Molecular mechanisms of dexamethasone actions in COVID-19: Ion channels and airway surface liquid dynamics

IF 2.1 4区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Steroids Pub Date : 2023-12-02 DOI:10.1016/j.steroids.2023.109348
Brian J. Harvey
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Abstract

The COVID-19 pandemic has been a global health crisis of unprecedented magnitude. In the battle against the SARS-CoV-2 coronavirus, dexamethasone, a widely used corticosteroid with potent anti-inflammatory properties, has emerged as a promising therapy in the fight against severe COVID-19.

Dexamethasone is a synthetic glucocorticoid that exerts its therapeutic effects by suppressing the immune system and reducing inflammation. In the context of COVID-19, the severe form of the disease is often characterized by a hyperactive immune response, known as a cytokine storm. Dexamethasone anti-inflammatory properties make it a potent tool in modulating this exaggerated immune response.

Lung inflammation may lead to excessive fluid accumulation in the airways which can reduce gas exchange and mucociliary clearance. Pulmonary oedema and flooding of the airways are hallmarks of severe COVID-19 lung disease. The volume of airway surface liquid is determined by a delicate balance of salt and water secretion and absorption across the airway epithelium. In addition to its anti-inflammatory actions, dexamethasone modulates the activity of ion channels which regulate electrolyte and water transport across the airway epithelium. The observations of dexamethasone activation of sodium ion absorption via ENaC Na+ channels and inhibition of chloride ion secretion via CFTR Cl channels to decrease airway surface liquid volume indicate a novel therapeutic action of the glucocorticoid to reverse airway flooding.

This brief review delves into the early non-genomic and late genomic signaling mechanisms of dexamethasone regulation of ion channels and airway surface liquid dynamics, shedding light on the molecular mechanisms underpinning the action of the glucocorticoid in managing COVID-19.

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地塞米松在COVID-19中的分子机制:离子通道和气道表面液体动力学。
COVID-19大流行是一场规模空前的全球卫生危机。在与SARS-CoV-2冠状病毒的斗争中,地塞米松是一种广泛使用的皮质类固醇,具有有效的抗炎特性,已成为对抗严重COVID-19的一种有希望的治疗方法。地塞米松是一种合成糖皮质激素,通过抑制免疫系统和减少炎症来发挥其治疗作用。在COVID-19的背景下,这种疾病的严重形式通常以过度活跃的免疫反应为特征,称为细胞因子风暴。地塞米松的抗炎特性使其成为调节这种夸大的免疫反应的有效工具。肺部炎症可导致气道中过多的液体积聚,从而减少气体交换和纤毛粘液的清除。肺水肿和气道充血是COVID-19严重肺部疾病的标志。气道表面液体的体积是由盐和水的分泌和吸收在气道上皮间的微妙平衡决定的。除了抗炎作用外,地塞米松还能调节调节电解质和水在气道上皮中的运输的离子通道的活性。地塞米松通过ENaC Na+通道激活钠离子吸收,并通过CFTR Cl-通道抑制氯离子分泌,从而减少气道表面液体体积,这表明糖皮质激素对逆转气道泛滥具有新的治疗作用。本文简要综述了地塞米松调控离子通道和气道表面液体动力学的早期非基因组和晚期基因组信号机制,揭示了糖皮质激素治疗COVID-19的分子机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Steroids
Steroids 医学-内分泌学与代谢
CiteScore
5.10
自引率
3.70%
发文量
120
审稿时长
73 days
期刊介绍: STEROIDS is an international research journal devoted to studies on all chemical and biological aspects of steroidal moieties. The journal focuses on both experimental and theoretical studies on the biology, chemistry, biosynthesis, metabolism, molecular biology, physiology and pharmacology of steroids and other molecules that target or regulate steroid receptors. Manuscripts presenting clinical research related to steroids, steroid drug development, comparative endocrinology of steroid hormones, investigations on the mechanism of steroid action and steroid chemistry are all appropriate for submission for peer review. STEROIDS publishes both original research and timely reviews. For details concerning the preparation of manuscripts see Instructions to Authors, which is published in each issue of the journal.
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