Effect of PCI on quality of life in patients with stable coronary disease

William S Weintraub; John A Spertus; Paul Kolm; David J Maron; Zefeng Zhang; Claudine Jurkovitz; Wei Zhang; Pamela M Hartigan; Cheryl Lewis; Emir Veledar; Jim Bowen; Sandra B Dunbar; Christi Deaton; Stanley Kaufman; Robert A O'Rourke; Ron Goeree; Paul G Barnett; Koon K Teo; William E Boden; COURAGE Trial Research Group; G B J Mancini

doi:10.1056/NEJMoa072771

Effect of PCI on quality of life in patients with stable coronary disease

N Engl J Med. 2008 Aug 14;359(7):677-87. doi: 10.1056/NEJMoa072771.

Collaborators

COURAGE Trial Research Group:
W E Boden, R A O'Rourke, K K Teo, P M Hartigan, W Weintraub, D Maron, G B J Mancini, W E Weintraub, W E Boden, R A O'Rourke, K K Teo, P M Hartigan, M Knudtson, D J Maron, E Bates, A S Blaustein, D C Booth, R G Carere, S G Ellis, G Gosselin, G Gau, A K Jacobs, S B King 3rd, W J Kostuk, C Harris, J Spertus, P Peduzzi, T Ryan, B Turnbull, T Feldman, R O Bonow, W L Haskell, P Diehr, P Lachenbruch, D D Waters, D E Johnstone, L S Cohen, B Cantin, W D Hager, F F Samaha, J L Januzzi, J Arrighi, B Chaitman, W S Weintraub, P Hartigan, R A O'Rourke, W E Boden, P Barnett, J Spertus, R Goeree, D Maron, W E Boden, R A O'Rourke, K K Teo, W W Weintraub, P Peduzzi, M Antonelli, J Smith, R Kilstrom, B Hunter, M Edgington, E Petrokaitis, L Durant, S O'Neil, T M Economou, J Nabors, P Collins, A Kossack, M Sather, C Harris, W Gagne, C Fye, R Marottoli, H G Allore, D G Beckwith, W Farrell, R C Feldman, R Mehta, J C Neiderman, E B Perry, S Kasl, M Zeman, T J O'Leary, G D Huang, W E Boden, M Dada, K Potter, R A O'Rourke, P Casperson, A O'Shea, G Jordan, K K Teo, J A Piette, G Woodcock, W S Weintraub, P Barnett, S Chen, R Goeree, B O'Brien, C Henderson, G B John Mancini, E Yeoh, J Ladenson, V Thompson, D Gibson, L Mischle, V Luzzi, T G Cole, J McDowell, B Chaitman, T Bertran, J Bussen, C Moore, D Berman, G Germano, J Gerlach, R Littman, R Miranda-Peats, A Hurayt, K Calfas, J Sallis, G L Freeman, R A O'Rourke, J Bolton, P Freeman, R Mercado-Young, P Baker, A Blaustein, C Rowe, K G Morris, S Hoffman, S P Sedlis, M K Scott, E Anteola, C Duvernoy, M Starling, C Majors, K Syzmanski, D C Booth, M L Shockey, R Zoble, I Fernandez, K Bell, K G Lehmann, J Dinkelspiel, M Abel, A Sorley, M W Sheldon, M Crawford, K Wagoner, E Murphy, K Avalos, J D Rossen, D Jagasia, A Ollinger, K Schneider, B Molavi, L Garza, J Saucedo, P Barton, R Pacheco, S S Dodson, S Kitchens, K Mavromatis, M Leimbach, Z Forghani, D House, R F Smith, C Mitchell, P Holzapfel, M J Brewer, K Ramanathan, T Touchstone, Z Qualls, W J Kostuk, S Carr, K Sridhar, S Nawaz, C Dion, S Musseau, R-A Poirier, T Sequin, G Gosselin, M Cuso, J Theberge, M Brouillette, P Thibeault, L M Title, P Simon, L Carroll, K Courtney-Cox, N Fitzgerald, C Carter, E A Cohen, E Hsu, L Balleza, V Dzavik, P A Barolet, McLaughlin, C Lazzam, J Lan, A Patel, M Knudtson, D Goodhart, D Lundberg, M Natarajan, G Cappelli, S Savoy, C Miller, M Kutryk, B Strauss, M Freeman, A DiMarco, K Young, A Fry, D O'Donnell, A Fung, C Buller, J Chow, D Marr, R Teskey, F Fitzgerald, E Collings, C Coyle, C Ramsay, A Williston, R Carere, C Thompson, T Nacario, T Williams, W Tymchak, L Harris, C Lazzam, Arlene Carter, D Palisaitis, C Mercure, M Bell, P G Gau, P Berger, T Allison, M E Peterson, T Malibago, R Vicari, M Carroll, N Scallon, L Parker, M Howard, A Snyman, E Bates, S Chetcuti, A Luciano, K McNeely, P Mahrer, S Reyes, R Browning, P Scutella, J Saucedo, S Sadanandan, A Kugelmass, D vanWieren, L Feddersen, K Husain, J Wells, J O'Keefe, B McAllister, P Kennedy, M Rossen, A Jacobs, A Jacobs, C Berger, S Mayo, D Fine, C Zingariello, J Hutchinson, D Gannon, J I Miller 3rd, S Manoukian, T Arnold, F Kiernan, M Dada, K Potter, D Murphy, A Kugelmass, R Pangilinan, R Schwartz, L Caufield, R Smith, D Hansen, C Mitchell, P Holzapfel, M J Brewer, R Carhart, A Pennella, M Jones, S G Ellis, C Stevenson, R J Krone, J Humphrey, K M Luepke, C Appleton, M Crawford, J Wisbey, L Wood, B Pyle, M E Stillabower, A DiSabatino, M Davidson, R Hendel, J Mathien

Affiliation

¹ Christiana Care Health System, Newark, DE 19718, USA. wweintraub@christianacare.org

PMID: 18703470
DOI: 10.1056/NEJMoa072771

Abstract

Background: It has not been clearly established whether percutaneous coronary intervention (PCI) can provide an incremental benefit in quality of life over that provided by optimal medical therapy among patients with chronic coronary artery disease.

Methods: We randomly assigned 2287 patients with stable coronary disease to PCI plus optimal medical therapy or to optimal medical therapy alone. We assessed angina-specific health status (with the use of the Seattle Angina Questionnaire) and overall physical and mental function (with the use of the RAND 36-item health survey [RAND-36]).

Results: At baseline, 22% of the patients were free of angina. At 3 months, 53% of the patients in the PCI group and 42% in the medical-therapy group were angina-free (P<0.001). Baseline mean (+/-SD) Seattle Angina Questionnaire scores (which range from 0 to 100, with higher scores indicating better health status) were 66+/-25 for physical limitations, 54+/-32 for angina stability, 69+/-26 for angina frequency, 87+/-16 for treatment satisfaction, and 51+/-25 for quality of life. By 3 months, these scores had increased in the PCI group, as compared with the medical-therapy group, to 76+/-24 versus 72+/-23 for physical limitation (P=0.004), 77+/-28 versus 73+/-27 for angina stability (P=0.002), 85+/-22 versus 80+/-23 for angina frequency (P<0.001), 92+/-12 versus 90+/-14 for treatment satisfaction (P<0.001), and 73+/-22 versus 68+/-23 for quality of life (P<0.001). In general, patients had an incremental benefit from PCI for 6 to 24 months; patients with more severe angina had a greater benefit from PCI. Similar incremental benefits from PCI were seen in some but not all RAND-36 domains. By 36 months, there was no significant difference in health status between the treatment groups.

Conclusions: Among patients with stable angina, both those treated with PCI and those treated with optimal medical therapy alone had marked improvements in health status during follow-up. The PCI group had small, but significant, incremental benefits that disappeared by 36 months. (ClinicalTrials.gov number, NCT00007657.)

2008 Massachusetts Medical Society

Publication types

Multicenter Study
Randomized Controlled Trial

MeSH terms

Adrenergic beta-Antagonists / therapeutic use
Amlodipine / therapeutic use
Angina Pectoris / drug therapy*
Angina Pectoris / etiology
Angina Pectoris / psychology
Angina Pectoris / therapy*
Angioplasty, Balloon, Coronary*
Aspirin / therapeutic use
Calcium Channel Blockers / therapeutic use
Clopidogrel
Combined Modality Therapy
Coronary Disease / complications
Coronary Disease / therapy
Cross-Over Studies
Drug Therapy, Combination
Female
Health Status
Humans
Isosorbide Dinitrate / therapeutic use
Male
Metoprolol / therapeutic use
Middle Aged
Patient Satisfaction
Platelet Aggregation Inhibitors / therapeutic use
Quality of Life*
Stents
Surveys and Questionnaires
Ticlopidine / analogs & derivatives
Ticlopidine / therapeutic use
Vasodilator Agents / therapeutic use

Substances

Adrenergic beta-Antagonists
Calcium Channel Blockers
Platelet Aggregation Inhibitors
Vasodilator Agents
Amlodipine
Clopidogrel
Metoprolol
Isosorbide Dinitrate
Ticlopidine
Aspirin

Associated data

ClinicalTrials.gov/NCT00007657