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61 results on '"Eosinophils -- Research"'

1. Findings on Immunology Reported by Investigators at University of Sao Paulo (Butyrate Attenuates Lung Inflammation by Negatively Modulating Th9 Cells)

Subjects
Cell differentiation -- Research, Eosinophils -- Research, Immunology -- Research, Lung diseases -- Care and treatment, T cells -- Research, Obesity, Inflammation, Esters, Physical fitness, Editors, Health
Abstract

2019 FEB 23 (NewsRx) -- By a News Reporter-Staff News Editor at Obesity, Fitness & Wellness Week -- A new study on Health and Medicine - Immunology is now available. [...]

Published
2019

2. A hidden residential cell in the lung

Author

Rothenberg, Marc E.

Subjects
Eosinophils -- Research, Immunity -- Research, Asthma -- Research -- Care and treatment -- Complications and side effects, Health care industry
Abstract

Eosinophils are classically known as proinflammatory cells, as they are equipped with a variety of preformed cytotoxic mediators and have been shown to definitively contribute to asthma. The connection between eosinophils and asthma development has led to a new class of asthma therapeutics based on blocking eosinophils with humanized antibodies that neutralize IL-5, a potent eosinophil growth, activation, and survival factor. Yet, recent studies have led to an increasing appreciation that eosinophils have a variety of homeostatic functions, including immunomodulation. In this issue of the JCI, Mesnil et al. identify a notable population of lung-resident eosinophils and demonstrate that, compared with traditional eosinophils, these cells have distinct characteristics, including nuclear structure, surface markers, IL-5 independence, and immunoregulatory function that is capable of polarizing adaptive immune responses, at least in vitro. Thus, these results reinforce a key homeostatic role for this enigmatic cell population, particularly in residing and regulating immunity in the lung., Eosinophils: traditionally proinflammatory Eosinophils are traditionally viewed as proinflammatory cells, as they are equipped with a variety of preformed cytotoxic mediators, including the granule proteins major basic protein (MBP) and [...]

Published
2016
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3. More than just counting eosinophils: proximal oesophageal involvement and subepithelial sclerosis are major diagnostic criteria for eosinophilic oesophagitis

Author

Lee, Stephen, de Boer, W. Bastiaan, Naran, Anupam, Leslie, Connull, Raftopoulous, Spiro, Ee, Hooi, and Kumarasinghe, M. Priyanthi

Subjects
Esophagitis -- Diagnosis, Esophagitis -- Research, Eosinophils -- Identification and classification, Eosinophils -- Research, Sclerosis -- Diagnosis, Sclerosis -- Research, Health
Published
2010

4. Psychological stress induces eosinophils to produce corticotrophin releasing hormone in the intestine

Author

Zheng, P.-Y., Feng, B.-S., Oluwole, C., Struiksma, S., Chen, X., Li, P., Tang, S.-G., and Yang, P.-C.

Subjects
Stress (Psychology) -- Research, Corticotropin releasing hormone -- Physiological aspects, Corticotropin releasing hormone -- Research, Eosinophils -- Physiological aspects, Eosinophils -- Research, Colorectal diseases -- Development and progression, Colorectal diseases -- Research, Gastrointestinal diseases -- Development and progression, Gastrointestinal diseases -- Research, Health
Published
2009

5. Environmental tobacco smoke exposure does not prevent corticosteroids reducing inflammation, remodeling, and airway hyperreactivity in mice exposed to allergen

Author

Song, Dae Jin, Min, Myung Goo, Miller, Marina, Cho, Jae Youn, and Broide, David H.

Subjects
Airway obstruction (Medicine) -- Risk factors, Airway obstruction (Medicine) -- Drug therapy, Airway obstruction (Medicine) -- Research, Allergens -- Health aspects, Corticosteroids -- Usage, Corticosteroids -- Health aspects, Eosinophils -- Physiological aspects, Eosinophils -- Research, Passive smoking -- Health aspects, Biological sciences
Abstract

The ability of corticosteroids to reduce airway inflammation and improve lung function is significantly reduced in asthmatics who are tobacco smokers compared with asthmatics who are nonsmokers. As not only high levels of tobacco smoke exposure in active smokers, but also significantly lower levels of tobacco smoke exposure from passive environmental tobacco smoke (ETS) exposure in nonsmokers can increase both asthma symptoms and the frequency of asthma exacerbations, we utilized a mouse model to determine whether corticosteroids can reduce levels of airway inflammation, airway remodeling, and airway hyperreactivity in mice exposed to the combination of chronic ETS and ovalbumin (OVA) allergen. Chronic ETS exposure alone did not induce increases in eosinophilic airway inflammation, airway remodeling, or airway hyperreactivity. Mice exposed to chronic OVA allergen had significantly increased levels of peribronchial fibrosis, increased thickening of the smooth muscle layer, increased mucus, and increased airway hyperreactivity, which was significantly enhanced by coexposure to the combination of chronic ETS and chronic OVA allergen. Administration of corticosteroids to mice exposed to chronic ETS and OVA allergen significantly reduced levels of eosinophilic airway inflammation, mucus production, peribronchial smooth muscle thickness, airway hyperreactivity, and the number of peribronchial TGF-[beta]1 + cells. Overall, this study demonstrates that corticosteroids can significantly reduce levels of eosinophilic inflammation, mucus expression, airway remodeling, and airway hyperreactivity in chronic ETS-exposed mice challenged with allergen. allergy; eosinophils

Published
2009

6. Atropine-enhanced, antigen challenge-induced airway hyperreactivity in guinea pigs is mediated by eosinophils and nerve growth factor

Author

Verbout, Norah G., Jacoby, David B., Gleich, Gerald J., and Fryer, Allison D.

Subjects
Asthma -- Drug therapy, Asthma -- Research, Eosinophils -- Health aspects, Eosinophils -- Research, Nerve growth factor -- Health aspects, Nerve growth factor -- Physiological aspects, Nerve growth factor -- Research, Parasympatholytic agents -- Dosage and administration, Parasympatholytic agents -- Research, Biological sciences
Abstract

Although anticholinergic therapy inhibits bronchoconstriction in asthmatic patients and antigen-challenged animals, administration of atropine 1 h before antigen challenge significantly potentiates airway hyperreactivity and eosinophil activation measured 24 h later. This potentiation in airway hyperreactivity is related to increased eosinophil activation and is mediated at the level of the airway nerves. Since eosinophils produce nerve growth factor (NGF), which is known to play a role in antigeninduced airway hyperreactivity, we tested whether NGF mediates atropine-enhanced, antigen challenge-induced hyperreactivity. Antibody to NGF (Ab NGF) was administered to sensitized guinea pigs with and without atropine pretreatment (1 mg/kg iv) 1 h before challenge. At 24 h after challenge, animals were anesthetized, vagotomized, paralyzed, and ventilated. Electrical stimulation of both vagus nerves caused bronchoconstriction that was increased in challenged animals. Atropine pretreatment potentiated antigen challenge-induced hyperreactivity. Ab NGF did not affect eosinophils or inflammatory cells in any group, nor did it prevent hyperreactivity in challenged animals that were not pretreated with atropine. However, Ab NGF did prevent atropine-enhanced, antigen challenge-induced hyperreactivity and eosinophil activation (assessed by immunohistochemistry). This effect was specific to NGF, since animals given control IgG remained hyperreactive. These data suggest that anticholinergic therapy amplifies eosinophil interactions with airway nerves via NGF. Therefore, therapeutic strategies that target both eosinophil activation and NGF-mediated inflammatory processes in allergic asthma are likely to be beneficial. anticholinergic; asthma; muscarinic receptors; parasympathetic nerves; neurotrophins

Published
2009

7. Eosinophilia-associated muscle disorders: an immunohistological study with tissue localisation of major basic protein in distinct clinicopathological forms

Author

Cantarini, L., Volpi, N., Carbotti, P., Greco, G., Agliano, M., Bellisai, F., Giannini, F., Alessandrini, C., Grasso, G., and Galeazzi, M.

Subjects
Muscle diseases -- Diagnosis, Eosinophils -- Research, Eosinophils -- Physiological aspects, Histology -- Usage, Histology -- Analysis, Proteins -- Research, Proteins -- Physiological aspects, Health
Published
2009

8. A severe deficiency of coagulation factor VIIa results in attenuation of the asthmatic response in mice

Author

Shinagawa, Kazuhiko, Ploplis, Victoria A., and Castellino, Francis J.

Subjects
Blood coagulation factors -- Physiological aspects, Blood coagulation factors -- Research, Eosinophils -- Physiological aspects, Eosinophils -- Research, Chemokines -- Physiological aspects, Chemokines -- Research, Biological sciences
Abstract

Eosinophil counts in the bronchoalveolar lavage fluid of wild-type (WT) mice increased after ovalbumin (OVA) challenge, a response that was diminished in comparably challenged low-expressing coagulation factor VII ([FVII.sup.tTA/tTA]) mice. Levels of T helper type 2 (Th2) cytokines, IL-4, IL-5, and IL-13, and eosinophil-attracting chemokines, eotaxin and RANTES, were also lower in the OVA-challenged [FVII.sup.tTA/tTA] mice. Eosinophils purified from low-FVII mice underwent apoptosis at a faster rate compared with WT eosinophils, and eosinophil migration in response to eotaxin was reduced in eosinophils obtained from [FVII.sup.tTA/tTA] mice. Airway hyperresponsiveness and mucous layer thickness were reduced in OVA-treated [FVII.sup.tTA/tTA] mice, and addition of exogenous coagulation factor X (FX) enhanced mucin production in human epithelial NCI-H292 cells. Correspondingly, incubation of FX with NCI-H292 cells resulted in activated (a) FX production, suggesting that the components required for FX activation were present on NCI-H292 cells. These results demonstrate that FVIIa functions in the asthmatic response to an allergen by stimulating lung eosinophilia, airway hyperresponsiveness, and mucin production, this latter effect through its ability to activate FX in conjunction with tissue factor. coagulation factor X; eosinophilia; T helper type 2 cytokines; chemokines; airway

Published
2009

9. Pin1 regulates TGF-[beta]1 production by activated human and murine eosinophils and contributes to allergic lung fibrosis

Author

Shen, Zhong-Jian, Esnault, Stephane, Rosenthal, Louis A., Szakaly, Renee J., Sorkness, Ronald L., Westmark, Pamela R., Sandor, Matyas, and Malter, James S.

Subjects
Eosinophils -- Health aspects, Eosinophils -- Genetic aspects, Eosinophils -- Research, Gene expression -- Methods, Gene expression -- Research, Pulmonary fibrosis -- Risk factors, Pulmonary fibrosis -- Genetic aspects, Pulmonary fibrosis -- Research
Abstract

Eosinophilic inflammation is a cornerstone of chronic asthma that often culminates in subepithelial fibrosis with variable airway obstruction. Pulmonary eosinophils (Eos) are a predominant source of TGF-[beta]1, which drives fibroblast proliferation and extracellular matrix deposition. We investigated the regulation of TGF-[beta]1 and show here that the peptidyl-prolyl isomerase (PPIase) Pin1 promoted the stability of TGF-[beta]1 mRNA in human Eos. In addition, Pin1 regulated cytokine production by both in vitro and in vivo activated human Eos. We found that Pin1 interacted with both PKC-[alpha] and protein phosphatase 2A, which together control Pin1 isomerase activity. Pharmacologic blockade of Pin1 in a rat asthma model selectively reduced eosinophilic pulmonary inflammation, TGF-[beta]1 and collagen expression, and airway remodeling. Furthermore, chronically challenged Pin1-/- mice showed reduced peribronchiolar collagen deposition compared with wild-type controls. These data suggest that pharmacologic suppression of Pin1 may be a novel therapeutic option to prevent airway fibrosis in individuals with chronic asthma., Introduction Persistent asthma is characterized by chronic pulmonary inflammation, which often culminates in airway fibrosis. The development of airway disease is referred to as remodeling and includes the deposition of [...]

Published
2008

10. Coarse particulate matter (P[M.sub.2.5-10]) affects heart rate variability, blood lipids, and circulating eosinophils in adults with asthma

Author

Yeatts, Karin, Svendsen, Erik, Creason, John, Alexis, Neil, Herbst, Margaret, Scott, James, Kupper, Lawrence, Williams, Ronald, Neas, Lucas, Cascio, Wayne, Devlin, Robert B., and Peden, David B.

Subjects
Asthmatics -- Research, Asthmatics -- Physiological aspects, Particles -- Health aspects, Blood lipids -- Research, Blood lipids -- Health aspects, Eosinophils -- Research, Eosinophils -- Health aspects
Abstract

INTRODUCTION: We investigated whether markers of airway and systemic inflammation, as well as heart rate variability (HRV) in asthmatics, change in response to fluctuations in ambient particulate matter (PM) in [...]

Published
2007

11. PCR-based detection of angiostrongylus cantonensis in tissue and mucus secretions from molluscan hosts

Author

Qvarnstrom, Yvonne, Sullivan, James J., Bishop, Henry S., Hollingsworth, Robert, and da Silva, Alexandre J.

Subjects
Mollusks -- Physiological aspects, Mollusks -- Genetic aspects, Eosinophils -- Research, Bacterial genetics -- Research, Biological sciences
Abstract

A PCR-based method was developed to detect Angiostrongylus cantonensis directly from molluscan tissue to control the outbreak of human eosinophilic meningitis.

Published
2007

12. Lymphopenic mice reconstituted with limited repertoire T cells develop severe, multiorgan, Th2-associated inflammatory disease

Author

Milner, Joshua D., Ward, Jerrold M., Keane-Myers, Andrea, and Paul, William E.

Subjects
Lymphocytopenia -- Research, Eosinophils -- Research, Macrophages -- Research, T cells -- Research, Science and technology
Abstract

Lymphopenia and restricted T cell repertoires in humans are often associated with severe eosinophilic disease and a T cell Th2 bias. To examine the pathogenesis of this phenomenon, C57BL/6 Rag2-/-mice received limited (3 x [10.sup.4]) or large (2 x [10.sup.6]) numbers of CD4 T cells. Three to 5 months after transfer, mice that had received 3 x [10.sup.4] T cells, but not those that received 2 x [10.sup.6], developed fulminant macrophage pneumonia with eosinophilia, Ym1 deposition, and methacholine-induced airway hyperresponsiveness, as well as eosinophilic gastritis; esophagitis and other organ damage occurred in some cases. Donor cells were enriched for IL-4, IL-5, and IL-13 producers. When 3 x [10.sup.4] cells were transferred into CD3[epsilon]-/-hosts, the mice developed strikingly elevated serum IgE. Prior transfer of 3 x [10.sup.5] CD25+ CD4 T cells into Rag2-/- recipients prevented disease upon subsequent transfer of CD25- CD4 T cells, whereas 3 x [10.sup.4] regulatory T cells (Tregs) did not, despite the fact that there were equal total numbers of Tregs in the host at the time of transfer of CD25- CD4 T cells. Limited repertoire complexity of Tregs may lead to a failure to control induction of immunopathologic responses, and limitation in repertoire complexity of conventional cells may be responsible for the Th2 phenotype. eosinophils | IgE ILL-4 | macrophages | pneumonia

Published
2007

13. TLR7 ligand prevents allergen-induced airway hyperresponsiveness and eosinophilia in allergic asthma by a MYD88-dependent and MK2-independent pathway

Author

Moisan, J., Camateros, P., Thuraisingam, T., Marion, D., Koohsari, H., Martin, P., Boghdady, M.L., Ding, A., Gaestel, M., Guiot, M.C., Martin, J.G., and Radzioch, D.

Subjects
Eosinophils -- Research, Protein kinases -- Research, Asthma in children -- Causes of, Asthma in children -- Care and treatment, Biological sciences
Abstract

Asthma is one of the leading causes of childhood hospitalization, and its incidence is on the rise throughout the world. Currently, the standard treatment for asthma is the use of corticosteroids to try to suppress the inflammatory reaction taking place in the bronchial tree. Using a murine model of atopic allergic asthma employing a methacholine-hyperresponsive (A/J) as well as a hyporesponsive (C57BL/6) strain of mice sensitized and challenged with ovalbumin, we show that treatment with a synthetic Toll-like receptor 7 (TLR7) ligand (S-28463, a member of the imidazoquinoline family) prevents development of the asthmatic phenotype. Treatment with S-28463 resulted in a reduction of airway resistance and elastance following ovalbumin sensitization and challenge. This was accompanied by a dramatic reduction in infiltration of leukocytes, especially eosinophils, into the lungs of both C57BL/6 and A/J mice following OVA challenge. Treatment with S-28463 also abolished both the elevation in serum IgE level as well as the induction of IL-4, IL-5, and IL-13 by OVA challenge. The protective effects of S-28463 were also observed in MK2 knockout, but not MYD88 knockout, mice. We did not observe a switch in cytokine profile from [T.sub.H]2 to [T.sub.H]1, as both 1L-12p70 and IFN-[gamma] levels were reduced following S-28463 treatment. These results clearly demonstrate the anti-inflammatory effect of imidazoquinolines in an allergic asthma model as well as the clinical potential of TLR7 ligands in the treatment of allergic diseases. Toll-like receptors; asthma; eosinophils; lung; inflammation; mitogen-activated protein kinase-activated protein-2

Published
2006

14. Cytokine receptor-mediated trafficking of preformed IL-4 in eosinophils identifies an innate immune mechanism of cytokine secretion

Author

Spencer, Lisa A., Melo, Rossana C.N., Perez, Sandra A.C., Bafford, Staci P., Dvorak, Ann M., and Weller, Peter F.

Subjects
Cytokine receptors -- Research, Eosinophils -- Research, Science and technology
Abstract

Although leukocytes of the innate immune system, including eosinophils, contain within their granules preformed stores of cytokines available for selective and rapid release, little is known about the mechanisms governing the mobilization and secretion of these cytokines. Here we show that a cytokine receptor, the IL-4 receptor [alpha] chain, mediates eotaxin-stimulated mobilization of preformed IL-4 from eosinophil granules into secretory vesicles. Eosinophils contain substantial intracellular quantities of several granule- and vesicle-associated cytokine receptors, including IL-4, IL-6, and IL-13 receptors as well as CCR3. Both IL-4 and IL-4 receptor [alpha] chain colocalized in eosinophil granules; and after eotaxin-stimulation, IL-4 receptor [alpha] chain, bearing bound IL-4, was mobilized into secretory vesicles. These findings indicate that intracellular cytokine receptors within secretory vesicles transport their cognate cytokines requisite for the secretion of cytokines preformed in innate immune leukocytes. intracellular cytokine receptor | intracellular cytokine trafficking piecemeal degranulation | vesicular transport

Published
2006

15. Diagnosing occupational asthma: insight from induced sputum (1)

Author

Lemiere, Catherine

Subjects
Eosinophils -- Research, Sputum -- Research, Asthma -- Diagnosis -- Research, Biological sciences, Diagnosis, Research
Abstract

Abstract: The diagnosis of occupational asthma needs to be made objectively using as many criteria as possible. The latter include laboratory exposure tests with occupational agent(s), which are only available [...]

Published
2006

16. Eosinophil granulocytes are activated during the remission phase of ulcerative colitis

Author

Lampinen, M., Ronnblom, A., Amin, K., Kristjansson, G., Rorsman, F., Sangfelt, P., Safsten, B., Wagner, M., Wanders, A., Winqvist, O., and Carlson, M.

Subjects
Ulcerative colitis -- Development and progression, Eosinophils -- Physiological aspects, Eosinophils -- Research, Neutrophils -- Physiological aspects, Neutrophils -- Research, Flow cytometry -- Usage, Health
Published
2005

17. Eosinophils alter colonic epithelial barrier function: role for major basic protein

Author

Furuta, Glenn T., Nieuwenhuis, Edward E.S., Karhausen, Jorn, Gleich, Gerald, Blumberg, Richard S., Lee, James J., and Ackerman, Steven J.

Subjects
Eosinophils -- Research, Eosinophils -- Health aspects, Food allergy -- Research, Food allergy -- Health aspects, Gastroenteritis -- Health aspects, Gastroenteritis -- Research, Proteins -- Health aspects, Biological sciences
Abstract

Mucosal eosinophils increase in a number of gastrointestinal diseases that are often associated with altered epithelial barrier function, including food allergic enteropathies and inflammatory bowel diseases. Although eosinophils are known to secrete biologically active mediators including granule proteins, their role in gastrointestinal diseases is uncertain. The aim of this study was to determine the impact of eosinophils on intestinal barrier function. Epithelial barrier function was determined in a coculture of eosinophils and T84 epithelial cells and in a routine model of T helper (Th) type 2-mediated colitis. Coculture conditions resulted in decreased transepithelial resistance (TER) and increased transepithelial flux. Cell-free coculture supematants contained a [greater than or equal to]5-kDa soluble factor that also diminished TER; these supernatants contained the eosinophil-granule proteins major basic protein (MBP) and eosinophil-derived neurotoxin (EDN). T84 barrier function decreased significantly when basolateral surfaces were exposed to native human MBP but not EDN. Additional studies identified downregulation of the tight junctional molecule occludin as at least one mechanism for MBP action. MBP-null mice were protected from inflammation associated with oxazolone colitis compared with wild-type mice. In conclusion, MBP decreases epithelial barrier function and in this manner contributes to the pathogenesis of inflammatory bowel diseases. tight junction; eosinophilic gastroenteritis; food allergy

Published
2005

18. The changing role of eosinophils in long-term hyperreactivity following a single ozone exposure

Author

Yost, Bethany L., Gleich, Gerald J., Jacoby, David B., and Fryer, Allison D.

Subjects
Eosinophils -- Research, Vagus nerve -- Research, Biological sciences
Abstract

Ozone hyperreactivity over 24 h is mediated by blockade of inhibitory [M.sub.2] muscarinic autoreceptors by eosinophil major basic protein. Because eosinophil populations in the lungs fluctuate following ozone, the contribution of eosinophils to [M.sub.2] dysfunction and airway hyperreactivity was measured over several days. After one exposure to ozone, [M.sub.2] function, vagal reactivity, smooth muscle responsiveness, and inflammation were measured in anesthetized guinea pigs. Ozone-induced hyperreactivity to vagal stimulation persisted over 3 days. Although hyperreactivity one day after ozone is mediated by eosinophils, AbVLA-4 did not inhibit either eosinophil accumulation in the lungs or around the nerves or prevent hyperreactivity at this time point. Two days after ozone, eosinophils in BAL, around airway nerves and in lungs, were decreased, and neuronal [M.sub.2] receptor function was normal, although animals were still hyperreactive to vagal stimulation. Depleting eosinophils with AbIL-5 prevented hyperreactivity, thus eosinophils contribute to vagal hyperreactivity by mechanisms separate from [M.sub.2] receptor blockade. Three days after ozone, vagal hyperreactivity persisted, eosinophils were again elevated in BAL in lungs and around nerves, and [M.sub.2] receptors were again dysfunctional. At this point, airway smooth muscle was also hyperresponsive to methacholine. Eosinophil depletion with AbIL-5, AbVLA-4, or cyclophosphamide protected [M.sub.2] function 3 days after ozone and prevented smooth muscle hyperreactivity. However, vagal hyperreactivity was significandy potentiated by eosinophil depletion. The site of hyperreactivity, muscle or nerve, changes over 3 days after a single exposure to ozone. Additionally, the role of eosinophils is complex; they mediate hyperreactivity acutely while chronically may be involved in repair. [M.sub.2] muscarinic receptors; vagus nerves

Published
2005

19. Intracellular chemical imaging of heme-containing enzymes involved in innate immunity using resonance Raman microscopy

Author

Manen, Henk-Jan van, Kraan, Yvonne M., Roos, Dirk, and Otto, Cees

Subjects
Eosinophils -- Research, Raman spectroscopy -- Usage, Coenzymes -- Research, Chemicals, plastics and rubber industries
Abstract

The visualization, by confocal Raman microscopy, of the intracellular distribution of two enzymes important in the immune eosinophil peroxidase (EPO) in eosinophils is reported. The effect of photobleaching of the Raman signal at 413.1 nm excitation on the reconstructed Raman images is discussed.

Published
2004

20. Role of Airway Eosinophilia and Eosinophil Activation in Sephadex-induced Inflammation

Author

Maghni, Karim, Nantel, Francois, Lanoue, Chantal, Cloutier, Solange, Cristol, Jean-Paul, Cadieux, Alain, and Sirois, Pierre

Subjects
Airway obstruction (Medicine) -- Research, Dextran -- Properties, Eosinophils -- Research, Guinea pigs -- Usage, Health
Abstract

Byline: Karim Maghni (1), Francois Nantel (2), Chantal Lanoue (1), Solange Cloutier (1), Jean-Paul Cristol (1), Alain Cadieux (1), Pierre Sirois (1,2) Keywords: airway inflammation; hyperresponsiveness; eosinophil; guinea-pig Abstract: The effects of an intravenous injection of Sephadex beads on lung eosinophil infiltration and eosinophil peroxydase activity and its relationship to bronchial hyperresponsiveness was examined in guinea pigs. This Sephadex beads injection led to blood, lung and airway eosinophilia in association with bronchial hyperresponsiveness. Histologic examination of the lower bronchus indicated that the eosinophil number increased markedly in the mucosa and submucosa. In addition, the eosinophils surrounding the bronchioles 1 day after the Sephadex injection migrated further in airway submucosa and mucosa 7 and 14 days after. Moreover, the bronchial hyperresponsiveness is observed without histologic evidence of airway epithelium damage. Therefore, the bronchial hyperresponsiveness seems to be more related to the eosinophil infiltration in the airway epithelium and possibly eosinophil activation rather than to the eosinophil number recovered in the BAL fluid. We conclude that the maintenance of hyperresponsiveness state could be associated with the persistence of blood and airway eosinophilia. Author Affiliation: (1) Institute of Pharmacology of Sherbrooke, Medical School, University of Sherbrooke, Sherbrooke, P.Q., Canada, J1H 5N4 (2) IPS Pharma, 3001 North 12th Avenue, Sherbrooke, P.Q., Canada, J1H 5N4 Article History: Registration Date: 20/12/2004

Published
2004

21. Case 19-2004: a 12-year-old boy with fatigue and eosinophilia

Author

Huang, Mary S. and Hasserjian, Robert P.

Subjects
Acute lymphocytic leukemia -- Research, Fatigue -- Research, Eosinophils -- Research
Abstract

The symptoms, and identification of eosinophilia are explained with the diagnosis report from a 12-year-old boy with fatigue and eosinophilia. The test report shows the presence of precursor B-cell acute lymphoblastic leukemia with eosinophilia and translocation.

Published
2004

22. Kinetic analysis of the reactions of hypobromous acid with protein components: implications for cellular damage and use of 30bromotyrosine as a marker of oxidative stress

Author

Pattison, David I. and Davies, Michael J.

Subjects
Macrophages -- Research, Eosinophils -- Research, Monocytes -- Research, Neutrophils -- Research, Biological sciences, Chemistry
Abstract

Hypophalous acids (HOX), which are produced by activated neutrophils, monocytes, eosinophils and possibly macrophages are crucial for immune response. However, excessive or misplaced generation can damage host tissues.

Published
2004

23. Interactions between electron and proton currents in excised patches from human eosinophils

Author

Petheo, Gabor L., Maturana, Andres, Spat, Andras, and Demaurex, Nicolas

Subjects
Eosinophils -- Physiological aspects, Eosinophils -- Research, Human physiology -- Research, Oxidases -- Physiological aspects, Oxidases -- Research, Biological sciences, Health
Abstract

The NADPH--oxidase is a plasma membrane enzyme complex that enables phagocytes to generate superoxide in order to kill invading pathogens, a critical step in the host defense against infections. The oxidase transfers electrons from cytosolic NADPH to extracellular oxygen, a process that requires concomitant [H.sup.+] extrusion through depolarization-activated [H.sup.+] channels. Whether [H.sup.+] fluxes are mediated by the oxidase itself is controversial, but there is a general agreement that the oxidase and [H.sup.+] channel are intimately connected. Oxidase activation evokes profound changes in whole-cell [H.sup.+] current ([I.sub.H]), causing an approximately--40-mV shift in the activation threshold that leads to the appearance of inward [I.sub.H]. To further explore the relationship between the oxidase and proton channel, we performed voltage-clamp experiments on inside-out patches from both resting and phorbol-12-myristate-13-acetate (PMA)-activated human eosinophils. Proton currents from resting cells displayed slow voltage-dependent activation, long-term stability, and were blocked by micromolar internal [[Zn.sup.2+]]. [I.sub.H] from PMA-treated cells activated faster and at lower voltages, enabling sustained [H.sup.+] influx, but ran down within minutes, regaining the current properties of nonactivated cells. Bath application of NADPH to patches excised from PMA-treated cells evoked electron currents ([I.sub.e]), which also ran down within minutes and were blocked by diphenylene iodonium (DPI). Run-down of both [I.sub.H] and [I.sub.e], was delayed, and sometimes prevented, by cytosolic ATP and GTP-[gamma]-S. A good correlation was observed between the amplitude of [I.sub.e] and both inward and outward [I.sub.H] when a stable driving force for [e.sup.-] was imposed. Combined application of NADPH and DPI reduced the inward [I.sub.H] amplitude, even in the absence of concomitant oxidase activity. The strict correlation between [I.sub.e] and [I.sub.H] amplitudes and the sensitivity of [I.sub.H] to oxidase-specific agents suggest that the proton channel is either part of the oxidase complex or linked by a membrane-limited mediator. KEY WORDS: physiology * NADPH-oxidase * zinc * phagocyte * patch-clamp

Published
2003

24. Eosinophil-induced release of acetylcholine from differentiated cholinergic nerve cells

Author

Sawatzky, Deborah A., Kingham, Paul J., Durcan, Niamh, McLean, W. Graham, and Costello, Richard W.

Subjects
Asthma -- Research, Eosinophils -- Research, Biological sciences
Abstract

One immunological component of asthma is believed to be the interaction of eosinophils with parasympathetic cholinergic nerves and a consequent inhibition of acetylcholine muscarinic [M.sub.2] receptor activity, leading to enhanced acetylcholine release and bronchoconstriction. Here we have used an in vitro model of cholinergic nerve function, the human IMR32 cell line, to study this interaction. IMR32 cells, differentiated in culture for 7 days, expressed M2 receptors. Cells were radiolabeled with [[sup.3]H]choline and electrically stimulated. The stimulation-induced release of acetylcholine was prevented by the removal of [Ca.sup.2+]. The muscarinic [M.sub.1]/[M.sub.2] receptor agonist arecaidine reduced the release of acetylcholine after stimulation (to 82 [+ or -] 2% of control at [10.sup.-7] M), and the [M.sub.2] receptor antagonist AF-DX 116 increased it (to 175 [+ or -] 23% of control at [10.sup.-5] M), indicating the presence of a functional [M.sub.2] receptor that modulated acetylcholine release. When human eosinophils were added to IMR32 cells, they enhanced acetylcholine release by 36 [+ or -] 10%. This effect was prevented by inhibitors of adhesion of the eosinophils to the IMR32 cells. Pretreatment of IMR32 cells with 10 mM carbachol, to desensitize acetylcholine receptors, prevented the potentiation of acetylcholine release by eosinophils or AF-DX 116. Acetylcholine release was similarly potentiated (by up to 45 [+ or -] 7%) by degranulation products from eosinophils that had been treated with N-formyl-methionyl-leucyl-phenylalanine or that had been in contact with IMR32 cells. Contact between eosinophils and IMR32 cells led to an initial increase in expression of [M.sub.2] receptors, whereas prolonged exposure reduced [M.sub.2] receptor expression. adhesion molecule; [M.sub.2] receptor; asthma

Published
2003

25. Effects of eosinophils on nerve cell morphology and development: the role of reactive oxygen species and p38 MAP kinase

Author

Kingham, Paul J., McLean, W. Graham, Walsh, Marie-Therese, Fryer, Allison D., Gleich, Gerald J., and Costello, Richard W.

Subjects
Neurons -- Research, Eosinophils -- Research, Biological sciences
Abstract

The adhesion of eosinophils to nerve cells and the subsequent release of eosinophil products may contribute to the pathogenesis of conditions such as asthma and inflammatory bowel disease. In this study we have separately examined the consequences of eosinophil adhesion and degranulation for nerve cell morphology and development. Eosinophils induced neurite retraction of cultured guinea pig parasympathetic nerves and differentiated IMR32 cholinergic neuroblastoma cells. Inhibition of eosinophil adhesion to IMR32 cells attenuated this retraction. Eosinophil adhesion to IMR32 cells led to tyrosine phosphorylation of a number of nerve cell proteins, activation of p38 MAP kinase, and generation of neuronal reactive oxygen species (ROS). Inhibition of tyrosine kinases with genistein prevented both the generation of ROS in the nerve cells and neurite retraction. The p38 MAP kinase inhibitor SB-239063 prevented neurite retraction but had no effect on the induction of ROS. Thus eosinophils induced neurite retraction via two distinct pathways: by generation of tyrosine kinase-dependent ROS and by p38 MAP kinase. Eosinophils also prevented neurite outgrowth during differentiation of IMR32 cells. In contrast to their effect on neurite retraction, this effect was mimicked by medium containing products released from eosinophils and by eosinophil major basic protein. These results indicate that eosinophils modify the morphology of nerve cells by distinct mechanisms that involve adhesion and released proteins. inflammation; cell adhesion molecule; cholinergic nerve; major basic protein

Published
2003

26. Possible Involvement of C-C Chemokines in Functional Augmentation of Adhesion Molecules in Asthmatic Patients

Author

Saito, N., Yamada, Y., Sannohe, S., Honda, K., Adachi, T., Kayaba, H., and Chihara, J.

Subjects
Asthma -- Research, Asthma -- Care and treatment, Cell adhesion molecules -- Research, Chemokines -- Research, Eosinophils -- Research
Abstract

Byline: N. Saito (), Y. Yamada (), S. Sannohe (), K. Honda (), T. Adachi (), H. Kayaba (), J. Chihara () Abstract: Adhesion molecules and C-C chemokines play an important role in the accumulation of eosinophils in allergic inflammation. In the present study, the expression and function of adhesion molecules on eosinophils from asthmatic patients and involvement of RANTES and eotaxin were examined. Eosinophils isolated by the CD16 negative selection method were stimulated with or without RANTES or eotaxin. Expression of b integrins on eosinophils and the functional adherence to recombinant soluble intercellular adhesion molecule-1 (r-sICAM-1)-coated plates were examined. Compared with normal subjects, eosinophils from asthmatic patients showed increased expression of b2 integrins and functional adherence to r-sICAM-1-coated plates. RANTES and eotaxin augmented the functional adherence of eosinophils without a significant upregulation of b2 integrins. Anti-b2 integrin antibody inhibited the augmentative effect on eosinophil adherence of RANTES and eotaxin. Pertussis toxin, wortmannin, and genistein inhibited chemokine-induced adherence. RANTES and eotaxin are closely related to eosinophil accumulation not only as chemotactic agents but also as augmentative agents for eosinophil adherence through involvement in functional eosinophil adherence to ICAM-1 by a possible qualitative change of b2 integrins. Pertussis toxin-sensitive G proteins, PI3 kinase, and tyrosine kinase are involved in signal transduction leading to activation of b2 integrins on eosinophil following stimulation with RANTES and eotaxin. Author Affiliation: () Department of Clinical and Laboratory Medicine, Akita University School of Medicine, 1-1-1 Hondo, Akita, Japan 010-8543, JP Article History: Accepted Date: 13/08/2002

Published
2002
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27. Functional Effects of Eotaxin Are Selectively Upregulated on IL-5 Transgenic Mouse Eosinophils

Author

Kudlacz, Elizabeth, Whitney, Carrie, Andresen, Catharine, and Conklyn, Maryrose

Subjects
Interleukin-5 -- Research, Interleukin-5 -- Physiological aspects, Inflammation -- Research, Chemokines -- Research, Chemokines -- Physiological aspects, Eosinophils -- Research, Health
Abstract

Byline: Elizabeth Kudlacz (1), Carrie Whitney (1), Catharine Andresen (1), Maryrose Conklyn (1) Keywords: Eosinophil; chemokine; lung; rodent; eotaxin; adhesion molecules Abstract: Synergistic interactions between cytokines, chemokines and adhesion molecules may facilitate the selective recruitment of eosinophils into sites of allergic inflammation. Ovalbumin-sensitized IL5TG mice responded to antigen challenge with robust airway eosinophilia 24 and 72 hr post-exposure. Adhesion molecule expression and functional responsiveness of immune cells derived from IL5TG mice to various inflammatory mediators were evaluated. IL5TG-derived eosinophils, but not neutrophils, expressed higher levels of CD49d and CD11b relative to WT. Functional responsiveness to eotaxin was increased in IL5TG eosinophils as demonstrated by a 10x increase in its potency in producing actin polymerization and 3x increase in CD11b upregulation relative to WT. These data are consistent with increased CCR3 expression on IL5TG eosinophils. Responsiveness of eosinophils to LTB4 or MIP-1[alpha] was similar between WT and IL-5TG mice. These data provide evidence of synergy between eosinophil-specific cytokines and chemokines that may promote accumulation of this cell type under conditions of allergic inflammation in vivo. Author Affiliation: (1) Pfizer Global Research and Development, Eastern Point Road, Groton, CT, 06340 Article History: Registration Date: 12/10/2004

Published
2002

28. Effects of an Eosinophil Chemotaxis Inhibitor, TAK-661, on Antigen-Induced Asthmatic Responses in Allergic Sheep

Author

Fujimoto, K., Tsunoda, T., Koizumi, T., and Kubo, K.

Subjects
Anti-inflammatory drugs -- Dosage and administration, Asthma -- Research, Asthma -- Care and treatment, Eosinophils -- Research
Abstract

Byline: K. Fujimoto (), T. Tsunoda (), T. Koizumi (), K. Kubo () Abstract: Eosinophils have been shown to play a role in allergen-induced airway responses. The aim in this study was to examine the effects of TAK-661, a newly developed product as a specific inhibitory agent of eosinophil chemotaxis, on antigen-induced asthmatic responses in allergic sheep model. Seven Ascaris-sensitive, "dual-respondent" allergic sheep were provocated by an Ascaris suum antigen or phosphate-buffered saline 2 hrs after intra-stomach administration of TAK-661 or a placebo. Pulmonary resistances were measured throughout the experiment, and airway responsiveness to methacholine, bronchoalveolar lavage (BAL), and histological examination were performed 8 hrs after the antigen challenge. Antigen provocation induced dual-phase bronchoconstriction, eosinophilia in BAL and eosinophil infiltration into the airway wall, and an increase in airway responsiveness in placebo-treated sheep. The administration of TAK-661 significantly reduced the bronchoconstriction during the late phase, along with the inhibition of eosinophilia in BAL and the eosinophil infiltration into the airway wall. TAK-661 had a tendency to reduce early-phase bronchoconstriction and airway hyperresponsiveness, but there were no significant differences. These findings suggest that the eosinophil accumulation into the airway induced by antigen provocation may contribute to the development of late-phase bronchoconstriction, however, the development of airway hyperresponsiveness during late asthmatic response may not always be due to only eosinophilic inflammation in the airway. Author Affiliation: () The First Department of Internal Medicine, Shinshu University School of Medicine, 3-1-1 Asahi, Matsumoto, 390 Japan, JP Article History: Accepted Date: 23/04/2002

Published
2002
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29. Thermal Injury Increases the Number of Eosinophil Progenitors in Rat Spleen and Bone Marrow

Author

Noel, J. Gregory, Wells, Denise A., Guo, Xialing, Kong, Fansheng, Lovell, Glenda J., and Ogle, Cora K.

Subjects
Burns and scalds -- Research, Eosinophils -- Research, Interleukins -- Research, Health
Abstract

Byline: J. Gregory Noel (1), Denise A. Wells (1), Xialing Guo (1), Fansheng Kong (2), Glenda J. Lovell (1), Cora K. Ogle (1,2) Keywords: Thermal injury; myelopoiesis; eosinophils; GM-CSF; IL-5 Abstract: We have investigated the effects of thermal injury upon myelopoiesis. IL-3, GM-CSF, and IL-5 were used to stimulate myeloid colony formation. IL-3 induces early myeloid progenitors and a more developed myeloid progenitor, the granulocyte-macrophage colony-forming unit (GM-CFU), to multiply and develop into mature myeloid cells. GM-CSF induces GM-CFU to become mature myeloid cells, while IL-5 induces eosinophil progenitors to become mature eosinophils. Stem Cell Factor (SCF) + IL-6 and FLT3 ligand, which have no effect on colony formation by themselves, were used to enhance the effects of IL-3 and GM-CSF, respectively. We found that thermal injury increased the number of early myeloid progenitors and GM-CFU in the spleen with either IL-3 or GM-CSF as a stimulant. Thermal injury increased the number of early myeloid progenitors in the bone marrow when GM-CSF, but not IL-3, was used to stimulate colony growth. Also, thermal injury increased the numbers of eosinophil progenitors in rat spleen and bone marrow and increased splenic levels of IL-5 mRNA. Author Affiliation: (1) Shriners Hospital for Children, Cincinnati, OH (2) Department of Surgery, University of Cincinnati, Cincinnati, OH Article History: Registration Date: 17/10/2004

Published
2001

30. Inhibitory Role of Eosinophils on Cell Surface Plasmin Generation by Bronchial Epithelial Cells: Inhibitory Effects of Transforming Growth Factor [beta]

Author

Hara, K., Hasegawa, T., Ooi, H., Koya, T., Tanabe, Y., Tsukada, H., Igarashi, K., Suzuki, E., Arakawa, M., and Gejyo, F.

Subjects
Asthma -- Care and treatment, Eosinophils -- Research, Thrombolytic drugs -- Research, Transforming growth factors -- Properties
Abstract

Byline: K. Hara (1), T. Hasegawa (1), H. Ooi (1), T. Koya (1), Y. Tanabe (1), H. Tsukada (1), K. Igarashi (1), E. Suzuki (1), M. Arakawa (1), F. Gejyo (1) Keywords: Key words: Eosinophil--Transforming growth factor [beta]--Plasmin--Plasminogen activator--Bronchial asthma. Abstract: Eosinophilic bronchitis is an essential component of bronchial asthma, and eosinophils play an important role. We studied the effect of eosinophils on cell surface plasmin generation by bronchial epithelial cells, because plasmin is thought to be involved in bronchial tissue repair/remodeling by means of fibrinolysis and the activation of proteases such as matrix metalloproteases. Plasmin was generated from exogenous plasminogen on the cell surface of cultured bronchial epithelial cells, NCI-H292. Transforming growth factor [beta] (TGF-[beta]) treatment resulted in reduced cell surface plasmin generation and a large increase in plasminogen activator inhibitor-type 1 (PAI-1) antigen production in NCI-H292 cells, whereas no conspicuous effects were observed with IL-1[beta] and TNF[alpha] treatment (regulators in pulmonary epithelial cells). On the other hand, this cell surface plasmin generation was reduced by co-incubation with Eol-1, an eosinophil cell line. The addition of TGF-[beta] antisense and anti-TGF-[beta] antibodies attenuated this adverse effect of Eol-1 cell co-incubation. These data suggest that eosinophils play an inhibitory role on cell surface plasmin generation by bronchial epithelial cells by means of the up-regulation of PAI-1 expression induced by TGF-[beta]. Therefore, the accumulation of eosinophils in bronchial walls is thought to be involved in bronchial tissue repair/remodeling in asthma through this protease network. Author Affiliation: (1) Department of Medicine (II), Niigata University School of Medicine, Niigata, Japan, JP Article note: Accepted for publication: 10 January 2001

Published
2001
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31. Effects of Several Glucocorticosteroids and PDE4 Inhibitors on Increases in Total Lung Eosinophil Peroxidase (EPO) Levels Following Either Systemic or Intratracheal Administration in Sephadexor Ovalbumin-induced Inflammatory Models

Author

Hammerbeck, David M., Mcgurran, Sean M., Radziszewski, Pam L., Egging, Elaine A., Johnson, David D., Hupperts, Ann M., and Gullikson, Gary W.

Subjects
Dextran -- Dosage and administration, Eosinophils -- Research, Corticosteroids -- Properties, Lung diseases -- Care and treatment, Peroxidase -- Properties, Health
Abstract

Byline: David M. Hammerbeck (1), Sean M. Mcgurran (1), Pam L. Radziszewski (1), Elaine A. Egging (1), David D. Johnson (1), Ann M. Hupperts (1), Gary W. Gullikson (1) Abstract: Representative glucocorticosteroids (GCS) and phosphodiesterase IV (PDE4) inhibitors were compared in several models of pulmonary inflammation ranging in severity. Lung tissue eosinophil peroxidase (EPO) levels rather than bronchoalveolar lavage fluid (BALF) EPO or eosinophil percentages were used to indicate eosinophil recruitment after intratracheal instillation of sephadex beads in rats or nebulized ovalbumin in sensitized guinea pigs. A single oral or intratracheal administration of a GCS was effective against mild and robust sephadex-induced eosinophilia whereas the PDE.sub.4 inhibitors evaluated appeared more effective in the milder sephadex models. The GCS were also more effective against sephadex-induced than ovalbumin-induced eosinophilia. The effectiveness of the GCS and PDE.sub.4 inhibitors improved when the severity of the ovalbumin-induced eosinophilia was decreased. Multiple day dosing also improved activity. These studies indicated that activity was influenced greatly by administration protocols, the severity of the inflammatory response and possibly the method used for estimating eosinophil recruitment. Author Affiliation: (1) 3M Pharmaceuticals, 3M Company, St. Paul, Minnesota, 55144 Article History: Registration Date: 09/10/2004

Published
2000

32. The Impact of Eotaxin- and IL-5-Induced Adhesion and Transmigration on Eosinophil Activity Markers

Author

Fernvik, Eva, Lundahl, Joachim, and Hallden, Gunilla

Subjects
Eosinophils -- Research, Asthma -- Research, Interleukins -- Research, Health
Abstract

Byline: Eva Fernvik (1), Joachim Lundahl (1), Gunilla Hallden (1) Abstract: Eosinophils accumulate at sites of allergic inflammation, and play important roles in asthma/allergic disorders. The mechanism of eosinophil recruitment into tissues is not fully understood. In this study, we evaluated whether adhesion and/or transmigration, in the presence of IL-5 and eotaxin, alter the expression of CD9, CD11b, the [beta].sub.1[alpha].sub.4-integrin, and the EG2-epitope on intracellular ECP. We also investigated whether CD9 is involved in the adhesion process. With flow cytometry the surface expression of CD9, CD11b and the [beta].sub.1[alpha].sub.4-integrin, and the intracellular expression of EG2, were analyzed before, and after transmigration/adhesion to fibronectin. To evaluate the eventual role of CD9 in adhesion, eosinophils were preincubated with monoclonal antibodies to CD9. We observed decreased expression of CD9, and increased expression of CD11b on eosinophils, after adhesion and transmigration. The transmigration did not change the expression of the [beta].sub.1[alpha].sub.4-integrin or EG2, whereas the adhesion resulted in a decreased EG2 expression. Antibodies to CD9 decreased the adhesion property of eosinophils. The eosinophils are activated after both adhesion and transmigration by means of decreased CD9 and increased CD11b expression. The expression of the EG2-epitope on intracellular ECP was decreased when eosinophils adhered to fibronectin, probably due to degranulation. Our results also indicate that CD9 is involved in the adhesion of eosinophils to fibronectin. Author Affiliation: (1) Department of Laboratory Medicine, Division of Clinical Immunology, Karolinska Hospital and Institute, Stockholm, Sweden Article History: Registration Date: 09/10/2004

Published
2000

33. Budesonide Down-Regulates Eosinophil Locomotion But Has No Effects on ECP Release or on [H.sub.2]O.sub.2 Production

Author

Lantero, S., Oddera, S., Silvestri, M., Gonzalez Rodriguez, R., Morelli, M.C., and Rossi, G.A.

Subjects
Asthma -- Research, Asthma -- Care and treatment, Corticosteroids -- Dosage and administration, Eosinophils -- Research
Abstract

Byline: S. Lantero (1), S. Oddera (1), M. Silvestri (1), R. Gonzalez Rodriguez (1), M. C. Morelli (2), G. A. Rossi (1) Keywords: Key words: Allergic asthma--T-lymphocytes--Cytokines--Granulocytes--Chemotaxis--Interleukin-5--Corticosteroids. Abstract: Treatment of allergic asthma with inhaled corticosteroids results in local down-regulation of proinflammatory cytokine synthesis and in marked decrease in tissue eosinophilia. Blood concentrations of inhaled corticosteroids, although significantly lower than those measured in the lung, may still have antiinflammatory effects on circulating eosinophils, reducing their ability to migrate. The aim of our study was to evaluate in vitro the activity of budesonide on blood eosinophils by measuring their chemotactic response, eosinophil cationic protein (ECP) release, and hydrogen peroxide ([H.sub.2]O.sub.2) production in the presence of different drug concentrations similar to those obtained at airway level (10.sup.-8 and 10.sup.-7 M) and at blood level (10.sup.-10 and 10.sup.-9 M). Partially purified blood eosinophils, isolated from 23 asthmatic subjects, were used to evaluate the activity of budesonide on: (1) chemotaxis toward the activated fifth component of complement (C5a, 0.1 ug/ml) or recombinant human (rh) interleukin (IL)-5 (200 pg/ml), (2) ECP release by cells stimulated with tetradecanoylphorbol acetate (TPA) and (3) [H.sub.2]O.sub.2 production by TPA-activated cells. The chemotactic response to C5a was down-regulated significantly by budesonide only by the highest concentrations tested (10.sup.-8 and 10.sup.-7 M) differently, budesonide was effective in inhibiting eosinophil migration toward rhIL-5, at all concentrations tested (p &lt 0.01, each comparison). By contrast, no drug-induced modifications were observed in ECP release or in [H.sub.2]O.sub.2 production (p &gt 0.05, each comparison). We conclude that concentrations of budesonide similar to those obtained in vivo are effective in inhibiting eosinophil locomotion but not in down-regulating the release of reactive oxygen species and granule-associated proteins. Author Affiliation: (1) Pulmonary Division, G. Gaslini Institute, Genoa, Italy, IT (2) Astra Farmaceutici, Milan, Italy, IT Article note: Accepted for publication: 11 February 1999

Published
1999
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34. Exhaled nitric oxide thresholds associated with a sputum eosinophil count (greater than or equal to) 3% in a cohort of unselected patients with asthma

Author

Schleich, Florence N., Seidel, Laurence, Sele, Jocelyne, Manise, Maite, Quaedvlieg, Valerie, Michils, Alain, and Louis, Renaud

Subjects
Asthma -- Diagnosis, Asthma -- Research, Nitric oxide -- Measurement, Nitric oxide -- Health aspects, Nitric oxide -- Research, Pulmonary function tests -- Methods, Pulmonary function tests -- Research, Eosinophils -- Measurement, Eosinophils -- Physiological aspects, Eosinophils -- Research, Cultures (Biology) -- Analysis, Health
Published
2010

35. Inflammatory subtypes in cough-variant asthma: association with maintenance doses of inhaled corticosteroids

Author

Matsuoka, Hirofumi, Niimi, Akio, Matsumoto, Hisako, Takemura, Masaya, Ueda, Tetsuya, Yamaguchi, Masafumi, Jinnai, Makiko, Inoue, Hideki, Ito, Isao, Chin, Kazuo, and Mishima, Michiaki

Subjects
Corticosteroids -- Dosage and administration, Corticosteroids -- Health aspects, Asthma -- Research, Asthma -- Physiological aspects, Asthma -- Drug therapy, Airway obstruction (Medicine) -- Research, Airway obstruction (Medicine) -- Physiological aspects, Airway obstruction (Medicine) -- Care and treatment, Eosinophils -- Research, Eosinophils -- Physiological aspects, Health
Published
2010

36. Schistosomal-derived lysophosphatidylcholine are involved in eosinophil activation and recruitment through toll-like receptor-2-dependent mechanisms

Author

Magalhaes, Kelly G., Almeida, Patricia E., Atella, Georgia C., Maya-Monteiro, Clarissa M., Castro-Faria-Neto, Hugo C., Pelajo-Machado, Marcelo, Lenzi, Henrique L., Bozza, Marcelo T., and Bozza, Patricia T.

Subjects
Schistosomiasis -- Development and progression, Schistosomiasis -- Research, Eosinophils -- Physiological aspects, Eosinophils -- Research, Phospholipids -- Physiological aspects, Phospholipids -- Research, Toll-like receptors -- Physiological aspects, Toll-like receptors -- Research, Health
Published
2010

37. Investigation of occupational asthma: sputum cell counts or exhaled nitric oxide?

Author

Lemiere, Catherine, D'Alpaos, Vinciane, Chaboillez, Simone, Cesar, Melanie, Wattiez, Mathieu, Chiry, Samah, and Vandenplas, Olivier

Subjects
Asthma -- Diagnosis, Asthma -- Care and treatment, Asthma -- Patient outcomes, Asthma -- Research, Cultures (Biology) -- Analysis, Eosinophils -- Measurement, Eosinophils -- Physiological aspects, Eosinophils -- Research, Pulmonary function tests -- Research, Health
Published
2010

38. Airway Eosinophilic Inflammation and Bronchial Hyperresponsiveness after Allergen Inhalation Challenge in Asthma

Author

Oddera, S., Silvestri, M., Penna, R., Galeazzi, G., Crimi, E., and Rossi, G. A.

Subjects
Allergens -- Properties, Asthma -- Research, Eosinophils -- Research
Abstract

Byline: S. Oddera (1), M. Silvestri (1), R. Penna (2), G. Galeazzi (2), E. Crimi (3), G. A. Rossi (1) Keywords: Key words: Eosinophils--Eosinophil cationic protein--Asthma--Atopy--Bronchial hyperresponsiveness--Methacholine--Bronchoalveolar lavage--Inflammation. Abstract: Allergen exposure in atopic asthmatic patients is associated with recruitment and activation of eosinophils in the airways. Once activated, eosinophils release toxic products, including the eosinophil cationic protein (ECP), able to damage bronchial structures and to increase bronchial hyperresponsiveness. With this background, the present study was designed to evaluate whether ECP levels in bronchoalveolar lavage (BAL) fluid could reflect, better than BAL eosinophil counts, the cellular activation that follows allergen exposure in atopic asthmatics. Twenty-two atopic patients attended the laboratory on two separate days. On the 1st day, they underwent methacholine (MCh) inhalation challenge to detect the degree of nonspecific bronchial hyperresponsiveness. On the 2nd day, they underwent fiberoptic bronchoscopy and BAL, at baseline or 4--6 h after allergen inhalation challenge. In this latter patient group, MCh challenge was repeated 3--5 h after allergen challenge, 1 h before fiberoptic bronchoscopy. The analysis of the mean baseline FEV.sub.1 values and the degree of bronchial reactivity to MCh (MCh Pd.sub.20) on the 1st study day did not demonstrate differences between the two patient groups (p &gt 0.1, each comparison). In addition, in the allergen-challenged group, MCh Pd.sub.20 was decreased significantly after allergen challenge (151.4 ug/ml and 67.6 ug/ml, respectively, before and after challenge p &lt 0.05). Evaluation of the different BAL cell types demonstrated that the proportions of eosinophils and epithelial cells were increased significantly in the allergen-challenged group compared with the group evaluated at baseline (p &lt 0.01 and p &lt 0.05, respectively). Moreover, ECP levels, corrected by the correspondent albumin levels (ECP/Alb), were higher in the allergen-challenged group compared with the group evaluated at baseline (p &lt 0.05). In addition, although a positive correlation was demonstrated between BAL eosinophil percentages and ECP/Alb values (r= 0.72, p &lt 0.05) in the group evaluated at baseline, no links were found between these parameters in the allergen-challenged group (p &gt 0.1). However, in this latter group, a weak positive correlation was demonstrated between eosinophil percentages and IMch, i.e., the increased nonspecific bronchial reactivity, which is observed after allergen challenge (r= 0.55 p &lt 0.05). Thus, in stable asthmatic patients an ongoing activation of eosinophils parallels their migration, but this eosinophilic inflammation is not strictly related to bronchial reactivity to Mch. By contrast, after allergen inhalation challenge, eosinophil recruitment and activation seem to follow different temporal kinetics, and eosinophilic inflammation may be partially associated with the degree of airway hyperresponsiveness. Author Affiliation: (1) Divisione di Pneumologia, Istituto G. Gaslini, Universita di Genova, Genova, Italy, IT (2) Laboratorio di Analisi, Istituto G. Gaslini, Universita di Genova, Genova, Italy, IT (3) Cattedra di Fisiopatologia Respiratoria, Universita di Genova, Genova, Italy, IT Article note: Accepted for publication: 15 September 1997

Published
1998
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39. Eotaxin Increases the Expression of CD11b/CD18 and Adhesion Properties in IL5, But Not fMLP-Prestimulated Human Peripheral Blood Eosinophils

Author

Lundahl, Joachim, Moshfegh, Ali, Gronneberg, Reidar, and Hallden, Gunilla

Subjects
Chemotaxis -- Analysis, Eosinophils -- Research, Eosinophils -- Chemical properties, Inflammation -- Research, Health
Abstract

Byline: Joachim Lundahl (1), Ali Moshfegh (1), Reidar Gronneberg (2), Gunilla Hallden (1) Abstract: A selective recruitment of eosinophils to sites of inflammation is claimed to be controlled by regulation of cytokines, chemokines and adhesion molecules. In animal models, eotaxin has been suggested to be a potent chemokine since it in cooperation with interleukin-5 induce selective chemotaxis and infiltration of eosinophils to lung tissue after an allergen provocation. We have investigated the in vitro effect of eotaxin on human peripheral blood eosinophils with respect to CD11b/CD18 expression and adhesion properties to the matrix protein fibronectin. We did not find any effect of eotaxin per se on CD11b/CD18 expression, neither on eosinophils from healthy subjects nor from patients with asymptomatic pollen related asthma. However, eotaxin significantly upregulated the quantitative level of CD11b/CD18 and increased the adhesion to fibronectin in eosinophils from healthy subjects preincubated in vitro with interleukin-5, but not in eosinophils preincubated with fMLP. Moreover, eosinophils harvested 24 hours after an in vivo allergen inhalation provocation in asthmatics, upregulated CD11b/CD18 after in vitro incubation with eotaxin alone. Author Affiliation: (1) Department of Laboratory Medicine, Division of Clinical Immunology, Karolinska Hospital, Sweden (2) Department of Medicine, Division of Respiratory and Allergic Diseases, Huddinge University Hospital, Karolinska Institute, Stockholm, Sweden Article History: Registration Date: 03/10/2004

Published
1998

41. Eicosanoids in exhaled breath condensate and BAL fluid of patients with sarcoidosis

Author

Piotrowski, Wojciech J., Antczak, Adam, Marczak, Jerzy, Nawrocka, Agnieszka, Kurmanowska, Zofia, and Gorski, Pawel

Subjects
Sarcoidosis -- Research, Sarcoidosis -- Physiological aspects, Sarcoidosis -- Diagnosis, Inflammation -- Diagnosis, Inflammation -- Physiological aspects, Eosinophils -- Research, Eosinophils -- Physiological aspects, Biological markers -- Usage, Oxidative stress -- Physiological aspects, Oxidative stress -- Research, Health
Published
2007

42. Repeated sputum inductions induce a transient neutrophilic and eosinophilic response

Author

van der Vaart, Hester, Postma, Dirkje S., Timens, Wim, Kauffman, Henk F., Hylkema, Machteld N., and ten Hacken, Nick H.T.

Subjects
Eosinophils -- Research, Eosinophils -- Physiological aspects, Neutrophils -- Research, Neutrophils -- Physiological aspects, Inflammation -- Research, Inflammation -- Diagnosis, Health
Published
2006

44. Interferon-γ up-regulates expression of Cysteinyl leukotriene type 2 receptors on eosinophils in asthmatic patients *

Author

Fujii, Masaru, Tanaka, Hiroshi, and Abe, Shosaku

Subjects
Asthmatics -- Care and treatment -- Research, Interferon gamma -- Research, Eosinophils -- Research, Health, Care and treatment, Research
Abstract

Study objectives: Cysteinyl leukotrienes (cysLTs) are strong bronchoeonstrietive mediators that play a key role in asthma inflammation. They act through specific receptors including cysLT type 1 receptor (CysLT1R) and cysLT [...]

Published
2005

45. Step-down compared to fixed-dose treatment with inhaled fluticasone propionate in asthma *

Author

Foresi, Antonio, Mastropasqua, Berardino, Chetta, Alfredo, D'Ippolito, Raffaele, Testi, Renato, Olivieri, Dario, and Pelucchi, Andrea

Subjects
Eosinophils -- Research, Fluticasone -- Dosage and administration -- Research, Inhaled medication -- Dosage and administration -- Research, Asthma -- Drug therapy -- Research, Health, Drug therapy, Research, Dosage and administration
Abstract

Background: Inhaled corticosteroids (ICSs) are an effective treatment of asthma even when administered at a low dose. Once asthma is controlled, current guidelines recommend that the dose of ICS be [...]

Published
2005

46. Calcium gradients underlying polarization and chemotaxis of eosinophils

Author

Brundage, Rodney A., Fogarty, Kevin E., Tuft, Richard A., and Fay, Fredric S.

Subjects
Eosinophils -- Research, Cell migration -- Research, Chemotaxis -- Research, Calcium, Dietary -- Research, Science and technology, Research
Abstract

The concentration of intracellular free calcium ([[Ca.sup.2+]]i) in polarized eosinophils was imaged during chemotaxis by monitoring fluorescence of the calcium-sensitive dye Fura-2 with a modified digital imaging microscope. Chemotactic stimuli caused [[Ca.sup.2+]]i to increase in a nonuniform manner that was related to cell activity. In cells moving persistently in one direction, [[Ca.sup.2+]]i was highest at the rear and lowest at the front of the cell. Before cells turned, [[Ca.sup.2+]]i transiently increased. The region of the cell that became the new leading edge had the lowest [[Ca.sup.2+]]i. These changes in [[Ca.sup.2+]]i provide a basis for understanding the organization and local activity of cytoskeletal proteins thought to underlie the directed migration of many cells., THE ABILITY OF CELLS TO MIGRATE toward a directional stimulus is a basic property of virtually all cells at some stage in their development [1] Directed migration results from the [...]

Published
1991

47. Mitochondrial missile defense

Author

Nizet, Victor and Rothenberg, Marc E.

Subjects
Eosinophils -- Health aspects, Eosinophils -- Research, Gastrointestinal diseases -- Risk factors, Gastrointestinal diseases -- Genetic aspects, Gastrointestinal diseases -- Care and treatment, Gastrointestinal diseases -- Research, Mitochondrial DNA -- Health aspects, Mitochondrial DNA -- Research
Abstract

A relatively obscure immune cell, the eosinophil, has a dramatic way of defending against pathogens. It rapidly ejects mitochondrial DNA, ensnaring bacteria and hastening their demise (pages 949-953). Eosinophils, a [...]

Published
2008

48. Data from Federal University of Rio de Janeiro Update Knowledge in Microbiology (Structural and Signaling Events Driving Aspergillus fumigatus-Induced Human Eosinophil Extracellular Trap Release)

Subjects
Medical research, Medicine, Experimental, Eosinophils -- Research, Immune response -- Research, Aspergillus -- Research, Biological sciences, Health
Abstract

2021 MAR 9 (NewsRx) -- By a News Reporter-Staff News Editor at Life Science Weekly -- A new study on microbiology is now available. According to news reporting originating from [...]

Published
2021

49. Eosinophils in asthma: remodeling a tangled tale

Author

Wills-Karp, Marsha and Karp, Christopher L.

Subjects
Eosinophils -- Research, Asthma -- Research -- Causes of, Science and technology, Research, Causes of
Abstract

The ongoing epidemic of allergic asthma in the developed world has lent urgency to the quest to understand the pathogenesis of this chronic, often debilitating, inflammatory disease. There is a [...]

Published
2004

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