- B D Pethica, research fellow (Sec{at}wnmeds.ac.nz)a,
- A Penrose, junior research fellowb,
- D MacKenzie, junior research fellowb,
- J Hall, junior research fellowb,
- R Beasley, professor of medicinea,
- M Tilyard, professor of general practiceb
- a Wellington Asthma Research Group, Wellington School of Medicine, University of Otago, Wellington, PO Box 7343, Wellington South, New Zealand
- bRoyal New Zealand College of General Practitioners Research Unit, Department of General Practice, Dunedin School of Medicine, University of Otago, PO Box 913, Dunedin, New Zealand
- Correspondence to: Dr Pethica WARG.
- Accepted 7 August 1998
Abstract
Objective To determine whether inhaled budesonide and beclomethasone are equipotent in the treatment of asthma in primary care.
Design Retrospective study of computerised clinical records from 28 general practices in New Zealand.
Subjects 5930 patients who received 16 725 prescriptions for inhaled budesonide or beclomethasone from 1 July 1994 to 30 June 1995.
Setting General practices on the database of the Royal New Zealand College of General Practitioners Research Unit. Linked information from secondary care was available for a subset of the practices.
Main outcome measure Mean prescribed daily inhaled corticosteroid dose.
Results The daily prescribed dose was higher for patients receiving inhaled budesonide (mean 979 μg) than beclomethasone (mean 635 μg), a difference of 344 μg (95% confidence interval 313 to 376 μg). This difference was consistent in all age bands and with different types of inhalation device. Evidence of systematic prescribing of higher doses of budesonide to patients with more severe asthma was not found.
Conclusions In primary care in New Zealand evidence suggests that budesonide is less potent than beclomethasone. Consideration of validated, established, and other possible markers of asthma severity did not support confounding by severity as a reason for the higher prescribed doses of budesonide. Pending further epidemiological evaluation, international asthma guidelines may need to be modified on the equivalence of inhaled corticosteroid doses. Furthermore, the comparative potency of newly developed inhaled steroids in clinical trials will need to be confirmed in appropriately designed epidemiological studies based in general practice.
Key messages
Important limitations of the randomised clinical trials comparing beclomethasone and budesonide have usually resulted in failure to detect differences in potency
In this study using a computerised database in primary care inhaled budesonide had about two thirds of the potency of inhaled beclomethasone
Asthma treatment guidelines may need to be modified concerning the dose equivalence of inhaled corticosteroids
The relative potency of newly developed inhaled corticosteroids needs to be assessed in primary care
Footnotes
- Accepted 7 August 1998
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