平降低。Ang(1-7)水平降低,Ang II 积累。VILI 小鼠明显诱导 ERS,细胞发生细胞焦亡。当抑制 ERS 时,VILI 条件下的细胞焦亡明显受到抑制。Ang(1-7)在 CS 下缓解 ERS 和细胞焦亡。当持续激活 ERS 时,Ang(1-7)抑制细胞焦亡的功能被阻断。间苯二酚萘酚(RES)有效促进 Ang II 转化,减轻 VILI 中 Ang(1-7)水平,改善肺损伤,抑制 ERS 和细胞焦亡。在 VILI 中抑制 ACE2 的功能会阻碍 Ang(1-7)的产生,促进 Ang II 的积累,并加重 ERS 和细胞焦亡以及肺损伤。Mas 拮抗剂显著阻断了 ACE2 在 VILI 中对 ERS 和细胞焦亡的抑制作用。
结论
VILI 中 ACE2 表达减少与 ERS 和细胞焦亡相关损伤有关。ACE2 通过催化 Ang(1-7)的产生来减轻肺泡细胞中的 ERS,从而抑制 VILI 中的细胞焦亡。
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