Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial

Thérése S. Lapperre; Jiska B. Snoeck-Stroband; Margot M.E. Gosman; Désirée F. Jansen; Annemarie Van Schadewijk; Henk A. Thiadens; Judith M. Vonk; H. Marike Boezen; Nick H.T. Ten Hacken; Jacob K. Sont; Klaus F. Rabe; Huib A.M. Kerstjens; Pieter S. Hiemstra; Wim Timens; Dirkje S. Postma; Peter J. Sterk; H. F. Kauffman; D. De Reus; M. D.W. Barentsen; M. Zeinstra-Smit; A. J. Luteijn; T. Van Der Molen; G. Ter Veen; M. S. Van Maaren; C. A. Veltman; A. Verbokkem; I. Verhage; H. K. Vink-Klooster; J. Gast-Strookman; K. Janssen; J. A. Schrumpf; J. Smit-Bakker; J. Stolk; A. C.J.A. Tiré; H. Van Der Veen; M. M.E. Wijffels; L. N.A. Willems; T. Mauad

doi:10.7326/0003-4819-151-8-200910200-00004

Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial

Thérése S. Lapperre
, Jiska B. Snoeck-Stroband
, Margot M.E. Gosman
, Désirée F. Jansen
, Annemarie Van Schadewijk
, Henk A. Thiadens
, Judith M. Vonk
, H. Marike Boezen
, Nick H.T. Ten Hacken
, Jacob K. Sont
, Klaus F. Rabe
, Huib A.M. Kerstjens
, Pieter S. Hiemstra
, Wim Timens
, Dirkje S. Postma
, Peter J. Sterk
, H. F. Kauffman
, D. De Reus
, M. D.W. Barentsen
, M. Zeinstra-Smit

A. J. Luteijn, T. Van Der Molen, G. Ter Veen, M. S. Van Maaren, C. A. Veltman, A. Verbokkem, I. Verhage, H. K. Vink-Klooster, J. Gast-Strookman, K. Janssen, J. A. Schrumpf, J. Smit-Bakker, J. Stolk, A. C.J.A. Tiré, H. Van Der Veen, M. M.E. Wijffels, L. N.A. Willems, T. Mauad

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Abstract

Background: Inhaled corticosteroids (ICSs) and long-acting β₂-agonists (LABAs) are used to treat moderate to severe chronic obstructive pulmonary disease (COPD). Objective: To determine whether long-term ICS therapy, with and without LABAs, reduces inflammation and improves pulmonary function in COPD. Design: Randomized, placebo-controlled trial. (ClinicalTrials.gov registration number: NCT00158847) Setting: 2 university medical centers in The Netherlands. Patients: 114 steroid-naive current or former smokers with moderate to severe COPD. Measurements: Cell counts in bronchial biopsies and sputum (primary outcome); methacholine responsiveness at baseline, 6, and 30 months; and clinical outcomes every 3 months. Intervention: Random assignment by minimization method to receive fluticasone propionate, 500 μg twice daily, for 6 months (n = 31) or 30 months (n = 26); fluticasone, 500 μg twice daily, and salmeterol, 50 μg twice daily, for 30 months (single inhaler; n = 28); or placebo twice daily (n = 29). Results: 101 patients were greater than 70% adherent to therapy. Fluticasone therapy decreased counts of mucosal CD3⁺ cells (-55% [95% CI, -74% to -22%]; P - 0.004), CD4- cells (-78% [CI, -88% to 60%]; P < 0.001), CD8⁺ cells (-57% [CI, -77% to -18%]; P = 0.010), and mast cells (-38% [CI, -60% to -2%]; P = 0.039) and reduced hyperresponsiveness (P = 0.036) versus placebo at 6 months, with effects maintained after 30 months. Fluticasone therapy for 30 months reduced mast cell count and increased eosinophil count and percentage of intact epithelium, with accompanying reductions in sputum neutrophil, macrophage, and lymphocyte counts and improvements in FEV₁ decline, dyspnea, and quality of life. Reductions in inflammatory cells correlated with clinical improvements. Discontinuing fluticasone therapy at 6 months increased counts of CD3⁺ cells (120% [CI, 24% to 289%]; P = 0.007), mast cells (218% [CI, 99% to 407%]; P < 0.001), and plasma cells (118% [CI, 9% to 336%]; P = 0.028) and worsened clinical outcome. Adding salmeterol improved FEV₁ level. Limitations: The study was not designed to evaluate clinical outcomes. Measurement of primary outcome was not available for 24% of patients at 30 months. Conclusion: ICS therapy decreases inflammation and can attenuate decline in lung function in steroid-naive patients with moderate to severe COPD. Adding LABAs does not enhance these effects. Primary Funding Source: Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center.

Original language	English
Pages (from-to)	517-527
Number of pages	11
Journal	Annals of Internal Medicine
Volume	151
Issue number	8
DOIs	https://doi.org/10.7326/0003-4819-151-8-200910200-00004
Publication status	Published - 20 Oct 2009

Bibliographical note

Role of the Funding Source:
This was an investigator-initiated trial. The study was
funded by the Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline
of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center. The funding sources had no role in the design, conduct, and analysis
of the study or in the decision to submit the manuscript for
publication.

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Lapperre et al._Ann Intern Med. 2009 Oct 20_151(8)_517-27Accepted author manuscript, 1.66 MB

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Lapperre, T. S., Snoeck-Stroband, J. B., Gosman, M. M. E., Jansen, D. F., Van Schadewijk, A., Thiadens, H. A., Vonk, J. M., Boezen, H. M., Ten Hacken, N. H. T., Sont, J. K., Rabe, K. F., Kerstjens, H. A. M., Hiemstra, P. S., Timens, W., Postma, D. S., Sterk, P. J., Kauffman, H. F., De Reus, D., Barentsen, M. D. W., ... Mauad, T. (2009). Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial. Annals of Internal Medicine, 151(8), 517-527. https://doi.org/10.7326/0003-4819-151-8-200910200-00004

@article{d2de84c492f94de49ed0886a30eccb16,

title = "Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial",

abstract = "Background: Inhaled corticosteroids (ICSs) and long-acting β2-agonists (LABAs) are used to treat moderate to severe chronic obstructive pulmonary disease (COPD). Objective: To determine whether long-term ICS therapy, with and without LABAs, reduces inflammation and improves pulmonary function in COPD. Design: Randomized, placebo-controlled trial. (ClinicalTrials.gov registration number: NCT00158847) Setting: 2 university medical centers in The Netherlands. Patients: 114 steroid-naive current or former smokers with moderate to severe COPD. Measurements: Cell counts in bronchial biopsies and sputum (primary outcome); methacholine responsiveness at baseline, 6, and 30 months; and clinical outcomes every 3 months. Intervention: Random assignment by minimization method to receive fluticasone propionate, 500 μg twice daily, for 6 months (n = 31) or 30 months (n = 26); fluticasone, 500 μg twice daily, and salmeterol, 50 μg twice daily, for 30 months (single inhaler; n = 28); or placebo twice daily (n = 29). Results: 101 patients were greater than 70\% adherent to therapy. Fluticasone therapy decreased counts of mucosal CD3+ cells (-55\% [95\% CI, -74\% to -22\%]; P - 0.004), CD4- cells (-78\% [CI, -88\% to 60\%]; P < 0.001), CD8+ cells (-57\% [CI, -77\% to -18\%]; P = 0.010), and mast cells (-38\% [CI, -60\% to -2\%]; P = 0.039) and reduced hyperresponsiveness (P = 0.036) versus placebo at 6 months, with effects maintained after 30 months. Fluticasone therapy for 30 months reduced mast cell count and increased eosinophil count and percentage of intact epithelium, with accompanying reductions in sputum neutrophil, macrophage, and lymphocyte counts and improvements in FEV1 decline, dyspnea, and quality of life. Reductions in inflammatory cells correlated with clinical improvements. Discontinuing fluticasone therapy at 6 months increased counts of CD3+ cells (120\% [CI, 24\% to 289\%]; P = 0.007), mast cells (218\% [CI, 99\% to 407\%]; P < 0.001), and plasma cells (118\% [CI, 9\% to 336\%]; P = 0.028) and worsened clinical outcome. Adding salmeterol improved FEV1 level. Limitations: The study was not designed to evaluate clinical outcomes. Measurement of primary outcome was not available for 24\% of patients at 30 months. Conclusion: ICS therapy decreases inflammation and can attenuate decline in lung function in steroid-naive patients with moderate to severe COPD. Adding LABAs does not enhance these effects. Primary Funding Source: Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center.",

author = "Lapperre, \{Th{\'e}r{\'e}se S.\} and Snoeck-Stroband, \{Jiska B.\} and Gosman, \{Margot M.E.\} and Jansen, \{D{\'e}sir{\'e}e F.\} and \{Van Schadewijk\}, Annemarie and Thiadens, \{Henk A.\} and Vonk, \{Judith M.\} and Boezen, \{H. Marike\} and \{Ten Hacken\}, \{Nick H.T.\} and Sont, \{Jacob K.\} and Rabe, \{Klaus F.\} and Kerstjens, \{Huib A.M.\} and Hiemstra, \{Pieter S.\} and Wim Timens and Postma, \{Dirkje S.\} and Sterk, \{Peter J.\} and Kauffman, \{H. F.\} and \{De Reus\}, D. and Barentsen, \{M. D.W.\} and M. Zeinstra-Smit and Luteijn, \{A. J.\} and \{Van Der Molen\}, T. and \{Ter Veen\}, G. and \{Van Maaren\}, \{M. S.\} and Veltman, \{C. A.\} and A. Verbokkem and I. Verhage and Vink-Klooster, \{H. K.\} and J. Gast-Strookman and K. Janssen and Schrumpf, \{J. A.\} and J. Smit-Bakker and J. Stolk and Tir{\'e}, \{A. C.J.A.\} and \{Van Der Veen\}, H. and Wijffels, \{M. M.E.\} and Willems, \{L. N.A.\} and T. Mauad",

note = "Role of the Funding Source: This was an investigator-initiated trial. The study was funded by the Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center. The funding sources had no role in the design, conduct, and analysis of the study or in the decision to submit the manuscript for publication.",

year = "2009",

month = oct,

day = "20",

doi = "10.7326/0003-4819-151-8-200910200-00004",

language = "English",

volume = "151",

pages = "517--527",

journal = "Annals of Internal Medicine",

issn = "0003-4819",

publisher = "American College of Physicians",

number = "8",

}

Lapperre, TS, Snoeck-Stroband, JB, Gosman, MME, Jansen, DF, Van Schadewijk, A, Thiadens, HA, Vonk, JM, Boezen, HM, Ten Hacken, NHT, Sont, JK, Rabe, KF, Kerstjens, HAM, Hiemstra, PS, Timens, W, Postma, DS, Sterk, PJ, Kauffman, HF, De Reus, D, Barentsen, MDW, Zeinstra-Smit, M, Luteijn, AJ, Van Der Molen, T, Ter Veen, G, Van Maaren, MS, Veltman, CA, Verbokkem, A, Verhage, I, Vink-Klooster, HK, Gast-Strookman, J, Janssen, K, Schrumpf, JA, Smit-Bakker, J, Stolk, J, Tiré, ACJA, Van Der Veen, H, Wijffels, MME, Willems, LNA & Mauad, T 2009, 'Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial', Annals of Internal Medicine, vol. 151, no. 8, pp. 517-527. https://doi.org/10.7326/0003-4819-151-8-200910200-00004

TY - JOUR

T1 - Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease

T2 - A randomized trial

AU - Lapperre, Thérése S.

AU - Snoeck-Stroband, Jiska B.

AU - Gosman, Margot M.E.

AU - Jansen, Désirée F.

AU - Van Schadewijk, Annemarie

AU - Thiadens, Henk A.

AU - Vonk, Judith M.

AU - Boezen, H. Marike

AU - Ten Hacken, Nick H.T.

AU - Sont, Jacob K.

AU - Rabe, Klaus F.

AU - Kerstjens, Huib A.M.

AU - Hiemstra, Pieter S.

AU - Timens, Wim

AU - Postma, Dirkje S.

AU - Sterk, Peter J.

AU - Kauffman, H. F.

AU - De Reus, D.

AU - Barentsen, M. D.W.

AU - Zeinstra-Smit, M.

AU - Luteijn, A. J.

AU - Van Der Molen, T.

AU - Ter Veen, G.

AU - Van Maaren, M. S.

AU - Veltman, C. A.

AU - Verbokkem, A.

AU - Verhage, I.

AU - Vink-Klooster, H. K.

AU - Gast-Strookman, J.

AU - Janssen, K.

AU - Schrumpf, J. A.

AU - Smit-Bakker, J.

AU - Stolk, J.

AU - Tiré, A. C.J.A.

AU - Van Der Veen, H.

AU - Wijffels, M. M.E.

AU - Willems, L. N.A.

AU - Mauad, T.

N1 - Role of the Funding Source: This was an investigator-initiated trial. The study was funded by the Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center. The funding sources had no role in the design, conduct, and analysis of the study or in the decision to submit the manuscript for publication.

PY - 2009/10/20

Y1 - 2009/10/20

N2 - Background: Inhaled corticosteroids (ICSs) and long-acting β2-agonists (LABAs) are used to treat moderate to severe chronic obstructive pulmonary disease (COPD). Objective: To determine whether long-term ICS therapy, with and without LABAs, reduces inflammation and improves pulmonary function in COPD. Design: Randomized, placebo-controlled trial. (ClinicalTrials.gov registration number: NCT00158847) Setting: 2 university medical centers in The Netherlands. Patients: 114 steroid-naive current or former smokers with moderate to severe COPD. Measurements: Cell counts in bronchial biopsies and sputum (primary outcome); methacholine responsiveness at baseline, 6, and 30 months; and clinical outcomes every 3 months. Intervention: Random assignment by minimization method to receive fluticasone propionate, 500 μg twice daily, for 6 months (n = 31) or 30 months (n = 26); fluticasone, 500 μg twice daily, and salmeterol, 50 μg twice daily, for 30 months (single inhaler; n = 28); or placebo twice daily (n = 29). Results: 101 patients were greater than 70% adherent to therapy. Fluticasone therapy decreased counts of mucosal CD3+ cells (-55% [95% CI, -74% to -22%]; P - 0.004), CD4- cells (-78% [CI, -88% to 60%]; P < 0.001), CD8+ cells (-57% [CI, -77% to -18%]; P = 0.010), and mast cells (-38% [CI, -60% to -2%]; P = 0.039) and reduced hyperresponsiveness (P = 0.036) versus placebo at 6 months, with effects maintained after 30 months. Fluticasone therapy for 30 months reduced mast cell count and increased eosinophil count and percentage of intact epithelium, with accompanying reductions in sputum neutrophil, macrophage, and lymphocyte counts and improvements in FEV1 decline, dyspnea, and quality of life. Reductions in inflammatory cells correlated with clinical improvements. Discontinuing fluticasone therapy at 6 months increased counts of CD3+ cells (120% [CI, 24% to 289%]; P = 0.007), mast cells (218% [CI, 99% to 407%]; P < 0.001), and plasma cells (118% [CI, 9% to 336%]; P = 0.028) and worsened clinical outcome. Adding salmeterol improved FEV1 level. Limitations: The study was not designed to evaluate clinical outcomes. Measurement of primary outcome was not available for 24% of patients at 30 months. Conclusion: ICS therapy decreases inflammation and can attenuate decline in lung function in steroid-naive patients with moderate to severe COPD. Adding LABAs does not enhance these effects. Primary Funding Source: Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center.

AB - Background: Inhaled corticosteroids (ICSs) and long-acting β2-agonists (LABAs) are used to treat moderate to severe chronic obstructive pulmonary disease (COPD). Objective: To determine whether long-term ICS therapy, with and without LABAs, reduces inflammation and improves pulmonary function in COPD. Design: Randomized, placebo-controlled trial. (ClinicalTrials.gov registration number: NCT00158847) Setting: 2 university medical centers in The Netherlands. Patients: 114 steroid-naive current or former smokers with moderate to severe COPD. Measurements: Cell counts in bronchial biopsies and sputum (primary outcome); methacholine responsiveness at baseline, 6, and 30 months; and clinical outcomes every 3 months. Intervention: Random assignment by minimization method to receive fluticasone propionate, 500 μg twice daily, for 6 months (n = 31) or 30 months (n = 26); fluticasone, 500 μg twice daily, and salmeterol, 50 μg twice daily, for 30 months (single inhaler; n = 28); or placebo twice daily (n = 29). Results: 101 patients were greater than 70% adherent to therapy. Fluticasone therapy decreased counts of mucosal CD3+ cells (-55% [95% CI, -74% to -22%]; P - 0.004), CD4- cells (-78% [CI, -88% to 60%]; P < 0.001), CD8+ cells (-57% [CI, -77% to -18%]; P = 0.010), and mast cells (-38% [CI, -60% to -2%]; P = 0.039) and reduced hyperresponsiveness (P = 0.036) versus placebo at 6 months, with effects maintained after 30 months. Fluticasone therapy for 30 months reduced mast cell count and increased eosinophil count and percentage of intact epithelium, with accompanying reductions in sputum neutrophil, macrophage, and lymphocyte counts and improvements in FEV1 decline, dyspnea, and quality of life. Reductions in inflammatory cells correlated with clinical improvements. Discontinuing fluticasone therapy at 6 months increased counts of CD3+ cells (120% [CI, 24% to 289%]; P = 0.007), mast cells (218% [CI, 99% to 407%]; P < 0.001), and plasma cells (118% [CI, 9% to 336%]; P = 0.028) and worsened clinical outcome. Adding salmeterol improved FEV1 level. Limitations: The study was not designed to evaluate clinical outcomes. Measurement of primary outcome was not available for 24% of patients at 30 months. Conclusion: ICS therapy decreases inflammation and can attenuate decline in lung function in steroid-naive patients with moderate to severe COPD. Adding LABAs does not enhance these effects. Primary Funding Source: Netherlands Organization for Scientific Research, Netherlands Asthma Foundation, GlaxoSmithKline of The Netherlands, University Medical Center Groningen, and Leiden University Medical Center.

UR - https://www.scopus.com/pages/publications/70350219119

U2 - 10.7326/0003-4819-151-8-200910200-00004

DO - 10.7326/0003-4819-151-8-200910200-00004

M3 - Article

C2 - 19841453

AN - SCOPUS:70350219119

SN - 0003-4819

VL - 151

SP - 517

EP - 527

JO - Annals of Internal Medicine

JF - Annals of Internal Medicine

IS - 8

ER -

Effect of fluticasone with and without salmeterol on pulmonary outcomes in chronic obstructive pulmonary disease: A randomized trial

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