Hydroxychloroquine improves airflow and lowers circulating IgE levels in subjects with moderate symptomatic asthma
Identifieur interne : 002822 ( Main/Exploration ); précédent : 002821; suivant : 002823Hydroxychloroquine improves airflow and lowers circulating IgE levels in subjects with moderate symptomatic asthma
Auteurs : B. Lauren Charous ; Elkan F. Halpern ; Gary C. StevenSource :
- The Journal of Allergy and Clinical Immunology [ 0091-6749 ] ; 1998.
Descripteurs français
- Pascal (Inist)
- Wicri :
- topic : Homme.
English descriptors
- KwdEn :
- Teeft :
- Allergy, Allergy clin immunol, Allergy clin immunol volume, Antiallergic effects, Antiasthmatic, Antiasthmatic agent, Antiasthmatic effects, Asthma, Asthma results, Asthma therapy, Asthmatic, Asthmatic subjects, Baseline, Blood institute, Bronchial asthma, Bronchodilator, Charous, Clin, Control group, Corticosteroid, Definitive conclusions, Evening peak flows, Fasting cholesterol, Fev1, Hydroxychloroquine, Immunoglobulin levels, Immunol, Immunosuppressive agents, Inhaled, Inhaled corticosteroid, Inhaled corticosteroids, Lauren charous, Lipid, Lipid levels, Lipid profiles, National heart, Objective measures, Ocular safety, Oral asthmatic subjects, Oral corticosteroids, Peak expiratory flow rate, Peak flow, Pefr, Placebo, Placebo group, Potential utility, Previous observations, Respir crit care, Respiratory care center, Rheumatic disease, Rheumatoid arthritis, Significant change, Significant decreases, Significant differences, Slow onset, Stable doses, Statistical analysis, Study drug, Study exit, Symptom scores, Symptomatic asthmatic subjects, Theophylline levels, Treatment group.
Abstract
Abstract: Background Although antiinflammatory therapy is accepted as the cornerstone of asthma treatment, available systemic immunosuppressive agents are not widely used because of justified concerns over potential toxicity. Hydroxychloroquine (HCQ) is a well-tolerated, safe immunomodulating drug, with proven efficacy in rheumatic diseases and known actions that suggest potential utility in the treatment of asthma. Objective: We sought to assess the effectiveness of HCQ in subjects with moderate symptomatic asthma. Methods: Symptomatic asthmatic subjects receiving stable doses of at least 6 puffs of inhaled corticosteroid per day with daily need for β2-adrenergic agonists were studied. After baseline run-in, these subjects were randomized to 30 weeks of HCQ (n = 8) or placebo (n = 9). Objective measures included change from baseline mean FEV1, morning and evening peak flows, β2-agonist use, IgE level, and need for rescue cortico-steroids. Subjective symptom scores from bidaily diaries were also obtained. Results: In the treatment group, mean FEV1 at the last 2 visits on therapy increased by 10.8% (P < .05), morning peak flows rose 16.2% (P < .03), evening peak flows rose 14.2% (P < .04), and β2-agonist use fell 18.6% (P < .03). Mean IgE level declined 48% from 240 to 125 IU/mL (P < .05). In the placebo group no significant change in these parameters occurred. Comparison of changes in these objective measures between the treatment and placebo groups failed to reach significance in the small population studied. Corticosteroid rescue interventions were required in 4 patients receiving placebo and 2 receiving HCQ. HCQ was well tolerated without notable side effects. Conclusions: Although the size of our sample population precludes definitive conclusions, these findings extend previous open-label observations. The late improvement in the HCQ group is consistent with its known slow onset of action. Further studies are warranted to confirm the antiasthmatic and antiallergic effects of HCQ and to investigate its potential as a disease-modifying agent. (J Allergy Clin Immunol 1998;102:198-203).
Url:
DOI: 10.1016/S0091-6749(98)70086-7
Affiliations:
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Le document en format XML
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Steven</name><affiliation><wicri:noCountry code="subField">Wis</wicri:noCountry></affiliation></author></analytic><monogr></monogr><series><title level="j">The Journal of Allergy and Clinical Immunology</title><title level="j" type="abbrev">YMAI</title><idno type="ISSN">0091-6749</idno><imprint><publisher>ELSEVIER</publisher><date type="published" when="1998">1998</date><biblScope unit="volume">102</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="198">198</biblScope><biblScope unit="page" to="203">203</biblScope></imprint><idno type="ISSN">0091-6749</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0091-6749</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Antiallergic</term><term>Antiasthma agent</term><term>Asthma</term><term>Chemotherapy</term><term>Controlled therapeutic trial</term><term>HCQ:</term><term>Human</term><term>Hydroxychloroquine</term><term>IgE</term><term>Immunoglobulins</term><term>Lung function</term><term>PEFR:</term><term>Treatment</term><term>Treatment efficiency</term><term>antiinflammatory agents</term><term>antimalarial</term><term>asthma therapy</term><term>hydroxychloroquine</term></keywords><keywords scheme="Pascal" xml:lang="fr"><term>Antiallergique</term><term>Antiasthmatique</term><term>Asthme</term><term>Chimiothérapie</term><term>Efficacité traitement</term><term>Essai thérapeutique contrôlé</term><term>Fonction respiratoire</term><term>Homme</term><term>Hydroxychloroquine</term><term>IgE</term><term>Immunoglobuline</term><term>Traitement</term></keywords><keywords scheme="Teeft" xml:lang="en"><term>Allergy</term><term>Allergy clin immunol</term><term>Allergy clin immunol volume</term><term>Antiallergic effects</term><term>Antiasthmatic</term><term>Antiasthmatic agent</term><term>Antiasthmatic effects</term><term>Asthma</term><term>Asthma results</term><term>Asthma therapy</term><term>Asthmatic</term><term>Asthmatic subjects</term><term>Baseline</term><term>Blood institute</term><term>Bronchial asthma</term><term>Bronchodilator</term><term>Charous</term><term>Clin</term><term>Control group</term><term>Corticosteroid</term><term>Definitive conclusions</term><term>Evening peak flows</term><term>Fasting cholesterol</term><term>Fev1</term><term>Hydroxychloroquine</term><term>Immunoglobulin levels</term><term>Immunol</term><term>Immunosuppressive agents</term><term>Inhaled</term><term>Inhaled corticosteroid</term><term>Inhaled corticosteroids</term><term>Lauren charous</term><term>Lipid</term><term>Lipid levels</term><term>Lipid profiles</term><term>National heart</term><term>Objective measures</term><term>Ocular safety</term><term>Oral asthmatic subjects</term><term>Oral corticosteroids</term><term>Peak expiratory flow rate</term><term>Peak flow</term><term>Pefr</term><term>Placebo</term><term>Placebo group</term><term>Potential utility</term><term>Previous observations</term><term>Respir crit care</term><term>Respiratory care center</term><term>Rheumatic disease</term><term>Rheumatoid arthritis</term><term>Significant change</term><term>Significant decreases</term><term>Significant differences</term><term>Slow onset</term><term>Stable doses</term><term>Statistical analysis</term><term>Study drug</term><term>Study exit</term><term>Symptom scores</term><term>Symptomatic asthmatic subjects</term><term>Theophylline levels</term><term>Treatment group</term></keywords><keywords scheme="Wicri" type="topic" xml:lang="fr"><term>Homme</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">Abstract: Background Although antiinflammatory therapy is accepted as the cornerstone of asthma treatment, available systemic immunosuppressive agents are not widely used because of justified concerns over potential toxicity. Hydroxychloroquine (HCQ) is a well-tolerated, safe immunomodulating drug, with proven efficacy in rheumatic diseases and known actions that suggest potential utility in the treatment of asthma. Objective: We sought to assess the effectiveness of HCQ in subjects with moderate symptomatic asthma. Methods: Symptomatic asthmatic subjects receiving stable doses of at least 6 puffs of inhaled corticosteroid per day with daily need for β2-adrenergic agonists were studied. After baseline run-in, these subjects were randomized to 30 weeks of HCQ (n = 8) or placebo (n = 9). Objective measures included change from baseline mean FEV1, morning and evening peak flows, β2-agonist use, IgE level, and need for rescue cortico-steroids. Subjective symptom scores from bidaily diaries were also obtained. Results: In the treatment group, mean FEV1 at the last 2 visits on therapy increased by 10.8% (P < .05), morning peak flows rose 16.2% (P < .03), evening peak flows rose 14.2% (P < .04), and β2-agonist use fell 18.6% (P < .03). Mean IgE level declined 48% from 240 to 125 IU/mL (P < .05). In the placebo group no significant change in these parameters occurred. Comparison of changes in these objective measures between the treatment and placebo groups failed to reach significance in the small population studied. Corticosteroid rescue interventions were required in 4 patients receiving placebo and 2 receiving HCQ. HCQ was well tolerated without notable side effects. Conclusions: Although the size of our sample population precludes definitive conclusions, these findings extend previous open-label observations. The late improvement in the HCQ group is consistent with its known slow onset of action. Further studies are warranted to confirm the antiasthmatic and antiallergic effects of HCQ and to investigate its potential as a disease-modifying agent. (J Allergy Clin Immunol 1998;102:198-203).</div></front></TEI><affiliations><list></list><tree><noCountry><name sortKey="Charous, B Lauren" sort="Charous, B Lauren" uniqKey="Charous B" first="B. Lauren" last="Charous">B. Lauren Charous</name><name sortKey="Halpern, Elkan F" sort="Halpern, Elkan F" uniqKey="Halpern E" first="Elkan F." last="Halpern">Elkan F. Halpern</name><name sortKey="Steven, Gary C" sort="Steven, Gary C" uniqKey="Steven G" first="Gary C." last="Steven">Gary C. Steven</name></noCountry></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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