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1. Sputum proteomic signature of gastro-oesophageal reflux in patients with severe asthma

Author

Tariq, K., Schofield, J.P.R., Nicholas, B.L., Burg, D., Brandsma, J., Bansal, A.T., Wilson, S.J., Lutter, R., Fowler, S.J., Bakke, Caruso, M., Dahlen, B., Horváth, I., Krug, N., Montuschi, P., Sanak, M., Sandström, T., Geiser, T., Pandis, I., Sousa, A.R., Adcock, I.M., Shaw, D.E., Auffray, C., Howarth, P.H., Sterk, P.J., Chung, K.F., Skipp, P.J., Dimitrov, B., and Djukanović, R.

Published
2019
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3. Mépolizumab réduit le besoin en chirurgie chez les patients avec polypose nasosinusienne (PNS)

Author

Fokkens, W.F., primary, Mullol, J.M., additional, Kennedy, D.K., additional, Philpott, C.P., additional, Seccia, V.S., additional, Kern, R.K., additional, Coste, A.C., additional, Sousa, A.S., additional, Howarth, P.H., additional, Benson, V.B., additional, Mayer, B.M., additional, Yancey, S.Y., additional, Chan, R.C., additional, Gane, S.G., additional, and Iaz-Chachuat, L.I.C., additional

Published
2022
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4. Plasma proteins elevated in severe asthma despite oral steroid use and unrelated to Type-2 inflammation

Author

Mikus, M.S. Kolmert, J. Andersson, L.I. Östling, J. Knowles, R.G. Gómez, C. Ericsson, M. Thörngren, J.-O. Khoonsari, P.E. Dahlén, B. Kupczyk, M. de Meulder, B. Auffray, C. Bakke, P.S. Beghe, B. Bel, E.H. Caruso, M. Chanez, P. Chawes, B. Fowler, S.J. Gaga, M. Geiser, T. Gjomarkaj, M. Horváth, I. Howarth, P.H. Johnston, S.L. Joos, G. Krug, N. Montuschi, P. Musial, J. Niżankowska-Mogilnicka, E. Olsson, H.K. Papi, A. Rabe, K.F. Sandström, T. Shaw, D.E. Siafakas, N.M. Uhlén, M. Riley, J.H. Bates, S. Middelveld, R.J.M. Wheelock, C.E. Chung, K.F. Adcock, I.M. Sterk, P.J. Djukanovic, R. Nilsson, P. Dahlén, S.-E. James, A. Ahmed, H. Balgoma, D. Bansal, A.T. Baribaud, F. Bigler, J. Billing, B. Bisgaard, H. Boedigheimer, M.J. Bønnelykke, K. Brandsma, J. Brinkman, P. Bucchioni, E. Burg, D. Bush, A. Chaiboonchoe, A. Checa, T. Compton, C.H. Corfield, J. Cunoosamy, D. D’Amico, A. Emma, R. Erpenbeck, V.J. Erzen, D. Fichtner, K. Fitch, N. Fleming, L.J. Formaggio, E. Frey, U. Gahlemann, M. Goss, V. Guo, Y.-K. Hashimoto, S. Haughney, J. Hedlin, G. Hekking, P.-P.W. Higenbottam, T. Hohlfeld, J.M. Holweg, C.T.J. Knox, A.J. Konradsen, J. Lazarinis, N. Lefaudeux, D. Li, T. Loza, M.J. Lutter, R. Manta, A. Masefield, S. Matthews, J.G. Mazein, A. Meiser, A. Miralpeix, M. Mores, N. Murray, C.S. Myles, D. Naz, S. Nordlund, B. Pahus, L. Pandis, I. Pavlidis, S. Postle, A. Powel, P. Rao, N. Reinke, S. Roberts, A. Roberts, G. Rowe, A. Schofield, J.P.R. Seibold, W. Selby, A. Sigmund, R. Singer, F. Sjödin, M. Skipp, P.J. Sousa, A.R. Sun, K. Thornton, B. Uddin, M. van Aalderen, W.M. van Geest, M. Vestbo, J. Vissing, N.H. Wagener, A.H. Wagers, S.S. Weiszhart, Z. Wheelock, C.E. Wheelock, Å. Wilson, S.J. Yasinska, V. Brusselle, G.G. Campbell, D.A. Contoli, M. Damm, K. de Rudder, I. Delin, I. Devautour, C. Duplaga, M. Eduards, M. Ek, A. Ekström, T. Figiel, E. Gaber, F. Gauw, S. Gawlewicz-Mroczka, A. Gerding, D. Haque, S. Hewitt, L. Hiemstra, P.S. Holgate, S.T. Holloway, J. Kania, A. Kanniess, F. Karlsson, Ö. Kips, J.C. Kumlin, M. Lantz, A.-S. Lazarinis, N. Magnussen, H. Mallia, P. Martling, I. Meziane, L. Oikonomidou, E. Olsson, M. Pace, E. Papadopouli, E. Papadopoulos, N. Plataki, M. Profita, M. Reinius, L.E. Richter, K. Robinson, D.S. Romagnoli, M. Samara, K. Schelfhout, V. Skedinger, M. Stamataki, E. ten Brinke, A. Vachier, I. Wallén-Nielsen, E. van Veen, I. Weersink, E. Wilson, S.J. Yasinska, V. Zervas, E. Ziolkowska-Graca, B. U-BIOPRED (Unbiased Biomarkers for the Prediction of Respiratory Disease outcome) Study Group BIOAIR (Longitudinal Assessment of Clinical Course Biomarkers in Severe Chronic Airway Disease) Consortium

Abstract

Rationale Asthma phenotyping requires novel biomarker discovery. Objectives To identify plasma biomarkers associated with asthma phenotypes by application of a new proteomic panel to samples from two well-characterised cohorts of severe (SA) and mild-to-moderate (MMA) asthmatics, COPD subjects and healthy controls (HCs). Methods An antibody-based array targeting 177 proteins predominantly involved in pathways relevant to inflammation, lipid metabolism, signal transduction and extracellular matrix was applied to plasma from 525 asthmatics and HCs in the U-BIOPRED cohort, and 142 subjects with asthma and COPD from the validation cohort BIOAIR. Effects of oral corticosteroids (OCS) were determined by a 2-week, placebo-controlled OCS trial in BIOAIR, and confirmed by relation to objective OCS measures in U-BIOPRED. Results In U-BIOPRED, 110 proteins were significantly different, mostly elevated, in SA compared to MMA and HCs. 10 proteins were elevated in SA versus MMA in both U-BIOPRED and BIOAIR (alpha-1-antichymotrypsin, apolipoprotein-E, complement component 9, complement factor I, macrophage inflammatory protein-3, interleukin-6, sphingomyelin phosphodiesterase 3, TNF receptor superfamily member 11a, transforming growth factor-β and glutathione S-transferase). OCS treatment decreased most proteins, yet differences between SA and MMA remained following correction for OCS use. Consensus clustering of U-BIOPRED protein data yielded six clusters associated with asthma control, quality of life, blood neutrophils, high-sensitivity C-reactive protein and body mass index, but not Type-2 inflammatory biomarkers. The mast cell specific enzyme carboxypeptidase A3 was one major contributor to cluster differentiation. Conclusions The plasma proteomic panel revealed previously unexplored yet potentially useful Type-2independent biomarkers and validated several proteins with established involvement in the pathophysiology of SA. © 2022 European Respiratory Society. All rights reserved.

Published
2022

5. Lung function fluctuation patterns unveil asthma and COPD phenotypes unrelated to type 2 inflammation

Author

Delgado-Eckert, E. James, A. Meier-Girard, D. Kupczyk, M. Andersson, L.I. Bossios, A. Mikus, M. Ono, J. Izuhara, K. Middelveld, R. Dahlén, B. Gaga, M. Siafakas, N.M. Papi, A. Beghe, B. Joos, G. Rabe, K.F. Sterk, P.J. Bel, E.H. Johnston, S.L. Chanez, P. Gjomarkaj, M. Howarth, P.H. Niżankowska-Mogilnicka, E. Dahlén, S.-E. Frey, U.

Subjects
respiratory system, respiratory tract diseases
Abstract

Background: In all chronic airway diseases, the dynamics of airway function are influenced by underlying airway inflammation and bronchial hyperresponsiveness along with limitations in reversibility owing to airway and lung remodeling as well as mucous plugging. The relative contribution of each component translates into specific clinical patterns of symptoms, quality of life, exacerbation risk, and treatment success. Objective: We aimed to evaluate whether subgrouping of patients with obstructive airway diseases according to patterns of fluctuation in lung function allows identification of specific phenotypes with distinct clinical characteristics. Methods: We applied the novel method of fluctuation-based clustering (FBC) to twice-daily FEV1 measurements recorded over a 1-year period in a mixed group of 134 adults with mild-to-moderate asthma, severe asthma, or chronic obstructive pulmonary disease from the European BIOAIR cohort. Results: Independently of clinical diagnosis, FBC divided patients into 4 fluctuation-based clusters with progressively increasing alterations in lung function that corresponded to patterns of increasing clinical severity, risk of exacerbation, and lower quality of life. Clusters of patients with airway disease with significantly elevated levels of biomarkers relating to remodeling (osteonectin) and cellular senescence (plasminogen activator inhibitor-1), accompanied by a loss of airway reversibility, pulmonary hyperinflation, and loss of diffusion capacity, were identified. The 4 clusters generated were stable over time and revealed no differences in levels of markers of type 2 inflammation (blood eosinophils and periostin). Conclusion: FBC-based phenotyping provides another level of information that is complementary to clinical diagnosis and unrelated to eosinophilic inflammation, which could identify patients who may benefit from specific treatment strategies or closer monitoring. © 2021

Published
2021

6. Airway Elastin is increased in severe asthma and relates to proximal wall area: Histological and computed tomography findings from the U-BIOPRED severe asthma study

Author

Wilson, S.J., Ward, J.A., Pickett, H.M., Baldi, S., Sousa, A.R., Sterk, P.J., Chung, K.F., Djukanovic, R., Dahlen, B., Billing, B., Shaw, D., Krug, N., Sandström, T., Brightling, C., Howarth, P.H., and Publica

Abstract

Background Airway remodelling, which may include goblet cell hyperplasia / hypertrophy, changes in epithelial integrity, accumulation of extracellular matrix components, smooth muscle hypertrophy and thickening of the lamina reticularis, is a feature of severe asthma and contributes to the clinical phenotype. Objective Within the U-BIOPRED severe asthma study, we have assessed histological elements of airway remodelling and their relationship to computed tomography (CT) measures of proximal airway dimensions. Methods Bronchial biopsies were collected from two severe asthma groups, one non-smoker (SAn, n = 28) and one current/ex-smoker (SAs/ex, n = 13), and a mild-moderate asthma group (MMA, n = 28) classified and treated according to GINA guidelines, plus a healthy control group (HC, n = 33). Movat's pentachrome technique was used to identify mucin, elastin and total collagen in these biopsies. The number of goblet cells (mucin+) was counted as a percentage of the total number of epithelial cells and the percentage mucin epithelial area measured. The percentage area of elastic fibres and total collagen within the submucosa was also measured, and the morphology of the elastic fibres classified. Participants in the asthma groups also had a CT scan to assess large airway morphometry. Results The submucosal tissue elastin percentage was higher in both severe asthma groups (16.1% SAn, 18.9% SAs/ex) compared with the HC (9.7%) but did not differ between asthma groups. There was a positive relationship between elastin and airway wall area measured by CT (n = 18-20, rho=0.544, p = 0.024), which also related to an increase in elastic fibres with a thickened lamellar morphological appearance. Mucin epithelial area and total collagen were not different between the four groups. Due to small numbers of suitable CT scans, it was not feasible to compare airway morphometry between the asthma groups. Conclusion These findings identify a link between extent of elastin deposition and airway wall thickening in severe asthma.

Published
2021

8. Pharmacotherapy and airway remodelling in asthma? (Occasional Review)

Author

Beckett, P.A. and Howarth, P.H.

Subjects
Respiratory insufficiency -- Physiological aspects -- Drug therapy, Respiratory physiology -- Physiological aspects -- Analysis, Asthma -- Drug therapy -- Physiological aspects, Health, Drug therapy, Analysis, Physiological aspects
Abstract

Over the last few decades attention has largely focused on airway inflammation in asthma, but more recently it has been appreciated that there are important structural airway changes which have [...]

Published
2003

9. Functional Translation of IL33 Locus Polymorphisms Into Altered Epithelial Cell Function Underlying Asthma

Author

Ketelaar, M., primary, Portelli, M.A., additional, Dijk, F.N., additional, Faiz, A., additional, Shrine, N., additional, Hankinson, J., additional, Bhaker, S., additional, Henry, A.P., additional, Billington, C.K., additional, Shaw, D., additional, Johnson, S.R., additional, Benest, A.V., additional, Pogson, Z.E.K., additional, Fogarty, A., additional, McKeever, T.M., additional, Singapuri, A., additional, Heaney, L., additional, Mansur, A., additional, Gaudhuri, R., additional, Thomson, N.C., additional, Holloway, J.W., additional, Lockett, G.A., additional, Howarth, P.H., additional, Niven, R., additional, Simpson, A., additional, Tobin, M.D., additional, Postma, D.S., additional, Hall, I.P., additional, Wain, L.V., additional, Brightling, C.E., additional, Obeidat, M., additional, Sin, D.D., additional, van den Berge, M., additional, Koppelman, G.H., additional, Sayers, I., additional, and Nawijn, M.C., additional

Published
2019
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10. Mucosal inflammation in asthma

Author

Djukanovic, R., Roche, W.R., Wilson, J.W., Beasley, C.R.W., Twentyman, O.P., Howarth, P.H., and Holgate, S.T.

Subjects
Inflammation -- Mediators, Inflammation -- Physiological aspects, Asthma -- Physiological aspects, Health
Abstract

One of the major features of asthma is inflammation of the airways. The disease processes resulting in asthma have previously been studied by measuring the responsiveness of the bronchi (airways) and mediators (factors causing allergic reactions). With the use of improved diagnostic methods, the disease mechanisms and inflammatory changes in asthma can now be studied where they occur. Bronchoalveolar lavage (BAL), which is used to obtain fluids from the lungs for diagnostic purposes, has demonstrated the presence of various types of cells, such as mast cells and eosinophils, which contribute to inflammation and increased airway responsiveness. Endobronchial biopsies have yielded results consistent with autopsy findings and shown varying degrees of inflammation in living asthmatics. Tissue microscopic findings are consistent with the presence of chronic inflammation in bronchial asthma. Exposure to allergy-causing agents is associated with bronchial hyperresponsiveness and increased levels of inflammatory cells and mediators in the mucous tissue lining the airways. However, the activation of inflammatory cells by mediators in addition to the presence of these cells in the airways must be demonstrated to confirm their role in inflammation associated with asthma. Mast cells, eosinophils, neutrophils, macrophages, platelets, and lymphocytes have all been implicated in the disease process of mucosal inflammation in asthma, although the most important contributor to the disease process has not been identified. The possible roles of each of these cells is discussed. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

11. temperature-controlled laminar airflow in severe asthmas for exacerbation reduction (The LASER Trial)

Author

Storrar, W., Fogg, C., Brown, T., Dennison, P., Yu, L.M., Dewey, A., Luengo-Fernandez, R., Dean, T., Rahman, N., Mansur, A., Howarth, P.H., Bradding, P., and Chauhan, A.J.

Subjects
respiratory tract diseases
Abstract

Background: Asthma affects more than 5 million patients in the United Kingdom. Nearly 500,000 of these patients have severe asthma with severe symptoms and frequent exacerbations that are inadequately controlled with available treatments. The burden of severe asthma on the NHS is enormous, accounting for 80 % of the total asthma cost (£1 billion), with frequent exacerbations and expensive medications generating much of this cost.Of those patients with severe asthma, 70 % are sensitised to indoor aeroallergens, and the level of exposure to allergens determines the symptoms; patients exposed to high levels are therefore most at risk of exacerbations and hospital admissions.The LASER trial aims to assess whether a new treatment, temperature controlled laminar airflow (TLA) delivered by the Airsonett™ device, can reduce the frequency of exacerbations in patients with severe allergic asthma by reducing exposure to aeroallergens overnight.Methods: This multicentre study is a placebo-controlled, blinded, randomised controlled, parallel group trial. A total of 222 patients with a new or current diagnosis of severe allergic asthma will be assigned with a random element in a 1:1 ratio to receive either an active device for one year or a placebo device. The primary outcome is the frequency of severe asthma exacerbations occurring over a 12-month period, defined in accordance with the American Thoracic Society/European Respiratory Society (ATS/ERS) guidelines. Secondary outcomes include changes in asthma control, lung function, asthma-specific and global quality of life for participants and their carers, adherence to intervention, healthcare resource use and costs, and cost-effectiveness. Qualitative interviews will be conducted to elicit participant’s and their partner’s perceptions of the treatment.Discussion: Effective measures of allergen avoidance have, to date, proved elusive. The LASER trial aims to address this. The study will ascertain whether home-based nocturnal TLA usage over a 12-month period can reduce the frequency of exacerbations and improve asthma control and quality of life as compared to placebo, whilst being cost-effective and acceptable to adults with poorly controlled, severe allergic asthma. The results of this study will be widely applicable to the many patients with allergic asthma both in the UK and internationally.Trial registration: Current controlled trials ISRCTN46346208 (Date assigned 22 January 2014).

Published
2016

12. Increased YKL-40 and chitotriosidase in asthma and chronic obstructive pulmonary disease

Author

James, A.J. Reinius, L.E. Verhoek, M. Gomes, A. Kupczyk, M. Hammar, U. Ono, J. Ohta, S. Izuhara, K. Bel, E. Kere, J. Söderhäll, C. Dahlén, B. Boot, R.G. Dahlén, S.-E. Gaga, M. Siafakas, N.M. Papi, A. Fabbri, L.M. Joos, G. Brusselle, G. Rabe, K.F. Kanniess, F. Hiemstra, P. Johnston, S.L. Chanez, P. Vachier, I. Gjomarkaj, M. Sterk, P.J. Howarth, P.H. Nizankowska-Mogilnicka, E. Middelveld, R. Holgate, S.T. Wilson, S.

Subjects
respiratory tract diseases
Abstract

Rationale: Serum chitinases may be novel biomarkers of airway inflammation and remodeling, but less is known about factors regulating their levels. Objectives: To examine serum chitotriosidase activity and YKL-40 levels in patients with asthma and chronic obstructive pulmonary disease (COPD) and evaluate clinically relevant factors that may affect chitinase levels, including genetic variability, corticosteroid treatment, disease exacerbations, and allergen exposure. Methods: Serum chitotriosidase (CHIT1) activity and YKL-40 (CHI3L1) levels, as well as the CHIT1 rs3831317 and CHI3L1 rs4950928 genotypes, were examined in subsets of patients with mild to moderate asthma (n = 76), severe asthma (n = 93), and COPD (n = 64) taking part in the European multicenter BIOAIR (Longitudinal Assessment of Clinical Course and Biomarkers in Severe Chronic Airway Disease) study. Blood was obtained at baseline, before and after a 2-week oral steroid intervention, up to six times during a 1-year period, and during exacerbations. Baseline chitinase levels were also measured in 72 healthy control subjects. The effect of allergen inhalation on blood and sputum YKL-40 levels was measured in two separate groups of patients with mild atopic asthma; one group underwent repeated low-dose allergen challenge (n = 15), and the other underwent high-dose allergen challenge (n = 16). Measurements and Main Results: Serum chitotriosidase and YKL-40 were significantly elevated in patients with asthma and those with COPD compared with healthy control subjects. Genotype and age strongly affected both YKL-40 and chitotriosidase activity, but associations with disease remained following adjustment for these factors. Correlations were observed with lung function but not with other biomarkers, including exhaled nitric oxide, blood eosinophils, periostin, and IgE. Generally, acute exacerbations, allergen-induced airway obstruction, and corticosteroid treatment did not affect circulating chitinase levels. Conclusions: YKL-40 and chitotriosidase are increased in asthma and more so in COPD. The data in the present study support these substances as being relatively steroid-insensitive, non-T-helper cell type 2-type biomarkers distinctly related to chronic inflammatory disease processes. Copyright © 2016 by the American Thoracic Society.

Published
2016

13. MACVIA clinical decision algorithm in adolescents and adults with allergic rhinitis

Author

Bousquet, J. Schünemann, H.J. Hellings, P.W. Arnavielhe, S. Bachert, C. Bedbrook, A. Bergmann, K.-C. Bosnic-Anticevich, S. Brozek, J. Calderon, M. Canonica, G.W. Casale, T.B. Chavannes, N.H. Cox, L. Chrystyn, H. Cruz, A.A. Dahl, R. De Carlo, G. Demoly, P. Devillier, P. Dray, G. Fletcher, M. Fokkens, W.J. Fonseca, J. Gonzalez-Diaz, S.N. Grouse, L. Keil, T. Kuna, P. Larenas-Linnemann, D. Lodrup Carlsen, K.C. Meltzer, E.O. Mullol, J. Muraro, A. Naclerio, R.N. Palkonen, S. Papadopoulos, N.G. Passalacqua, G. Price, D. Ryan, D. Samolinski, B. Scadding, G.K. Sheikh, A. Spertini, F. Valiulis, A. Valovirta, E. Walker, S. Wickman, M. Yorgancioglu, A. Haahtela, T. Zuberbier, T. Aberer, W. Adachi, M. Agache, I. Akdis, C. Akdis, M. Annesi-Maesano, I. Ansotegui, I.J. Anto, J.M. Arshad, S.H. Baiardini, I. Baigenzhin, A.K. Barbara, C. Bateman, E.D. Beghé, B. Bel, E.H. Ben Kheder, A. Bennoor, K.S. Benson, M. Bernstein, D. Michael, B. Thomas, B. Bindslev-Jensen, C. Bjermer, L. Blain, H. Boner, A. Bonini, M. Bonini, S. Bosse, I. Bouchard, J. Boulet, L.-P. Bourret, R.A. Bousquet, P.J. Braido, F. Briggs, A.H. Brightling, C.E. Buhl, R. Burney, P. Bush, A. Caballero-Fonseca, F. Caimmi, D.P. Camargos, P. Camuzat, T. Carlsen, K.-H. Carr, W. Casale, T.B. Sarabia, A.C. Chatzi, L. Chen, Y. Chiron, R. Chkhartishvili, E. Chuchalin, A. Ciprandi, G. Cirule, I. Correia de Sousa, J. Costa, D. Crooks, G. Custovic, A. Dahlen, S.-E. Darsow, U. De Blay, F. De Manuel Keenoy, E. Dedeu, T. Deleanu, D. Denburg, J. Didier, A. Dinh-Xuan, A.-T. Dokic, D. Douagui, H.B. Dubakiene, R. Durham, S. Dykewicz, M. El-Gamal, Y. Emuzyte, R. Fink-Wagner, A. Fiocchi, A. Forastiere, F. Gamkrelidze, A. Gemicioğlu, B. Gereda, J.E. Gerth van Wijk, R. Gotua, M. Grisle, I. Guzmán, M.A. Haahtela, T. Heinrich, J. Hellquist-Dahl, B. Horak, F. Howarth, P.H. Humbert, M. Hyland, M. Ivancevich, J.-C. Jares, E.J. Johnston, S.L. Jonquet, O. Joos, G. Jung, K.-S. Just, J. Jutel, M. Kaidashev, I.P. Khaitov, M. Kalayci, O. Kalyoncu, F. Keith, P. Khaltaev, N. Kleine-Tebbe, J. Klimek, L. N'Goran, B.K. Kolek, V. Koppelman, G.H. Kowalski, M. Kull, I. Kvedariene, V. Lambrecht, B. Lau, S. Laune, D. Le Thi Tuyet, L. Li, J. Lieberman, P. Lipworth, B.J. Renaud, L. Magard, Y. Magnan, A. Mahboub, B. Majer, I. Makela, M. Manning, P.J. Masjedi, M.R. Maurer, M. Mavale-Manuel, S. Melén, E. Melo-Gomes, E. Mercier, J. Merk, H. Miculinic, N. Mihaltan, F. Milenkovic, B. Mohammad, Y. Molimard, M. Momas, I. Montilla-Santana, A. Morais-Almeida, M. Mösges, R. Nadif, R. Namazova-Baranova, L. Neffen, H. Nekam, K. Neou, A. Niggemann, B. Nyembue, D. O'Hehir, R. Ohta, K. Okamoto, Y. Okubo, K. Ouedraogo, S. Paggiaro, P.-L. Pali-Schöll, I. Palmer, S. Panzner, P. Papi, A. Park, H.-S. Pavord, I. Pawankar, R. Pfaar, O. Picard, R. Pigearias, B. Pin, I. Plavec, D. Pohl, W. Popov, T. Postma, D.S. Potter, P. Poulsen, L.K. Rabe, K.F. Raciborski, F. Pontal, F.R. Reitamo, S. Repka-Ramirez, M.-S. Robalo-Cordeiro, C. Roberts, G. Rodenas, F. Rolland, C. Rodriguez, M.R. Romano, A. Rosado-Pinto, J. Rosario, N.A. Rosenwasser, L. Rottem, M. Sanchez-Borges, M. Sastre-Dominguez, J. Schmid-Grendelmeier, P. Serrano, E. Simons, F.E.R. Sisul, J.-C. Skrindo, I. Smit, H.A. Solé, D. Sooronbaev, T. Spranger, O. Stelmach, R. Strandberg, T. Sunyer, J. Thijs, C. Todo-Bom, A.-M. Triggiani, M. Valenta, R. Valero, A.L. van Hage, M. Vandenplas, O. Vezzani, G. Vichyanond, P. Viegi, G. Wagenmann, M. Wahn, U. De Yun, W. Williams, D. Wright, J. Yawn, B.P. Yiallouros, P. Yusuf, O.M. Zar, H.J. Zernotti, M. Zhang, L. Zhong, N. Zidarn, M.

Abstract

The selection of pharmacotherapy for patients with allergic rhinitis (AR) depends on several factors, including age, prominent symptoms, symptom severity, control of AR, patient preferences, and cost. Allergen exposure and the resulting symptoms vary, and treatment adjustment is required. Clinical decision support systems (CDSSs) might be beneficial for the assessment of disease control. CDSSs should be based on the best evidence and algorithms to aid patients and health care professionals to jointly determine treatment and its step-up or step-down strategy depending on AR control. Contre les MAladies Chroniques pour un VIeillissement Actif en Languedoc-Roussillon (MACVIA-LR [fighting chronic diseases for active and healthy ageing]), one of the reference sites of the European Innovation Partnership on Active and Healthy Ageing, has initiated an allergy sentinel network (the MACVIA-ARIA Sentinel Network). A CDSS is currently being developed to optimize AR control. An algorithm developed by consensus is presented in this article. This algorithm should be confirmed by appropriate trials. © 2016 The Authors

Published
2016

15. Frequent exacerbators - a distinct phenotype of severe asthma

Author

Kupczyk, M. ten Brinke, A. Sterk, P.J. Bel, E.H. Papi, A. Chanez, P. Nizankowska-Mogilnicka, E. Gjomarkaj, M. Gaga, M. Brusselle, G. Dahlén, B. Dahlén, S.-E. Weersink, E. Papadopoulos, N. Oikonomidou, E. Zervas, E. Contoli, M. Pauwels, R.A. Joos, G.F. de Rudder, I. Schelfhout, V. Richter, K. Gerding, D. Magnussen, H. Siafakas, N.M. Tzortzaki, E. Samara, K. Plataki, M. Papadopouli, E. Szczeklik, A. Ziolkowska-Graca, B. Kania, A. Gawlewicz-Mroczka, A. Duplaga, M. Figiel, E. Rabe, K.F. Hiemstra, P.S. Gauw, S. van Veen, I. Kips, J.C. Johnston, S.L. Mallia, P. Campbell, D.A. Robinson, D.S. Kanniess, F. Fabbri, L.M. Romagnoli, M. Vachier, I. Devautour, C. Meziane, L. Vignola, A.M. Pace, E. Profita, M. Holgate, S.T. Howarth, P.H. Wilson, S.J. Hewitt, L. Holoway, J.

Abstract

Background: Exacerbations represent a major source of morbidity and mortality in asthma and are a prominent feature of poorly controlled, difficult-to-treat disease. Objective: The goal of our study was to provide a detailed characterization of the frequent exacerbator phenotype and to identify risk factors associated with frequent and seasonal exacerbations. Methods: Ninety-three severe asthmatics (SA) and 76 mild-to-moderate patients (MA) were screened and prospectively followed up for 1 year (NCT00555607). Medical history, baseline clinical data and biomarkers were used to assess risk factors for frequent exacerbations. Results: During the study, 104 exacerbations were recorded in the SA group and 18 in the MA. Frequent exacerbators were characterized by use of higher doses of inhaled (1700 vs. 800 μg) and oral (6.7 vs. 1.7 mg) glucocorticosteroids, worse asthma control (ACQ score 2.3 vs. 1.4), lower quality of life (SGRQ score 48.5 vs. 33.3), higher sputum eosinophils (25.7% vs. 8.2%) and a more rapid decline in FEV1/FVC ratio (-0.07 vs. -0.01 ΔFEV1/FVC, frequent vs. non-frequent, respectively, P 45 p.p.b. and a history of smoking were associated with an increased risk of frequent exacerbations (odds ratios: 4.32 and 2.90 respectively). Conclusion and Clinical Relevance: We were able to distinguish and characterize a subphenotype of asthma subjects - frequent exacerbators - who are significantly more prone to exacerbations. Patients with FeNO > 45 p.p.b. and a history of smoking are at increased risk of frequent exacerbations and require careful monitoring in clinical practice. © 2013 John Wiley & Sons Ltd.

Published
2014

16. U-BIOPRED asthma cohort: Inflammatory markers and corticosteroid use

Author

Gibeon, D., Wagener, A.H., Yang, X., Sousa, A.R., Corfield, J., Shaw, D.E., Fowler, S., Flemming, L.J., Jeyasingham, E., Rowe, A., Fichtner, K., Robberts, G., Bakke, P., Singer, T., Geiser, T., Frey, U., Horvarth, I., Polosa, R., Bonnelykke, K., Krug, Norbert, Middelveld, R., Dahlen, S.-E., Dahlen, B., Hedlin, G., Hashimoto, S., Nordlund, B., Musial, J., Woodcock, A., Murray, C.S., Pahus, L., Myles, D., Compton, C., Higenbottam, T.W., Montuschi, P., Vestbo, J., Larsson, L., Sandstrom, T., Bisgaard, H., Wagers, S.S., Howarth, P.H., Bel, E.H., Djukanovic, R., Sterk, P.J., Chung, K.F., and Publica

Abstract

Rationale: U-BIOPRED, a European public-private collaboration, aims to subphenotype severe asthma using a systems medicine approach to describe its handprint. Methods: An interim analysis of the characteristics and inflammatory markers of severe asthma defined according to Thorax 2011; 66: 910 is presented. (TABLE SEE LINKED PDF-FILE) NA: not available Results: The adult severe asthma cohort had chronic airflow obstruction, with higher sputum eosinophils (SpE) compared to moderate asthma. The school-age severe asthma cohort had no evidence of obstruction but higher FeNO levels than moderate asthma. Pre-bronchodilator FEV1 (% pred) in adults inversely correlated with SpE and neutrophils, while SpE positively correlated with FeNO. In children, preBD FEV1 inversely correlated with FeNO. Analysis of the adult cohort according to use of maintenance prednisolone showed that this subphenotype was associated with lower IgE and blood eosinophil level, but similar SpE and FeNO. Conclusions: Severe asthma patients characterised by high SpE and FeNO despite high corticosteroid therapy, represents a steroid-insensitive subgroup. Analysis of associated lipidomic, transcriptomic and proteomic data will provide a better handprint.

Published
2013

17. Detection of exacerbations in asthma based on electronic diary data: Results from the 1-year prospective BIOAIR study

Author

Kupczyk, M. Haque, S. Sterk, P.J. Nizankowska-Mogilnicka, E. Papi, A. Bel, E.H. Chanez, P. Dahlén, B. Gaga, M. Gjomarkaj, M. Howarth, P.H. Johnston, S.L. Joos, G.F. Kanniess, F. Tzortzaki, E. James, A. Middelveld, R.J.M. Dahlén, S.-E.

Abstract

Background Objective measures are required that may be used as a proxy for exacerbations in asthma. The aim was to determine the sensitivity and specificity of electronic diary data to detect severe exacerbations (SEs) of asthma. A secondary aim was to identify phenotypic variables associated with a higher risk of exacerbation. Methods In the BIOAIR study, 169 patients with asthma (93 severe (SA); 76 mild to moderate (MA)) recorded lung function, symptoms and medication use in electronic diaries for 1 year. Data were analysed using receiver-operator characteristics curves and related to physician-diagnosed exacerbations. Medical history and baseline clinical data were used to assess risk of exacerbation. Results Of 122 physician-diagnosed exacerbations, 104 occurred in the SA group (1.1 per patient/year), 18 in the MA group (0.2 per patient/year) and 63 were severe using American Thoracic Society/European Respiratory Society criteria. During exacerbations, peak expiratory flow (PEF) and forced expiratory volume in 1 s significantly decreased, whereas day and night symptoms significantly increased. An algorithm combining a 20% decrease in PEF or a 20% increase in day symptoms on 2 consecutive days was able to detect SEs with 65% sensitivity and 95% specificity. The strongest risk factors for SEs were low Asthma Control Questionnaire score, sputum eosinophils ≥3%, body mass index >25 and low quality of life (St George's Respiratory Questionnaire), with ORs between 3.61 and 2.22 ( p

Published
2013

18. Genome-wide association study to identify genetic determinants of severe asthma

Author

Wan, Y.I., Shrine, N.R.G., Soler Artigas, M., Wain, L.V., Blakey, J.D., Moffatt, M.F., Bush, A., Chung, K. F., Cookson, W.O.C.M., Strachan, D.P., Heaney, L., Al-Momani, B.A.H., Mansur, A.H., Manney, S., Thomson, N.C., Chaudhuri, R., Brightling, C.E., Bafadhel, M., Singapuri, A., Niven, R., Simpson, A., Holloway, J.W., Howarth, P.H., Hui, J., Musk, A.W., James, A.L., Brown, M.A., Baltic, S., Ferreira, M.A.R., Thompson, P.J., Tobin, M.D., Sayers, Ian, and Hall, Ian P.

Abstract

Background The genetic basis for developing asthma has been extensively studied. However, association studies to date have mostly focused on mild to moderate disease and genetic risk factors for severe asthma remain unclear.Objective To identify common genetic variants affecting susceptibility to severe asthma.Methods A genome-wide association study was undertaken in 933 European ancestry individuals with severe asthma based on Global Initiative for Asthma (GINA) criteria 3 or above and 3346 clean controls. After standard quality control measures, the association of 480 889 genotyped single nucleotide polymorphisms (SNPs) was tested. To improve the resolution of the association signals identified, non-genotyped SNPs were imputed in these regions using a dense reference panel of SNP genotypes from the 1000 Genomes Project. Then replication of SNPs of interest was undertaken in a further 231 cases and 1345 controls and a meta-analysis was performed to combine the results across studies.Results An association was confirmed in subjects with severe asthma of loci previously identified for association with mild to moderate asthma. The strongest evidence was seen for the ORMDL3/GSDMB locus on chromosome 17q12-21 (rs4794820, p=1.03×10(−8) following meta-analysis) meeting genome-wide significance. Strong evidence was also found for the IL1RL1/IL18R1 locus on 2q12 (rs9807989, p=5.59×10(−8) following meta-analysis) just below this threshold. No novel loci for susceptibility to severe asthma met strict criteria for genome-wide significance.Conclusions The largest genome-wide association study of severe asthma to date was carried out and strong evidence found for the association of two previously identified asthma susceptibility loci in patients with severe disease. A number of novel regions with suggestive evidence were also identified warranting further study.

Published
2012

19. Virus Infection of Grass can Alter the Allergenic Potency of Pollen

Author

Soh, E., Pallett, D.W., Bodey, K., Lau, L.C.K., Whitworth, H., Page, A., Edwards, M., Howarth, P.H., Cooper, J.I., Wang, H., Soh, E., Pallett, D.W., Bodey, K., Lau, L.C.K., Whitworth, H., Page, A., Edwards, M., Howarth, P.H., Cooper, J.I., and Wang, H.

Abstract

BACKGROUND: Wild plants harbour a variety of viruses and these have the potential to alter the composition of pollen. The potential consequences of virus infection of grasses on pollen-induced allergic disease are not known. METHODS: We have collected pollen from Dactylis glomerata (cocksfoot; a grass species implicated as a trigger of allergic rhino-conjunctivitis) from Wytham Wood, Oxfordshire UK. Extracts were prepared from pollen from uninfected grass, and from grass naturally infected by the Cocksfoot streak potyvirus (CSV). Preparations of pollen from virus-infected and non-infected grasses were employed in skin testing 15 grass pollen-allergic subjects with hayfever. Allergen profiles of extracts were investigated by Western blotting for IgE with sera from allergic subjects. RESULTS: The prevalence of CSV infection in cocksfoot grasses sampled from the study site varied significantly over an eight-year period, but infection rates of up to 70% were detected. Virus infection was associated with small alterations in the quantities of pollen proteins detected by polyacrylamide gel electrophoresis, and in the patterns of allergens identified by Western blotting with IgE from grass pollen allergic subjects. For individual subjects there were differences in potencies of standardised extracts of pollen from virus-free and virus-infected plants as assessed by skin testing, though a consistent pattern was not established for the group of 15 subjects. CONCLUSION: Infection rates for CSV in cocksfoot grass can be high, though variable. Virus-induced alterations in components of grass pollen have the potential to alter the allergenic potency.

Published
2010

38. Allergic rhinitis: not purely a histamine-related disease.

Author

Howarth, P.H., Salagean, M., and Dokic, D.

Subjects
*LEUKOTRIENES, *HISTAMINE, *ALLERGIC rhinitis
Abstract

Reports on a study which suggested that the effects of both leukotrienes and histamine has complementary effects in relieving nasal symptoms; Relevance of leukotrienes and histamine in the disease expression.

Published
2000
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39. A comparison of the anti-inflammatory properties of intranasal corticosteroids and antihistamines in allergic rhinitis.

Author

Howarth, P.H.

Subjects
*ALLERGIC rhinitis, *RESPIRATORY allergy
Abstract

Analyzes the mechanisms involved in airways inflammation in allergic rhinitis. Examination of the in vitro and in vivo evidence for the relevant anti-inflammatory potential and effects of the pharmacological agents; Analysis of the major pathways involved in allergic airways inflammation.

Published
2000
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40. Is allergy increasing?--early life influences.

Author

Howarth, P.H.

Subjects
*ALLERGIES, *EPIDEMIOLOGY, *TH2 cells
Abstract

Studies the continuous prevalence of allergy in the U.S. from the 1940s to 1990s. Intrauterine environment TH[sub 2] cell development; Negative association of infections with the development of atopy.

Published
1998
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42. Inflammatory mediators in naturally occurring rhinitis.

Author

Wilson, S.J., Lau, L., and Howarth, P.H.

Subjects
RHINITIS, MAST cells, EOSINOPHILS, ALLERGIC rhinitis
Abstract

Measures mast cell and eosinophil mediator levels and indices of vascular permeability in naturally occurring rhinitis. Occurrence of mast cell and eosinophil activation in both seasonal allergic rhinitis and perennial allergic rhinitis; Increase in vascular permeability; Possible use of measurements in lavage fluid for monitoring the mucosal cellular events in response to therapy.

Published
1998
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43. TNFα is localized to nasal mucosal mast cells and is released in acute allergic rhinitis.

Author

Bradding, P., Mediwake, R., Feather, I.H., Madden, J., Church, M.K., Holgate, S.T., and Howarth, P.H.

Subjects
RHINITIS, MAST cells, T cells, CELL adhesion, TUMOR necrosis factors, RESPIRATORY therapy, RESPIRATORY allergy
Abstract

Allergic mucosal inflammation is characterized by tissue infiltration with eosinophils. and associated activation of mast cells and T lymphocytes. Tumour necrosis factor (TNF) alpha/cachectin is a candidate cytokine relevant to the pathogenesis of these events through its capacity to upregulate the expression of endothelial cell adhesion molecules, mediate granulocyte chemoattraction, and activate eosinophils, mast cells and T cells. To investigate the presence and localization of TNFα in the nasal mucosa in allergic rhinitis, nasal biopsies from perennial rhinitic (n=13) and non-rhinitic volunteers (n=11) were embedded in glycol methacrylate and immunostained with a monoclonal antibody directed against TNFα, and adjacent 2µm sections stained for tryptase, CD3 and eosinophil cationic protein. This identified positive immunostaining for TNFα in the submucosa of' both the rhinitic and normal subjects (median cell counts 13 and 23 cells/mm² respectively, P=0.24) with cellular localization to mast cells but not to T-lymphocytes or eosinophils. In a subsequent study of seven atopic subjects, nasal allergen challenge produced increases in lavage levels of histamine and albumin, which was associated with significant release of TNF& as early as 2 mm post-allergen when compared with the saline control day (P=0.05). This difference was also apparent when studying the area under the curve both at 30 and 60 mm posts challenge t-test (P=0.015 and 0.02 respectively). These findings which both locate immunoreactive TNFα to nasal mast cells and identify its release following in vivo exposure to allergen. provide evidence for mast cells as an important source of this cytokine in patients with allergic rhinitis. [ABSTRACT FROM AUTHOR]

Published
1995
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44. Why Particle Size Should Affect Clinical Response to Inhaled Therapy

Author

Howarth, P.H.

Abstract

Studies with β2-adrenergic agonists have shown that particle size and total dose are important determinants of optimum bronchodilation. Drug deposition in the airways is probably the most important factor for bronchodilation, since β2-adrenoceptors and muscarinic M3 receptors are present mainly in the peripheral and central airways, respectively. Furthermore, clinical efficacy can be maintained while minimizing systemic exposure by selecting an appropriate particle size. Changes in lung function provide a means of monitoring the relationship between delivery of the bronchodilator and its efficacy, whereas there is no such immediate means of assessing antiinflammatory preventative therapy such as inhaled corticosteroids. Asthma is primarily an inflammatory disease but there are no simple tests to detect the accumulation of inflammatory cells and mediators. Data are presented to demonstrate the reduction of certain inflammatory markers in bronchial biopsy tissue taken from asthmatic patients after corticosteroid therapy. Measurement of inflammatory markers in both bronchial biopsy tissue and bronchoalveolar lavage samples may provide a way of monitoring the site of action and efficacy of inhaled corticosteroids in the future. Furthermore, it is envisaged that the effect of corticosteroid particle size on efficacy and systemic bioavailability may be investigated by exploiting these methods.

Published
2001
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45. Double-blind, placebo-controlled study comparing the efficacy and safety of fexofenadine hydrochloride (120 and 180 mg once daily) and cetirizine in seasonal allergic rhinitis

Author

Howarth, P.H., Stern, M.A., Roi, L., Reynolds, R., and Bousquet, J.

Abstract

Background: Fexofenadine hydrochloride (HCl) is a new H "1 antihistamine used twice daily in some countries. Objective: A multicenter, double-blind, parallel-group, placebo-controlled trial compared the efficacy and safety of fexofenadine HCl (120 and 180 mg administered once daily) and cetirizine (10 mg once daily) in the treatment of seasonal allergic rhinitis. Methods: After a 3- to 5-day run-in period, patients meeting entrance criteria were randomized to receive placebo, fexofenadine HCl 120 mg once daily, fexofenadine HCl 180 mg once daily, or cetirizine 10 mg once daily (active control) for 2 weeks. Eight hundred twenty-one patients comprised the intention-to-treat population and 722 patients completed the study. Symptom assessments were conducted 12 hours after the dose for the previous 12 hours and again at 24 hours after the dose for the previous 12 hours. In addition, assessment was made immediately before dosing in the morning for the previous 30 minutes. Total symptom score was calculated as the sum of scores for the 4 individual symptoms: (1) sneezing, (2) rhinorrhea, (3) itchy nose, palate, or throat, and (4) itchy, watery, or red eyes; the nasal congestion score was also recorded. Results: Both doses of fexofenadine HCl were superior to placebo in reducing the total symptom score. Efficacy was maintained for the entire dosing interval (ie, for 24 hours). There were no differences in efficacy between the 2 doses of fexofenadine HCl or between either dose of fexofenadine HCl and cetirizine. There was no major side effect, but the combined incidence of drowsiness or fatigue was greater with ce-tirizine (9%) than with placebo (4%) (P = .07) or fexofenadine (4%) (P = .02). Conclusions: Once-daily fexofenadine is thus a valuable addition to the nonsedating group of H "1 receptor antagonists currently available for the treatment of seasonal allergic rhinitis. (J Allergy Clin Immunol 1999;104:927-33.)

Published
1999
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46. Cellular and mediator responses twenty-four hours after local endobronchial allergen challenge of asthmatic airways

Author

Frew, A.J., St-Pierre, J., Teran, L.M., Trefilieff, A., Madden, J., Peroni, D., Bodey, K.M., Walls, A.F., Howarth, P.H., Carroll, M.P., and Holgate, S.T.

Abstract

The effects of acute allergen exposure on bronchoalveolar lavage cells and mediators and mucosal inflammatory cells were evaluated in 10 subjects with atopic asthma who underwent lavage and biopsy 24 hours after segmental endobronchial allergen challenge. Increased numbers of bronchoalveolar lavage eosinophils were retrieved from the allergen-challenged sites compared with the saline-challenged sites (mean 21.4 vs 1.5 x 10^3 cells/ml; p < 0.02). Numbers of neutrophils and proportions of CD4^+, CD8^+, CD25^+, and HLA-DR^+ T cells were similar at the saline- and allergen-challenged sites. In contrast to the bronchoalveolar lavage findings, eosinophil numbers were not increased in the bronchial submucosa or epithelium. There was also no significant difference in neutrophils, mast cells, CD3^+, CD4^+, or CD8^+ T cells in the submucosa after allergen challenge, but the number of activated (CD25^+) T lymphocytes in the mucosa did increase after allergen challenge. Allergen challenge did not induce any significant change in endothelial expression of P-selectin, E-selectin, intercellular adhesion molecule-1, or vascular cell adhesion molecule-1. CD11a^+ and very late antigen-4^+ cell numbers were similar in the saline- and allergen-challenged sites. This study suggests that in patients with very mild asthma, local allergen challenge induces persistent bronchoalveolar lavage eosinophilia, but the recruitment process seems to have diminished or ceased by 24 hours. (J ALLERGY CLIN IMMUNOL 1996;98:133-43.)

Published
1996
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47. Cross refractoriness between bradykinin and hypertonic saline challenges in asthma

Author

Rajakulasingam, K., Makker, H.K., Howarth, P.H., and Holgate, S.T.

Abstract

Background: Repeated inhalation of bradykinin and hypertonic saline leads to refractoriness of the bronchoconstrictor response in asthma. It is not known whether cross-refractoriness exists between these stimuli. Objective: We postulated that repeated bradykinin and hypertonic saline bronchial challenges might reduce the airway response to subsequent hypertonic saline and bradykinin challenges, respectively. Methods: Eleven atopic asthmatic subjects underwent two concentration-response studies, separated by 1 hour, with either inhaled histamine or bradykinin. After recovery, a hypertonic saline challenge was performed. During the next phase, nine subjects underwent two concentration-response studies, separated by 1 hour, with hypertonic saline. After recovery, a bradykinin challenge was performed. Results: On the histamine study day, the mean provocative volume of agonist required to produce 20% drop in forced expiratory volume in 1 second (PD"2"0) hypertonic saline was 220.7 L (+/-42.7 L) and this was not significantly different from that measured at baseline. On the bradykinin study day, the geometric mean provocative concentration of agonist required to produce a 20% drop in forced expiratory volume in 1 second (PC"2"0) was 0.39 mg/ml (0.01 to 11.73 mg/ml) for the first test and significantly higher at 1.38 mg/ml (0.01 to >16.0 mg/ml) for the second test (p = 0.006). The hypertonic saline PD"2"0 increased significantly from a baseline of 159.2 L (+/-27.3 L) to 377.6 (+/-64.7 L) (p = 0.003). On the hypertonic saline study day, the mean PD"2"0 was 152.8 L for the first test, and 337.7 L for the second test (p = 0.01). PC"2"0 bradykinin increased significantly from a baseline of 0.57 to 2.56 mg/ml (p = 0.02). A significant correlation was found between loss of response to bradykinin and to hypertonic saline (r"s, 0.63 and 0.76). Conclusion: Refractoriness produced by repeated exposure of the airways to bradykinin and hypertonic saline results in loss of responsiveness to hypertonic saline and bradykinin respectively, suggesting a shared mechanism for refractoriness produced by these stimuli. (J Allergy Clin Immunol 1995;96:502-9.)

Published
1995
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48. Effect of systemic @b-agonist therapy on IgE production in allergic subjects in vivo

Author

Corne, J.M., Linaker, C.H., Howarth, P.H., Lau, L.C.K., Merrett, T., Beasely, R., and Church, M.

Abstract

Background: Although @b2-adrenoceptor agonists are widely used in the treatment of asthma, a number of studies have suggested that their long-term use may exacerbate the condition. One possible mechanism for this stems from the in vitro observation that @b2-agonists increase IgE synthesis by human blood mononuclear cells. Objective: We sought to examine the effect of regular @b2-agonist therapy on IgE production in vivo in human volunteers. Methods: Placebo or salbutamol (8 mg BD) tablets were given in a double-blind, randomized fashion to 25 volunteers allergic to grass pollen throughout a period encompassing the UK grass pollen season (April through September). Levels of serum IgE were measured monthly, and nasal IgE was measured at the height and end of the season. Efficacy was assessed through monthly recordings of symptoms of blocked nose (vascular) and other symptoms of rhinitis (nonvascular). Results: For the whole group the geometric mean of serum IgE levels rose from a baseline of 58.7 IU/mL (range, 0 to 1027 IU/mL) to 140 IU/mL (range, 12 to 878 IU/mL) at the height of the pollen season (P = .0001). There was no significant difference between the magnitude of the rise in IgE between the groups with a ratio of increase for salbutamol/placebo of 1.17 (confidence interval = 0.78 to 1.75). There was no change in nasal IgE levels. Total and nonvascular symptom scores were reduced by salbutamol, reaching statistical significance at the height of the pollen season (P < .05). Conclusion: An oral dose of the @b2-agonist salbutamol, sufficient to maintain therapeutic levels and provide clinical benefit, does not accentuate the seasonal increase of IgE in human atopic volunteers. (J Allergy Clin Immunol 1998;102:727-31.)

Published
1998
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49. Immunoreactive endothelin in bronchial biopsy specimens: Increased expression in asthma and modulation by corticosteroid therapy

Author

Redington, A.E., Springall, D.R., Meng, Q.H., Tuck^a, A.B., Holgate, S.T., Polak, J.M., and Howarth, P.H.

Abstract

Background: The human endothelin (ET) family comprises three 21-amino-acid peptides, which are potent bronchoconstrictors and have a number of other biologic properties relevant to the pathophysiology of asthma. Objective: We sought to compare the expression of immunoreactive ET in bronchial biopsy specimens from subjects with asthma treated only with inhaled @b"2-agonists, subjects with asthma treated with @b"2-agonists and corticosteroids, and control subjects without asthma. Methods: Biopsy specimens were obtained by fiberoptic bronchoscopy and stained immunohistochemically with a specific ET antiserum. Epithelial ET expression was quantitated by using a computer-assisted system of image analysis. Numbers of inflammatory cells and depth of subepithelial collagen deposition were also determined. Results: Immunoreactive ET was principally localized in the airway epithelium. The proportion of epithelium immunostained was significantly increased in the subjects with asthma not treated with steroids (35.4% +/- 3.8%) compared with that of both the control subjects (16.2% +/- 1.9%, p < 0.0001) and the subjects with asthma treated with steroids (14.3% +/- 2.0%, p < 0.0001). The last two groups did not differ significantly from one another. There were no significant correlations between ET expression and either physiologic parameters or indexes of airway inflammation and remodeling. Conclusion: Bronchial epithelial expression of immunoreactive ET is increased in subjects with asthma receiving treatment only with @b"2-agonists but not in subjects with asthma also receiving corticosteroid therapy. These findings are consistent with the hypothesis that ET is implicated in the pathophysiology of asthma. (J Allergy Clin Immunol 1997;100:544-52.)

Published
1997
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50. Genome-wide association study to identify genetic determinants of severe asthma

Author

Wan, Y.I., Shrine, N.R.G., Soler Artigas, M., Wain, L.V., Blakey, J.D., Moffatt, M.F., Bush, A., Chung, K. F., Cookson, W.O.C.M., Strachan, D.P., Heaney, L., Al-Momani, B.A.H., Mansur, A.H., Manney, S., Thomson, N.C., Chaudhuri, R., Brightling, C.E., Bafadhel, M., Singapuri, A., Niven, R., Simpson, A., Holloway, J.W., Howarth, P.H., Hui, J., Musk, A.W., James, A.L., Brown, M.A., Baltic, S., Ferreira, M.A.R., Thompson, P.J., Tobin, M.D., Sayers, Ian, Hall, Ian P., Wan, Y.I., Shrine, N.R.G., Soler Artigas, M., Wain, L.V., Blakey, J.D., Moffatt, M.F., Bush, A., Chung, K. F., Cookson, W.O.C.M., Strachan, D.P., Heaney, L., Al-Momani, B.A.H., Mansur, A.H., Manney, S., Thomson, N.C., Chaudhuri, R., Brightling, C.E., Bafadhel, M., Singapuri, A., Niven, R., Simpson, A., Holloway, J.W., Howarth, P.H., Hui, J., Musk, A.W., James, A.L., Brown, M.A., Baltic, S., Ferreira, M.A.R., Thompson, P.J., Tobin, M.D., Sayers, Ian, and Hall, Ian P.

Abstract

Background The genetic basis for developing asthma has been extensively studied. However, association studies to date have mostly focused on mild to moderate disease and genetic risk factors for severe asthma remain unclear. Objective To identify common genetic variants affecting susceptibility to severe asthma. Methods A genome-wide association study was undertaken in 933 European ancestry individuals with severe asthma based on Global Initiative for Asthma (GINA) criteria 3 or above and 3346 clean controls. After standard quality control measures, the association of 480 889 genotyped single nucleotide polymorphisms (SNPs) was tested. To improve the resolution of the association signals identified, non-genotyped SNPs were imputed in these regions using a dense reference panel of SNP genotypes from the 1000 Genomes Project. Then replication of SNPs of interest was undertaken in a further 231 cases and 1345 controls and a meta-analysis was performed to combine the results across studies. Results An association was confirmed in subjects with severe asthma of loci previously identified for association with mild to moderate asthma. The strongest evidence was seen for the ORMDL3/GSDMB locus on chromosome 17q12-21 (rs4794820, p=1.03×10(−8) following meta-analysis) meeting genome-wide significance. Strong evidence was also found for the IL1RL1/IL18R1 locus on 2q12 (rs9807989, p=5.59×10(−8) following meta-analysis) just below this threshold. No novel loci for susceptibility to severe asthma met strict criteria for genome-wide significance. Conclusions The largest genome-wide association study of severe asthma to date was carried out and strong evidence found for the association of two previously identified asthma susceptibility loci in patients with severe disease. A number of novel regions with suggestive evidence were also identified warranting further study.

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