Selner J, Boltansky H, Chervinsky P, Pearlman D, Pedinoff A, Weinstein S, Wolfe J, Stevens A, Prillaman B, Hamedani A, Harding S, Field E. Low dose inhaled fluticasone propionate administered once daily or twice daily via the Diskus is as safe and effective as beclomethasone diproprionate in steroid naïve patients with asthma. Poster presented at the AAAI/AAI/CIS Joint Meeting; February 21, 1997. [abstract] J Allergy Clin Immunol. 1997 Jan; 99(1 Part 2):1319. doi: 10.1016/S0091-6749(97)81066-4


12-week, multicenter, randomized, double-blind, double-dummy parallel-group trial compared efficacy and safety of fluticasone propionate (FP), beclomethasone dipropionate (BDP) and placebo (PLA) in 299 steroid naive asthma patients aged 12 and up previously treated with beta-agonist therapy. FP was administered via Diskus, a new 60-dose dry powder device, at blister doses of 100mcg BID (FP-BID) and 200mcg QD (FP-QD). BDP was given at 168mcg BID (exactuator dose) via metereddose inhaler. Visits were scheduled every 1-2 weeks. Subjects were dropped for lack of efficacy (LOE) when meeting predefined criteria for changes in FEV~, PEF, or nighttime awakenings. Fewer patients on FP-BID (n = 5) and FP-QD (n = 7) were dropped for LOE vs PLA (n = 19; p<0.01). There were no significant differences between BDP vs PLA treated patients in LOE withdrawal rates. Mean FEV l at baseline was 2.56-2.62L (67.7-68.8% predicted). After 1 week of treatment, FEV~ improved by 13-14% on all active treatments (p<0.05 vs PLA). FP-BID, FP-QD and BDP treatment significantly improved FEV 1 at endpoint (last treatment visit) (p<0.05 vs PLA). All active treatments significantly improved change in PEF from baseline to endpoint (p<0.005 vs PLA) with concurrent decreased use of beta-agonist (p<0.05 vs PLA). Adverse event rates were low and comparable across treatment groups. Overall, low dose FP-BID and FP-QD improved lung function with efficacy.

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