Author(s): Calverley PM, Anderson JA, Celli B, Ferguson GT, Jenkins C, et al.
Background: Long-acting beta-agonists and inhaled corticosteroids are used to treat chronic obstructive pulmonary disease (COPD), but their effect on survival is unknown.
Methods: We conducted a randomized, double-blind trial comparing salmeterol at a dose of 50 microg plus fluticasone propionate at a dose of 500 microg twice daily (combination regimen), administered with a single inhaler, with placebo, salmeterol alone, or fluticasone propionate alone for a period of 3 years. The primary outcome was death from any cause for the comparison between the combination regimen and placebo; the frequency of exacerbations, health status, and spirometric values were also assessed.
Results: Of 6112 patients in the efficacy population, 875 died within 3 years after the start of the study treatment. All-cause mortality rates were 12.6% in the combination-therapy group, 15.2% in the placebo group, 13.5% in the salmeterol group, and 16.0% in the fluticasone group. The hazard ratio for death in the combination-therapy group, as compared with the placebo group, was 0.825 (95% confidence interval [CI], 0.681 to 1.002; P=0.052, adjusted for the interim analyses), corresponding to a difference of 2.6 percentage points or a reduction in the risk of death of 17.5%. The mortality rate for salmeterol alone or fluticasone propionate alone did not differ significantly from that for placebo. As compared with placebo, the combination regimen reduced the annual rate of exacerbations from 1.13 to 0.85 and improved health status and spirometric values (P<0.001 for all comparisons with placebo). There was no difference in the incidence of ocular or bone side effects. The probability of having pneumonia reported as an adverse event was higher among patients receiving medications containing fluticasone propionate (19.6% in the combination-therapy group and 18.3% in the fluticasone group) than in the placebo group (12.3%, P<0.001 for comparisons between these treatments and placebo).
Conclusions: The reduction in death from all causes among patients with COPD in the combination-therapy group did not reach the predetermined level of statistical significance. There were significant benefits in all other outcomes among these patients. (ClinicalTrials.gov number, NCT00268216 [ClinicalTrials.gov].).
Referred From: https://www.ncbi.nlm.nih.gov/pubmed/17314337
Author(s): Mannino DM
Author(s): Mannino DM, Homa DM, Akinbami LJ, Ford ES, Redd SC
Author(s): Xu X, Weiss ST, Rijcken B, Schouten JP
Author(s): Anthonisen NR, Connett JE, Murray RP
Author(s): Guyatt GH, Townsend M, Pugsley SO, Keller JL, Short HD, et al.
Author(s): Man WD, Mustfa N, Nikoletou D, Kaul S, Hart N, et al.
Author(s): Nelson HS, Weiss ST, Bleecker ER, Yancey SW, Dorinsky PM, et al.
Author(s): Sin DD, McAlister FA, Man SF, Anthonisen NR
Author(s): Ram FS, Jones PW, Castro AA, DeBerito JA, Atallah AN, et al.
Author(s): Highland KB, Strange C, Heffner JE
Author(s): Sutherland ER, Allmers H, Ayas NT, Venn AJ, Martin RJ
Author(s): Alsaeedi, Sin DD, McAlister FA
Author(s): Burge PS, Calverley PM, Jones PW, Spencer S, Anderson JA, et al.
Author(s): Calverley P, Pauwels R, Vestbo J, Jones P, Pride N, et al.
Author(s): Mahler DA, Wire P, Horstman D, Chang C, Yates J, et al.
Author(s): Szafranski W, Cukier A, Ramirez A, Menga G, Sansores R, et al.
Author(s): Hanania NA, Darken P, Horstman D, Reisner C, Lee B, et al.
Author(s): Calverley PM, Boonsawat W, Cseke Z, Zhong N, Peterson S, et al.
Author(s): Burge PS, Calverley PM, Jones PW, Spencer S, Anderson JA, et al.
Author(s): Rice KL, Rubins JB, Lebahn F, Parenti CM, Duane PG, et al.
Author(s): Decramer M, Lacquet LM, Fagard R, Rogiers P
Author(s): Decramer M, Stas KJ
Author(s): Chong J, Poole P, Leung B, Black PN
Author(s): Calverley PM, Rabe KF, Goehring UM, Kristiansen S, Fabbri LM, et al.
Author(s): Seemungal TA, Wilkinson TM, Hurst JR, Perera WR, Sapsford RJ, et al.
Author(s): He ZY, Ou LM, Zhang JQ, Bai J, Liu GN, et al.
Author(s): Wongsurakiat P, Lertakyamanee J, Maranetra KN, Jongriratanakul S, Sangkaew S
Author(s): Granger R, Walters J, Poole PJ, Lasserson TJ, Mangtani P, et al.
Author(s): Centers for Disease Control and Prevention
Author(s): Nocturnal Oxygen Therapy Trial Group
Author(s): Takabatake N, Nakamura H, Abe S, Inoue S, Hino T, et al.
Author(s): Heindl S, Lehnert M, Criee CP, Hasenfuss G, Andreas S
Author(s): Bratel T, Wennlund A, Carlstrom K
Author(s): Guyatt GH, McKim DA, Austin P, Bryan R, Norgren J, et al.
Author(s): Griffiths TL, Burr ML, Campbell IA, Lewis-Jenkins V, Mullins J, et al.
Author(s): Mehran RJ, Deslauriers J
Author(s): Moayyedi P, Congleton J, Page RL, Pearson SB, Muers MF
Author(s): Thompson WH, Nielson CP, Carvalho P, Charan NB, Crowley JJ
Author(s): Davies L, Angus RM, Calverley PM
Author(s): Niewoehner DE, Erbland ML, Deupree RH, Collins D, Gross NJ, et al.
Author(s): Maltais F, Ostinelli J, Bourbeau J, Tonnel AB, Jacquemet N, et al.
Author(s): Sethi S, Evans N, Grant BJ, Murphy TF
Author(s): Anthonisen NR, Manfreda J, Warren CP, Hershfield ES, Harding GK, et al.
Author(s): Jorgensen AF, Coolidge J, Pedersen PA, Peterson KP, Waldorff S, et al.
