Hypoxia and bacterial infection frequently co-exist, in both acute and chronic clinical settings, and typically result in adverse clinical outcomes. To ameliorate this morbidity, we investigated the interaction between hypoxia and the host response. In the context of acute hypoxia, both S. aureus and S. pneumoniae infections rapidly induced progressive neutrophil mediated morbidity and mortality, with associated hypothermia and cardiovascular compromise. Preconditioning animals through longer exposures to hypoxia, prior to infection, prevented these pathophysiological responses and profoundly dampened the transcriptome of circulating leukocytes. Specifically, perturbation of HIF pathway and glycolysis genes by hypoxic preconditioning was associated with reduced leukocyte glucose utilisation, resulting in systemic rescue from a global negative energy state and myocardial protection. Thus we demonstrate that hypoxia preconditions the innate immune response and determines survival outcomes following bacterial infection through suppression of HIF-1α and neutrophil metabolism. The therapeutic implications of this work are that in the context of systemic or tissue hypoxia therapies that target the host response could improve infection associated morbidity and mortality.
Hypoxia determines survival outcomes of bacterial infection through HIF-1alpha dependent re-programming of leukocyte metabolism.
缺氧通过 HIF-1α 依赖性白细胞代谢重编程决定细菌感染的存活结果
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作者:Thompson A A R, Dickinson R S, Murphy F, Thomson J P, Marriott H M, Tavares A, Willson J, Williams L, Lewis A, Mirchandani A, Dos Santos Coelho P, Doherty C, Ryan E, Watts E, Morton N M, Forbes S, Stimson R H, Hameed A G, Arnold N, Preston J A, Lawrie A, Finisguerra V, Mazzone M, Sadiku P, Goveia J, Taverna F, Carmeliet P, Foster S J, Chilvers E R, Cowburn A S, Dockrell D H, Johnson R S, Meehan R R, Whyte M K B, Walmsley S R
| 期刊: | Science Immunology | 影响因子: | 16.300 |
| 时间: | 2017 | 起止号: | 2017 Feb 10; 2(8):eaal2861 |
| doi: | 10.1126/sciimmunol.aal2861 | 研究方向: | 代谢、细胞生物学 |
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