| Literature DB >> 25064128 |
Julie Gibbs1, Louise Ince2, Laura Matthews1, Junjie Mei3, Thomas Bell4, Nan Yang1, Ben Saer2, Nicola Begley2, Toryn Poolman1, Marie Pariollaud1, Stuart Farrow5, Francesco DeMayo6, Tracy Hussell4, G Scott Worthen3, David Ray1, Andrew Loudon2.
Abstract
The circadian system is an important regulator of immune function. Human inflammatory lung diseases frequently show time-of-day variation in symptom severity and lung function, but the mechanisms and cell types underlying these effects remain unclear. We show that pulmonary antibacterial responses are modulated by a circadian clock within epithelial club (Clara) cells. These drive circadian neutrophil recruitment to the lung via the chemokine CXCL5. Genetic ablation of the clock gene Bmal1 (also called Arntl or MOP3) in bronchiolar cells disrupts rhythmic Cxcl5 expression, resulting in exaggerated inflammatory responses to lipopolysaccharide and an impaired host response to Streptococcus pneumoniae infection. Adrenalectomy blocks rhythmic inflammatory responses and the circadian regulation of CXCL5, suggesting a key role for the adrenal axis in driving CXCL5 expression and pulmonary neutrophil recruitment. Glucocorticoid receptor occupancy at the Cxcl5 locus shows circadian oscillations, but this is disrupted in mice with bronchiole-specific ablation of Bmal1, leading to enhanced CXCL5 expression despite normal corticosteroid secretion. The therapeutic effects of the synthetic glucocorticoid dexamethasone depend on intact clock function in the airway. We now define a regulatory mechanism that links the circadian clock and glucocorticoid hormones to control both time-of-day variation and the magnitude of pulmonary inflammation and responses to bacterial infection.Entities:
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Year: 2014 PMID: 25064128 PMCID: PMC4268501 DOI: 10.1038/nm.3599
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440