The role of nitric oxide in pleural disease
Nitric oxide (NO) regulates various physiological and pathophysiological functions in the lungs. However, there is much less information about the effects of NO in the pleura. The present review aimed to explore the available evidence regarding the role of NO in pleural disease. NO, has a double-edg...
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Veröffentlicht in: | Respiratory medicine 2021-04, Vol.179, p.106350, Article 106350 |
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Sprache: | eng |
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Zusammenfassung: | Nitric oxide (NO) regulates various physiological and pathophysiological functions in the lungs. However, there is much less information about the effects of NO in the pleura. The present review aimed to explore the available evidence regarding the role of NO in pleural disease. NO, has a double-edged role in the pleural cavity. It is an essential signaling molecule mediating various physiological cell functions such as lymphatic drainage of the serous cavities, the immune response to intracellular multiplication of pathogens, and downregulation of neutrophil migration, but also induces genocytotoxic and mutagenic effects when present in excess. NO is implicated in the pathogenesis of asbestos-related or exudative pleural disease and mesothelioma. From a clinical point of view, the fraction of exhaled NO has been suggested as a potential non-invasive tool for the diagnosis of benign asbestos-related disorders. Under experimental conditions, NO-mimetics were found to attenuate hypoxia-induced therapy resistance in mesothelioma. Similarly, hybrid agents consisting of an NO donor coupled with a parent anti-inflammatory drug showed an enhancement of the anti-inflammatory activity of anti-inflammatory drugs. However, given the paucity of research work performed over the last years in this area, further research should be undertaken to establish reliable conclusions with respect to the feasibility of determining or targeting the NO signaling pathway for pleural disease diagnosis and therapeutic management.
•Endogenous eNOS-derived NO maintains pleural integrity, homeostasis, and repair.•Overexpression of iNOS-derived NO has been associated with pleural damage.•NO has been linked to asbestos-related pleural disease and mesothelioma.•NO is a mediator of membrane permeability implicated in pleural fluid production.•NO is a mediator of lymphatic absorption, and thus infection spread and metastasis. |
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ISSN: | 0954-6111 1532-3064 |
DOI: | 10.1016/j.rmed.2021.106350 |