Nitric oxide expression in airway epithelial cells in response to tubercle bacilli stimulation

Kwon, O Jung; Kim, J H; Kim, H C; Suh, Gee Young; Park, J W; Chung, Man Pyo; Rhee, Chong H

doi:10.1111/j.1440-1843.1998.tb00109.x

Cited by 15 publications

(16 citation statements)

References 14 publications

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“…This hypothesis is supported by reports of the localization of RANTES mRNA to macrophages within the granulomas related to sarcoidosis or tuberculosis [25]. In this context, it is interesting that Mycobacterium tuberculosis, which is considered to be a possible antigenic trigger in sarcoidosis, can induce RANTES production [29]. By contrast with sarcoidosis, patients with FA did not show a significant difference from controls with regard to the total number of cells expressing RANTES protein or the levels of RANTES mRNA in BAL cell pellets.…”

Section: The Relationship Of Rantes Expression and Interstitial Lung supporting

confidence: 64%

The source and role of RANTES in interstitial lung disease

Petřek

Pantelidis²,

Southcott³

et al. 1997

Eur Respir J

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The chemokine "regulated on activation, normal T-cell expressed and secreted" (RANTES) is a potent eosinophil and lymphocyte attractant with particular preference for CD45RO+ T-cells and eosinophils. These cells accumulate in the lungs of patients with sarcoidosis and fibrosing alveolitis. The purpose of this study was to determine whether RANTES mediates the inflammatory cell influx in these diffuse lung diseases.Cell types and number of bronchoalveolar cells expressing RANTES protein were investigated by immunocytochemistry using lavage cells obtained from 22 patients and 11 control subjects. Subsequently, RANTES messenger ribonucleic acid (mRNA) was semiquantitated using reverse transcription polymerase chain reaction (RT-PCR) methodology in unseparated lavage cell pellets in 26 patients and 13 control subjects. Cells expressing RANTES mRNA were identified by in situ hybridization.RANTES protein expression in lower respiratory tract (LRT) cells was identified in all study groups. The percentage of RANTES+ lavage cells in sarcoidosis was higher than in controls. RANTES was localized in the cytoplasm, mainly in alveolar macrophages (CD68+ cells) in sarcoidosis, and both in alveolar macrophages and eosinophils in fibrosing alveolitis. The same cell types which expressed RANTES protein expressed RANTES mRNA, as assessed by in situ hybridization. Sarcoidosis patients had higher levels of RANTES mRNA than the other groups. RANTES protein was higher in individuals with abnormal lymphocyte numbers: RANTES protein and mRNA expression was significantly correlated with lavage CD45RO+ lymphocyte numbers.These results indicate that RANTES may mediate T-lymphocyte influx in diffuse lung disease, particularly sarcoidosis. Moreover, they suggest that the cellular source of RANTES is the alveolar macrophage in sarcoidosis, and both macrophages and eosinophils in fibrosing alveolitis.

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Section: The Relationship Of Rantes Expression and Interstitial Lung supporting

confidence: 64%

The source and role of RANTES in interstitial lung disease

Petřek

Pantelidis²,

Southcott³

et al. 1997

Eur Respir J

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“…When produced at high levels for an extended period, nitric oxide and/or resulting reactive nitrogen intermediates are cytotoxic and can inhibit the replication of a variety of intracellular parasites in animal models of infection, including the aerosol-borne bacterial pathogens Mycobacterium tuberculosis (7) and Legionella pneumophila (31). Accumulating evidence also suggests that nitric oxide controls human infection by intracellular parasites, with the most compelling evidence coming from studies of infection by mycobacteria (24,30). Inducible NOS (iNOS), encoded by nos2, is the NOS isoform responsible for producing sustained bactericidal-bacteriostatic levels of nitric oxide in macrophages and other cell types (21).…”

mentioning

confidence: 99%

Nitric Oxide InhibitsCoxiella burnetiiReplication and Parasitophorous Vacuole Maturation

et al. 2002

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Coxiella burnetii is a bacterial obligate intracellular pathogen and the etiological agent of the zoonosis Q fever. The reservoir host range of C. burnetii is extensive and includes livestock, pets, and wildlife. Infected mammals rarely show signs of disease even when shedding large numbers of organisms (25). The primary route of human infection is via inhalation of contaminated aerosols generated by domestic livestock operations.

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“…in response to pathogens (20,21,26), and such nonspecific toxic mediators may be responsible for the reduced recovery of BCG-treated macrophages. Lung epithelial cells, unlike macrophages, produce no or low levels of nitric oxide in response to mycobacterial antigens (13,32). In our own experiments, BCG-treated PMs secreted 10-fold-larger amounts of TNF-␣ than those secreted by the similarly treated PLE cells (results not shown).…”

Section: Discussionmentioning

confidence: 99%