H<sub>2</sub>O<sub>2</sub>inhibits alveolar epithelial wound repair in vitro by induction of apoptosis

Geiser, Thomas; Ishigaki, Masanobu; Leer-Buter, Coretta van; Matthay, Michael A.; Broaddus, V. Courtney

doi:10.1152/ajplung.00177.2003

Cited by 69 publications

(50 citation statements)

References 26 publications

(37 reference statements)

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“…Reactive oxygen species (ROS) are released into the alveolar space and contribute to alveolar epithelial damage in patients with acute lung injury. It was shown that H 2 O 2 inhibits alveolar epithelial wound repair in large part by induction of apoptosis and that apoptosis inhibition can maintain wound repair and cell viability in the face of ROS (24). Consistent with this assumption, KGF inhibited H 2 O 2 -induced cleavage of both procaspase-3 and the substrate of caspase-3, the poly(ADP-ribose) polymerase protein, in murine lung cells (42).…”

mentioning

confidence: 60%

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Franco-Montoya

Bourbon

Durrmeyer

et al. 2009

American Journal of Physiology-Lung Cellular and Molecular Phys

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mentioning

confidence: 60%

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Franco-Montoya

Bourbon

Durrmeyer

et al. 2009

American Journal of Physiology-Lung Cellular and Molecular Phys

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“…An in vitro epithelial injury model that allows for the study of epithelial repair processes in the lung was adapted for use in this study (16)(17)(18). Briefly, at 0 hours on the timeline in Figure 1, epithelia were scraped in two perpendicular lines with a p1000 pipette tip and placed in bromodeoxyuridine (BrdU)-containing (10 mM) medium.…”

Section: Mechanical Injury Modelmentioning

confidence: 99%

Asthmatic Airway Epithelium Is Intrinsically Inflammatory and Mitotically Dyssynchronous

Freishtat¹,

Watson²,

Benton³

et al. 2011

Am J Respir Cell Mol Biol

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Asthma is an inflammatory condition for which anti-inflammatory glucocorticoids are the standard of care. However, similar efficacy has not been shown for agents targeting inflammatory cells and pathways. This suggests a noninflammatory cell contributor (e.g., epithelium) to asthmatic inflammation. Herein, we sought to define the intrinsic and glucocorticoid-affected properties of asthmatic airway epithelium compared with normal epithelium. Human primary differentiated normal and asthmatic airway epithelia were cultured in glucocorticoid-free medium beginning at 248 hours. They were pulsed with dexamethasone (20 nM) or vehicle for 2 hours at 226, 22, 122, and 146 hours. Cultures were mechanically scrapewounded at 0 hours and exposed continuously to bromodeoxyuridine (BrdU). Cytokine secretions were analyzed using cytometric bead assays. Wound regeneration/mitosis was analyzed by microscopy and flow cytometry. Quiescent normal (n 5 3) and asthmatic (n 5 6) epithelia showed similar minimal inflammatory cytokine secretion and mitotic indices. After wounding, asthmatic epithelia secreted more basolateral TGF-b1, IL-10, IL-13, and IL-1b (P , 0.05) and regenerated less efficiently than normal epithelia (148 h wound area reduction 5 [mean 6 SEM] 50.2 6 7.5% versus 78.6 6 7.7%; P 5 0.02). Asthmatic epithelia showed 40% fewer BrdU 1 cells at 148 hours (0.32 6 0.05% versus 0.56 6 0.07% of total cells; P 5 0.03), and those cells were more dyssynchronously distributed along the cell cycle (52 6 10, 25 6 4, 23 6 7% for G1/G0, S, and G2/M, respectively) than normal epithelia (71 6 1, 12 6 2, and 17 6 2% for G1/G0, S, and G2/M, respectively). Dexamethasone pulses improved asthmatic epithelial inflammation and regeneration/mitosis. In summary, we show that inflammatory/fibrogenic cytokine secretions are correlated with dyssynchronous mitosis upon injury. Intermittent glucocorticoids simultaneously decreased epithelial cytokine secretions and resynchronized mitosis. These data, generated in an airway model lacking inflammatory cells, support the concept that epithelium contributes to asthmatic inflammation.

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“…may signal to more distant surviving cells via calcium waves or paracrine mediators, as has been previously demonstrated (4,58), responses that could effectuate repair. As the CCN proteins are known to regulate apoptosis (41,63), an additional mechanism by which they might regulate wound repair is via decreased apoptosis of epithelial cells at the wound edge, an established mechanism for differential wound repair (20). Although neutrophil transmigration induces epithelial cell death and denudation of the epithelium in our models, the stimuli used (1 M fMLP in vitro or 1 g KC in vivo) are relatively modest, and the injury induced is relatively mild and repairs rapidly.…”

Section: Discussionmentioning

confidence: 99%

Role of β-catenin-regulated CCN matricellular proteins in epithelial repair after inflammatory lung injury

Zemans

McClendon

Aschner

et al. 2013

American Journal of Physiology-Lung Cellular and Molecular Phys

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H₂O₂inhibits alveolar epithelial wound repair in vitro by induction of apoptosis

Cited by 69 publications

References 26 publications

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Asthmatic Airway Epithelium Is Intrinsically Inflammatory and Mitotically Dyssynchronous

Role of β-catenin-regulated CCN matricellular proteins in epithelial repair after inflammatory lung injury

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H2O2inhibits alveolar epithelial wound repair in vitro by induction of apoptosis

Cited by 69 publications

References 26 publications

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Pulmonary effects of keratinocyte growth factor in newborn rats exposed to hyperoxia

Asthmatic Airway Epithelium Is Intrinsically Inflammatory and Mitotically Dyssynchronous

Role of β-catenin-regulated CCN matricellular proteins in epithelial repair after inflammatory lung injury

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H₂O₂inhibits alveolar epithelial wound repair in vitro by induction of apoptosis