Churg–Strauss syndrome and leukotriene antagonist use: a respiratory perspective
- 1Department of Respiratory Medicine, City Hospital, Birmingham, UK
- 2Lung Injury and Fibrosis Treatment Programme, Division of Medical Sciences, University of Birmingham, UK
- 3Division of Immunity and Infection, University of Birmingham, UK
- 4Department of Respiratory Medicine, Heartlands Hospital, Birmingham, UK
- 5Department of Respiratory Medicine, University Hospital, Birmingham, UK
- Dr N Nathani, Department of Thoracic Medicine, City Hospital, Dudley Road, Birmingham B18 7QH, UK; n.nathani{at}nhs.net
- Received 26 November 2007
- Accepted 28 March 2008
- Published Online First 20 May 2008
Abstract
Background: Churg–Strauss syndrome (CSS) is a rare granulomatous small vessel vasculitis that occurs against a background of longstanding asthma. Leukotriene antagonists (LTAs) are used in the management of asthma and may facilitate a reduction in steroid dosage. Reports of the development of CSS in patients with asthma following the initiation of LTA therapy suggest either a causal association or an unmasking of latent CSS as steroid doses fall. We have undertaken a systematic review to establish whether evidence of a drug induced syndrome exists.
Methods: Systematic review searching Medline from database inception to August 2007 to identify cases with a possible association between LTAs and CSS. Hill’s criteria of causation were used to assess strength of causality.
Results: 62 cases in which CSS developed after the introduction of LTA therapy were identified. Patients were divided into three groups: group 1 had received no previous steroid therapy; group 2 had been treated with oral and/or inhaled corticosteroids, but had no change in steroid therapy following LTA introduction; and group 3 had a clear reduction in steroid therapy following introduction of LTA therapy. The majority of patients from each group exhibited a clear temporal relationship between initiation of LTA and development of CSS, with no evidence of pre-existing disease.
Conclusions: Currently available evidence suggests an association between LTA and CSS that may be causal.
Footnotes
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Funding: DRT is funded by a Wellcome research grant. MAL is funded by the HEFCE Senior Lecturer scheme. NN was funded by UHB Charities.
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Competing interests: None.









