Activation of Calcitonin Gene-Related Peptide Receptor during Ozone Inhalation Contributes to Airway Epithelial Injury and Repair

Oslund, Karen; Hyde, Dallas M.; Putney, Lei; Alfaro, Mario F.; Walby, William F.; Tyler, Nancy K.; Schelegle, Edward S.

doi:10.1177/0192623309345691

Cited by 11 publications

(6 citation statements)

References 38 publications

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“…However, examination by electron microscopy showed clear alterations in the epithelial structure with enlarged intercellular space and disrupted junctions between adjacent cells in the tracheas of O 3 exposed newborn mice. This is in contrast to previous studies in adult rats where epithelial damage tended to occur more in distal airways than in the proximal airways after 8 h of exposure to 1000 ppb O 3 (Oslund et al, 2009). This apparent difference may be due to differences in the age of animals and duration of O 3 exposure.…”

Section: Discussioncontrasting

confidence: 98%

“…In our newborn mouse model, the results of rt-qPCR showed that CGRP mRNA expression was increased significantly (1.92 ± 0.16-fold) but transiently at 6 h post-O 3 exposure. CGRP may play a role in epithelial injury and repair after O 3 exposure as recently suggested (Oslund et al, 2009). Our results also demonstrate increased expression of the neuropeptide GRP at 24 h post-O 3 exposure.…”

Section: Discussionsupporting

confidence: 87%

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Transcriptome Profiling of the Newborn Mouse Lung Response to Acute Ozone Exposure

Gabehart¹,

Correll²,

Jing³

et al. 2013

Toxicological Sciences

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Ozone pollution is associated with adverse effects on respiratory health in adults and children but its effects on the neonatal lung remain unknown. This study was carried out to define the effect of acute ozone exposure on the neonatal lung and to profile the transcriptome response. Newborn mice were exposed to ozone or filtered air for 3h. Total RNA was isolated from lung tissues at 6 and 24h after exposure and was subjected to microarray gene expression analysis. Compared to filtered air-exposed littermates, ozone-exposed newborn mice developed a small but significant neutrophilic airway response associated with increased CXCL1 and CXCL5 expression in the lung. Transcriptome analysis indicated that 455 genes were down-regulated and 166 genes were up-regulated by at least 1.5-fold at 6h post-ozone exposure (t-test, p < .05). At 24h, 543 genes were down-regulated and 323 genes were up-regulated in the lungs of ozone-exposed, compared to filtered air-exposed, newborn mice (t-test, p < .05). After controlling for false discovery rate, 50 genes were identified as significantly down-regulated and only a few (RORC, GRP, VREB3, and CYP2B6) were up-regulated at 24h post-ozone exposure (q < .05). Gene ontology enrichment analysis revealed that cell cycle-associated functions including cell division/proliferation were the most impacted pathways, which were negatively regulated by ozone exposure, an adverse effect that was associated with reduced bromo-deoxyuridine incorporation. These results demonstrate that acute ozone exposure alters cell proliferation in the developing neonatal lung through a global suppression of cell cycle function.

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Section: Discussioncontrasting

confidence: 98%

Section: Discussionsupporting

confidence: 87%

Transcriptome Profiling of the Newborn Mouse Lung Response to Acute Ozone Exposure

Gabehart¹,

Correll²,

Jing³

et al. 2013

Toxicological Sciences

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“…On the other hand, a protective role of neuropeptitergic system has also been documented. VIP influences many respiratory functions, protects bronchial epithelial cells against damage, produces airway relaxation, inhibits SMC proliferation and reduces inflammation [ 74 ]. CGRP regulates inflammation and promotes epithelial repair [ 75 ].…”

Section: Discussionmentioning

confidence: 99%

Intratracheal Administration of Mesenchymal Stem Cells Modulates Tachykinin System, Suppresses Airway Remodeling and Reduces Airway Hyperresponsiveness in an Animal Model

et al. 2016

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BackgroundThe need for new options for chronic lung diseases promotes the research on stem cells for lung repair. Bone marrow-derived mesenchymal stem cells (MSCs) can modulate lung inflammation, but the data on cellular processes involved in early airway remodeling and the potential involvement of neuropeptides are scarce.ObjectivesTo elucidate the mechanisms by which local administration of MSCs interferes with pathophysiological features of airway hyperresponsiveness in an animal model.MethodsGFP-tagged mouse MSCs were intratracheally delivered in the ovalbumin mouse model with subsequent functional tests, the analysis of cytokine levels, neuropeptide expression and histological evaluation of MSCs fate and airway pathology. Additionally, MSCs were exposed to pro-inflammatory factors in vitro.ResultsFunctional improvement was observed after MSC administration. Although MSCs did not adopt lung cell phenotypes, cell therapy positively affected airway remodeling reducing the hyperplastic phase of the gain in bronchial smooth muscle mass, decreasing the proliferation of epithelium in which mucus metaplasia was also lowered. Decrease of interleukin-4, interleukin-5, interleukin-13 and increase of interleukin-10 in bronchoalveolar lavage was also observed. Exposed to pro-inflammatory cytokines, MSCs upregulated indoleamine 2,3-dioxygenase. Moreover, asthma-related in vivo upregulation of pro-inflammatory neurokinin 1 and neurokinin 2 receptors was counteracted by MSCs that also determined a partial restoration of VIP, a neuropeptide with anti-inflammatory properties.ConclusionIntratracheally administered MSCs positively modulate airway remodeling, reduce inflammation and improve function, demonstrating their ability to promote tissue homeostasis in the course of experimental allergic asthma. Because of a limited tissue retention, the functional impact of MSCs may be attributed to their immunomodulatory response combined with the interference of neuropeptide system activation and tissue remodeling.

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“…Ex vivo treatment with CGRP increased SPC‐ir granule size and number, suggesting an effect on AT2 cell quantity and function. While CGRP has previously been shown to induce epithelial cell proliferation in cell lines, changes in SPC granule number and size have rarely been reported in PCLS (Dakhama et al., 2004; Fu et al., 2010; Kawanami et al., 2009; Li, Cohen, et al., 2020; Oslund et al., 2009). The change in SPC immunoreactivity in the tissue may indicate a change in tissue alveolar cell coverage because a greater number of observed granules and AT2 cells will result in less space for alveolar type 1 (AT1) projections.…”

Section: Discussionmentioning

confidence: 99%

Neuropeptide stimulation of physiological and immunological responses in precision‐cut lung slices

Patlin,

Schwerdtfeger,

Tobet

2023

Physiological Reports

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Organotypic lung slices, sometimes known as precision‐cut lung slices (PCLS), provide an environment in which numerous cell types and interactions can be maintained outside the body (ex vivo). PCLS were maintained ex vivo for up to a week and demonstrated health via the presence of neurons, maintenance of tissue morphology, synthesis of mucopolysaccharides, and minimal cell death. Multiple phenotypes of neuronal fibers were present in lung slices with varied size, caliber, and neurotransmitter immunoreactivity. Of the neuropeptides present in fibers, calcitonin gene‐related peptide (CGRP) was the most prevalent. Exposing PCLS to recombinant CGRP resulted in the proliferation and dispersion of CD19+ B cells in slices taken selectively from females. The number of granules containing immunoreactive (ir) surfactant protein C (SPC), which are representative of alveolar type 2 cells, increased in slices from females within 24 h of exposure to CGRP. Additionally, ir‐SPC granule size increased in slices from males and females across 48 h of exposure to CGRP. Exposure of PCLS to exogenous CGRP did not alter the number of solitary pulmonary neuroendocrine cells (PNEC) but did result in neuroendocrine bodies that had significantly more cells. Neuronal fiber numbers were unchanged based on ir‐peripherin; however, ir‐CGRP became non‐detectable in fibers while unchanged in PNECs. The effects of exogenous CGRP provide insight into innate immune and neuroendocrine responses in the lungs that may be partially regulated by neural fibers. The sex‐dependent nature of these changes may point to the basis for sex‐selective outcomes among respiratory diseases.

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Activation of Calcitonin Gene-Related Peptide Receptor during Ozone Inhalation Contributes to Airway Epithelial Injury and Repair

Cited by 11 publications

References 38 publications

Transcriptome Profiling of the Newborn Mouse Lung Response to Acute Ozone Exposure

Transcriptome Profiling of the Newborn Mouse Lung Response to Acute Ozone Exposure

Intratracheal Administration of Mesenchymal Stem Cells Modulates Tachykinin System, Suppresses Airway Remodeling and Reduces Airway Hyperresponsiveness in an Animal Model

Neuropeptide stimulation of physiological and immunological responses in precision‐cut lung slices

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