Sundar Isaac K, Yao Hongwei, Sellix Michael T, Rahman Irfan
Department of Environmental Medicine, Lung Biology and Disease Program, University of Rochester Medical Center, Rochester, New York; and.
Department of Medicine, Division of Endocrinology, Diabetes and Metabolism, University of Rochester Medical Center, Rochester, New York.
Am J Physiol Lung Cell Mol Physiol. 2015 Nov 15;309(10):L1056-75. doi: 10.1152/ajplung.00152.2015. Epub 2015 Sep 11.
Disrupted daily or circadian rhythms of lung function and inflammatory responses are common features of chronic airway diseases. At the molecular level these circadian rhythms depend on the activity of an autoregulatory feedback loop oscillator of clock gene transcription factors, including the BMAL1:CLOCK activator complex and the repressors PERIOD and CRYPTOCHROME. The key nuclear receptors and transcription factors REV-ERBα and RORα regulate Bmal1 expression and provide stability to the oscillator. Circadian clock dysfunction is implicated in both immune and inflammatory responses to environmental, inflammatory, and infectious agents. Molecular clock function is altered by exposomes, tobacco smoke, lipopolysaccharide, hyperoxia, allergens, bleomycin, as well as bacterial and viral infections. The deacetylase Sirtuin 1 (SIRT1) regulates the timing of the clock through acetylation of BMAL1 and PER2 and controls the clock-dependent functions, which can also be affected by environmental stressors. Environmental agents and redox modulation may alter the levels of REV-ERBα and RORα in lung tissue in association with a heightened DNA damage response, cellular senescence, and inflammation. A reciprocal relationship exists between the molecular clock and immune/inflammatory responses in the lungs. Molecular clock function in lung cells may be used as a biomarker of disease severity and exacerbations or for assessing the efficacy of chronotherapy for disease management. Here, we provide a comprehensive overview of clock-controlled cellular and molecular functions in the lungs and highlight the repercussions of clock disruption on the pathophysiology of chronic airway diseases and their exacerbations. Furthermore, we highlight the potential for the molecular clock as a novel chronopharmacological target for the management of lung pathophysiology.
肺功能和炎症反应的日常或昼夜节律紊乱是慢性气道疾病的常见特征。在分子水平上,这些昼夜节律依赖于时钟基因转录因子的自动调节反馈环振荡器的活动,包括BMAL1:CLOCK激活复合物以及PERIOD和CRYPTOCHROME抑制因子。关键的核受体和转录因子REV-ERBα和RORα调节Bmal1的表达并为振荡器提供稳定性。昼夜节律功能障碍与对环境、炎症和传染因子的免疫及炎症反应均有关联。分子时钟功能会因暴露组、烟草烟雾、脂多糖、高氧、过敏原、博来霉素以及细菌和病毒感染而改变。去乙酰化酶沉默调节蛋白1(SIRT1)通过对BMAL1和PER2进行乙酰化来调节时钟的时间,并控制时钟依赖性功能,而这些功能也可能受到环境应激源的影响。环境因素和氧化还原调节可能会改变肺组织中REV-ERBα和RORα的水平,同时伴有DNA损伤反应增强、细胞衰老和炎症。肺中的分子时钟与免疫/炎症反应之间存在相互关系。肺细胞中的分子时钟功能可作为疾病严重程度和病情加重的生物标志物,或用于评估疾病管理中时辰疗法的疗效。在此,我们全面概述了肺中受时钟控制的细胞和分子功能,并强调了时钟紊乱对慢性气道疾病及其病情加重的病理生理学的影响。此外,我们强调了分子时钟作为管理肺病理生理学的新型时辰药理学靶点的潜力。