Fractional flow reserve and instantaneous wave-free ratio as predictors of the placebo-controlled response to percutaneous coronary intervention in stable coronary artery disease
Fractional flow reserve and instantaneous wave-free ratio as predictors of the placebo-controlled response to percutaneous coronary intervention in stable coronary artery disease
Background: the Placebo-controlled Trial of Percutaneous Coronary Intervention for the Relief of Stable Angina (ORBITA-2) provided evidence for the role of percutaneous coronary intervention (PCI) for angina relief in stable coronary artery disease (CAD). Fractional flow reserve (FFR) and instantaneous wave-free ratio (iFR) are often used to guide PCI, however their ability to predict placebo-controlled angina improvement is unknown.
Methods: participants with angina, ischemia, and stable CAD were enrolled and antianginal medications were stopped. Participants reported angina episodes daily for 2 weeks using the ORBITA-app. At the research angiogram, FFR and iFR were measured. After sedation and auditory isolation, participants were randomized to PCI or placebo, before entering a 12-week blinded follow-up phase with daily angina reporting. The ability of FFR and iFR, analyzed as continuous variables, to predict the placebo-controlled effect of PCI, was tested using Bayesian proportional odds modelling.
Results: invasive physiology data were available in 279 patients (140 PCI and 139 placebo). The median (IQR) age was 65 years (59.0 to 70.5) and 223 (79.9%) were male. Median FFR was 0.60 (0.46 to 0.73) and median iFR was 0.76 (0.50 to 0.86). The lower the FFR or iFR, the greater the placebo-controlled improvement with PCI across all endpoints. There was strong evidence that a patient with an FFR at the lower quartile would have a greater placebo-controlled improvement in angina symptom score with PCI than a patient at the upper quartile (FFR 0.46 vs. 0.73: OR 2.01, 95% CrI 1.79 to 2.26, Pr(Interaction)>99.9%). Similarly, there was strong evidence that a patient with an iFR at the lower quartile would have a greater placebo controlled improvement in angina symptom score with PCI than a patient with an iFR at the upper quartile (iFR 0.50 vs. 0.86: OR 2.13, 95% CrI 1.87 to 2.45, Pr(Interaction) >99.9%). The relationship between benefit and physiology was seen in both Rose angina and Rose nonangina.
Conclusions: physiological stenosis severity, as measured by FFR and iFR, predicts placebo-controlled angina relief from PCI. Invasive coronary physiology can be used to target PCI to those patients who are most likely to experience benefit.
Foley, Michael J.
5747a6e4-f237-4949-b907-a7fde46bc8f4
Rajkumar, Christopher A.
4d6e383e-4935-436c-8169-2ec20a98cd83
Ahmed-Jushuf, Fiyyaz
76bab8d8-c5c6-49d5-b7ec-25b97c529473
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4
the ORBITA-2 Investigators
Foley, Michael J.
5747a6e4-f237-4949-b907-a7fde46bc8f4
Rajkumar, Christopher A.
4d6e383e-4935-436c-8169-2ec20a98cd83
Ahmed-Jushuf, Fiyyaz
76bab8d8-c5c6-49d5-b7ec-25b97c529473
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4
Foley, Michael J., Rajkumar, Christopher A. and Ahmed-Jushuf, Fiyyaz
,
et al. and the ORBITA-2 Investigators
(2024)
Fractional flow reserve and instantaneous wave-free ratio as predictors of the placebo-controlled response to percutaneous coronary intervention in stable coronary artery disease.
Circulation.
(doi:10.1161/CIRCULATIONAHA.124.072281).
Abstract
Background: the Placebo-controlled Trial of Percutaneous Coronary Intervention for the Relief of Stable Angina (ORBITA-2) provided evidence for the role of percutaneous coronary intervention (PCI) for angina relief in stable coronary artery disease (CAD). Fractional flow reserve (FFR) and instantaneous wave-free ratio (iFR) are often used to guide PCI, however their ability to predict placebo-controlled angina improvement is unknown.
Methods: participants with angina, ischemia, and stable CAD were enrolled and antianginal medications were stopped. Participants reported angina episodes daily for 2 weeks using the ORBITA-app. At the research angiogram, FFR and iFR were measured. After sedation and auditory isolation, participants were randomized to PCI or placebo, before entering a 12-week blinded follow-up phase with daily angina reporting. The ability of FFR and iFR, analyzed as continuous variables, to predict the placebo-controlled effect of PCI, was tested using Bayesian proportional odds modelling.
Results: invasive physiology data were available in 279 patients (140 PCI and 139 placebo). The median (IQR) age was 65 years (59.0 to 70.5) and 223 (79.9%) were male. Median FFR was 0.60 (0.46 to 0.73) and median iFR was 0.76 (0.50 to 0.86). The lower the FFR or iFR, the greater the placebo-controlled improvement with PCI across all endpoints. There was strong evidence that a patient with an FFR at the lower quartile would have a greater placebo-controlled improvement in angina symptom score with PCI than a patient at the upper quartile (FFR 0.46 vs. 0.73: OR 2.01, 95% CrI 1.79 to 2.26, Pr(Interaction)>99.9%). Similarly, there was strong evidence that a patient with an iFR at the lower quartile would have a greater placebo controlled improvement in angina symptom score with PCI than a patient with an iFR at the upper quartile (iFR 0.50 vs. 0.86: OR 2.13, 95% CrI 1.87 to 2.45, Pr(Interaction) >99.9%). The relationship between benefit and physiology was seen in both Rose angina and Rose nonangina.
Conclusions: physiological stenosis severity, as measured by FFR and iFR, predicts placebo-controlled angina relief from PCI. Invasive coronary physiology can be used to target PCI to those patients who are most likely to experience benefit.
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ORBITA2_Physiology_second_resubmission_clean
- Accepted Manuscript
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foley-et-al-2024-fractional-flow-reserve-and-instantaneous-wave-free-ratio-as-predictors-of-the-placebo-controlled
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More information
Accepted/In Press date: 21 October 2024
e-pub ahead of print date: 27 October 2024
Additional Information:
Authors: Michael J Foley, Christopher A Rajkumar, Fiyyaz Ahmed-Jushuf, Florentina Simader, Shayna Chotai, Henry Seligman, Krzysztof Macierzanka, John R Davies, Thomas R Keeble, Peter O’Kane, Peter Haworth, Helen Routledge, Tushar Kotecha, Gerald Clesham, Rupert Williams, Jehangir Din, Sukhjinder S Nijjer, Nick Curzen, Manas Sinha, Ricardo Petraco, James Spratt, Sayan Sen, Graham D Cole, Frank E Harrell, James P Howard, Darrel P Francis, Matthew J Shun-Shin, Rasha Al-Lamee, for the ORBITA-2 investigators.
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Local EPrints ID: 496134
URI: http://eprints.soton.ac.uk/id/eprint/496134
ISSN: 0009-7322
PURE UUID: 0a7eedf6-e5d5-4c31-82ef-674d830b8126
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Date deposited: 05 Dec 2024 17:30
Last modified: 06 Dec 2024 02:40
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Author:
Michael J. Foley
Author:
Christopher A. Rajkumar
Author:
Fiyyaz Ahmed-Jushuf
Corporate Author: et al.
Corporate Author: the ORBITA-2 Investigators
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