Earliest Innate Immune Responses Require Macrophage RelA during Pneumococcal Pneumonia

Pittet, Lynnelle A.; Quinton, Lee J.; Yamamoto, Kazuko; Robson, Bryanne E.; Ferrari, Joseph D.; Algül, Hana; Schmid, Roland M.; Mizgerd, Joseph P.

doi:10.1165/rcmb.2010-0210oc

Cited by 49 publications

(75 citation statements)

References 54 publications

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“…The increased pneumococcal burden in the BAL fluid of LPL Ϫ/Ϫ mice as early as 3 h after infection distinguishes our model from previous models of pneumococcal susceptibility (45)(46)(47)(48). In a recent report, neutrophilic defects in antipneumococcal killing increased the pulmonary pneumococcal burden 12 and 24 h after challenge, but differences were not observed at 6 h, a point in infection when alveolar macrophages would be expected to dominate the initial immune response (46).…”

Section: Discussionmentioning

confidence: 71%

L-Plastin Is Essential for Alveolar Macrophage Production and Control of Pulmonary Pneumococcal Infection

et al. 2014

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We report that mice deficient for the hematopoietic-specific, actin-bundling protein L-plastin (LPL) succumb rapidly to intratracheal pneumococcal infection. The increased susceptibility of LPL ؊/؊ mice to pulmonary pneumococcal challenge correlated with reduced numbers of alveolar macrophages, consistent with a critical role for this cell type in the immediate response to pneumococcal infection. LPL ؊/؊ mice demonstrated a very early clearance defect, with an almost 10-fold-higher bacterial burden in the bronchoalveolar lavage fluid 3 h following infection. Clearance of pneumococci from the alveolar space in LPL ؊/؊ mice was defective compared to that in Rag1 ؊/؊ mice, which lack all B and T lymphocytes, indicating that innate immunity is defective in LPL ؊/؊ mice. We did not identify defects in neutrophil or monocyte recruitment or in the production of inflammatory cytokines or chemokines that would explain the early clearance defect. However, efficient alveolar macrophage regeneration following irradiation required LPL. We thus identify LPL as being key to alveolar macrophage development and essential to an effective antipneumococcal response. Further analysis of LPL ؊/؊ mice will illuminate critical regulators of the generation of alveolar macrophages and, thus, effective pulmonary innate immunity.

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Section: Discussionmentioning

confidence: 71%

L-Plastin Is Essential for Alveolar Macrophage Production and Control of Pulmonary Pneumococcal Infection

et al. 2014

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“…in part, to improved alveolar macrophage function. Interestingly, we observed an increase in CXCL2 expression in Miwi2 -/-mice, which is derived exclusively from macrophages during early stages of pneumococcal pneumonia (34). While secretory metaplasia and hypersecretory phenotypes are pathological in many lung diseases (35), such as cystic fibrosis and asthma, it is conceivable that small increases in club cell numbers may impart improved antibacterial defenses during infection.…”

Section: Discussionmentioning

confidence: 73%

Expression of Piwi protein MIWI2 defines a distinct population of multiciliated cells

Wasserman

Szymaniak²,

Hinds

et al. 2017

Journal of Clinical Investigation

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“…Among hematopoietic cells, the first responders are the alveolar macrophages. When pneumococcus enters the lung, alveolar macrophages mediate the initial recognition and elaboration of cytokine signals that coordinate the earliest steps of host defense (22). The subsequent recruitment of neutrophils is needed for effective immunity against diverse microbes in the lungs.…”

Section: Inflammation and Innate Immunity During Lung Infectionmentioning

confidence: 99%

Respiratory Infection and the Impact of Pulmonary Immunity on Lung Health and Disease

Mizgerd

2012

Am J Respir Crit Care Med

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Acute lower respiratory tract infection is responsible for an inordinate disease burden. Pulmonary immunity determines the outcomes of these infections. The innate and adaptive immune responses to microbes in the lung are critical to maintaining a healthy respiratory system and preventing pulmonary disease. In addition to balancing antimicrobial defense against the risk of lung injury during the immediate infection, the shaping of pulmonary immunity by respiratory infection contributes to the pathophysiology of many and even perhaps most chronic pulmonary diseases. This Pulmonary Perspective aims to communicate two interconnected points. First, tremendous morbidity and mortality result from inadequate, misguided, or excessive pulmonary immunity. Second, our understanding of pulmonary immunity is at an exciting stage of rapid developments and discoveries, but many questions remain. Further advances in pulmonary immunity and elucidation of the cellular and molecular responses to microbes in the lung are needed to develop novel approaches to predicting, preventing, and curing respiratory disease.

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Earliest Innate Immune Responses Require Macrophage RelA during Pneumococcal Pneumonia

Cited by 49 publications

References 54 publications

L-Plastin Is Essential for Alveolar Macrophage Production and Control of Pulmonary Pneumococcal Infection

L-Plastin Is Essential for Alveolar Macrophage Production and Control of Pulmonary Pneumococcal Infection

Expression of Piwi protein MIWI2 defines a distinct population of multiciliated cells

Respiratory Infection and the Impact of Pulmonary Immunity on Lung Health and Disease

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