The University of Southampton
×
Filter your search:
University of Southampton Institutional Repository

Effect of low-dose intracoronary alteplase during primary percutaneous coronary intervention on microvascular obstruction in patients with acute myocardial infarction: A randomized clinical trial

Effect of low-dose intracoronary alteplase during primary percutaneous coronary intervention on microvascular obstruction in patients with acute myocardial infarction: A randomized clinical trial
Effect of low-dose intracoronary alteplase during primary percutaneous coronary intervention on microvascular obstruction in patients with acute myocardial infarction: A randomized clinical trial

Importance: Microvascular obstruction commonly affects patients with acute ST-segment elevation myocardial infarction (STEMI) and is associated with adverse outcomes.

Objective: To determine whether a therapeutic strategy involving low-dose intracoronary fibrinolytic therapy with alteplase infused early after coronary reperfusion will reduce microvascular obstruction.

Design, Setting, and Participants: Between March 17, 2016, and December 21, 2017, 440 patients presenting at 11 hospitals in the United Kingdom within 6 hours of STEMI due to a proximal-mid-vessel occlusion of a major coronary artery were randomized in a 1:1:1 dose-ranging trial design. Patient follow-up to 3 months was completed on April 12, 2018.

Interventions: Participants were randomly assigned to treatment with placebo (n = 151), alteplase 10 mg (n = 144), or alteplase 20 mg (n = 145) by manual infusion over 5 to 10 minutes. The intervention was scheduled to occur early during the primary PCI procedure, after reperfusion of the infarct-related coronary artery and before stent implant.

Main Outcomes and Measures: The primary outcome was the amount of microvascular obstruction (% left ventricular mass) demonstrated by contrast-enhanced cardiac magnetic resonance imaging (MRI) conducted from days 2 through 7 after enrollment. The primary comparison was the alteplase 20-mg group vs the placebo group; if not significant, the alteplase 10-mg group vs the placebo group was considered a secondary analysis.

Results: Recruitment stopped on December 21, 2017, because conditional power for the primary outcome based on a prespecified analysis of the first 267 randomized participants was less than 30% in both treatment groups (futility criterion). Among the 440 patients randomized (mean age, 60.5 years; 15% women), the primary end point was achieved in 396 patients (90%), 17 (3.9%) withdrew, and all others were followed up to 3 months. In the primary analysis, the mean microvascular obstruction did not differ between the 20-mg alteplase and placebo groups (3.5% vs 2.3%; estimated difference, 1.16%; 95% CI, -0.08% to 2.41%; P = .32) nor in the analysis of 10-mg alteplase vs placebo groups (2.6% vs 2.3%; estimated difference, 0.29%; 95% CI, -0.76% to 1.35%; P = .74). Major adverse cardiac events (cardiac death, nonfatal MI, unplanned hospitalization for heart failure) occurred in 15 patients (10.1%) in the placebo group, 18 (12.9%) in the 10-mg alteplase group, and 12 (8.2%) in the 20-mg alteplase group.

Conclusions and Relevance: Among patients with acute STEMI presenting within 6 hours of symptoms, adjunctive low-dose intracoronary alteplase given during the primary percutaneous intervention did not reduce microvascular obstruction. The study findings do not support this treatment.

Trial Registration: ClinicalTrials.gov Identifier: NCT02257294.

Aged, Area Under Curve, Cardiac Catheters, Combined Modality Therapy, Coronary Angiography, Coronary Occlusion/drug therapy, Coronary Vessels, Dose-Response Relationship, Drug, Female, Humans, Infusions, Intra-Arterial, Magnetic Resonance Imaging, Male, Middle Aged, Percutaneous Coronary Intervention, Quality of Life, ST Elevation Myocardial Infarction/drug therapy, Tissue Plasminogen Activator/administration & dosage, Treatment Failure, Troponin T/blood
0098-7484
56-68
McCartney, Peter J.
528e0a77-0da8-4f58-a98c-ef26d008fbb2
Eteiba, Hany
4f08065f-3547-412a-83c9-3f5b37777745
Maznyczka, Annette M.
9cd9f743-128d-4644-ba7b-1ccb0ffa4aa9
McEntegart, Margaret
c663c90a-2511-4c90-87eb-0ac05d9ad464
Greenwood, John P.
af864161-94e9-4094-9c1f-85d696682fb7
Muir, Douglas F.
ac518ef9-fb4a-43ce-b57d-fb52a929ebd7
Chowdhary, Saqib
dc1f7414-d2b9-448c-b9f2-da9156aac1bf
Gershlick, Anthony H.
5beb7f92-68f7-41df-ba72-ef3d2cdf20b9
Appleby, Clare
bb8e2e92-71fa-4270-9382-f2923f02c2b1
Cotton, James M.
35dc9802-8e9b-46cd-9a33-7763594da9b8
Wragg, Andrew
7e403a07-92c2-4063-b8d4-0154a60b4ff8
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4
Oldroyd, Keith G.
536fd60e-50d0-4a76-a818-ab6b2b03567f
Lindsay, Mitchell
b175e163-4db8-4787-a7d1-b42554b034d0
Rocchiccioli, J. Paul
a7e2a518-c1d0-4d16-aa85-49d98eeb47ba
Shaukat, Aadil
ccc1e1cb-b707-4ed3-9659-94b30bf41fe9
Good, Richard
a2dcc49e-1b99-4812-ba60-072607bdfca3
Watkins, Stuart
0b6d0a61-ae26-43f0-a06d-404cc110f333
Robertson, Keith
1d515f05-83fd-47a4-9a3d-da0907c8a5a4
Malkin, Christopher
a0bf7f4c-88ed-45ae-af1e-729c8249733f
Martin, Lynn
e3837848-1e72-4bae-b062-07911dd64a74
Gillespie, Lynsey
a4f39f6f-0f97-47ca-9aa7-0c2d731cca60
Ford, Thomas J.
4b931a83-2d6e-4223-8137-c164067b197c
Petrie, Mark C.
f53b1a39-14d9-41ab-a384-6cc78f32183b
Macfarlane, Peter W.
c2cea789-4512-44df-9456-60083d17292e
Tait, R. Campbell
1162c7f2-55fb-428a-92ec-122dc9ed423e
Welsh, Paul
09de190a-183c-444a-aa04-4b57b4cc81b1
Sattar, Naveed
c81a1259-e177-4522-a732-52d8218384f6
Weir, Robin A.
22fdf7d8-99d5-4039-aea9-f1b2ccae218b
Fox, Keith A.
cb14d631-49e0-4eaa-9c31-bc8fa56bcf62
Ford, Ian
9fd64fa3-4f53-4b12-9536-4506f9759585
McConnachie, Alex
c930d8cf-ab00-47e9-a22d-dbcf7a26f039
Berry, Colin
106fbcaa-69ba-45ec-969f-6f18e06680cf
T-TIME Group
McCartney, Peter J.
528e0a77-0da8-4f58-a98c-ef26d008fbb2
Eteiba, Hany
4f08065f-3547-412a-83c9-3f5b37777745
Maznyczka, Annette M.
9cd9f743-128d-4644-ba7b-1ccb0ffa4aa9
McEntegart, Margaret
c663c90a-2511-4c90-87eb-0ac05d9ad464
Greenwood, John P.
af864161-94e9-4094-9c1f-85d696682fb7
Muir, Douglas F.
ac518ef9-fb4a-43ce-b57d-fb52a929ebd7
Chowdhary, Saqib
dc1f7414-d2b9-448c-b9f2-da9156aac1bf
Gershlick, Anthony H.
5beb7f92-68f7-41df-ba72-ef3d2cdf20b9
Appleby, Clare
bb8e2e92-71fa-4270-9382-f2923f02c2b1
Cotton, James M.
35dc9802-8e9b-46cd-9a33-7763594da9b8
Wragg, Andrew
7e403a07-92c2-4063-b8d4-0154a60b4ff8
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4
Oldroyd, Keith G.
536fd60e-50d0-4a76-a818-ab6b2b03567f
Lindsay, Mitchell
b175e163-4db8-4787-a7d1-b42554b034d0
Rocchiccioli, J. Paul
a7e2a518-c1d0-4d16-aa85-49d98eeb47ba
Shaukat, Aadil
ccc1e1cb-b707-4ed3-9659-94b30bf41fe9
Good, Richard
a2dcc49e-1b99-4812-ba60-072607bdfca3
Watkins, Stuart
0b6d0a61-ae26-43f0-a06d-404cc110f333
Robertson, Keith
1d515f05-83fd-47a4-9a3d-da0907c8a5a4
Malkin, Christopher
a0bf7f4c-88ed-45ae-af1e-729c8249733f
Martin, Lynn
e3837848-1e72-4bae-b062-07911dd64a74
Gillespie, Lynsey
a4f39f6f-0f97-47ca-9aa7-0c2d731cca60
Ford, Thomas J.
4b931a83-2d6e-4223-8137-c164067b197c
Petrie, Mark C.
f53b1a39-14d9-41ab-a384-6cc78f32183b
Macfarlane, Peter W.
c2cea789-4512-44df-9456-60083d17292e
Tait, R. Campbell
1162c7f2-55fb-428a-92ec-122dc9ed423e
Welsh, Paul
09de190a-183c-444a-aa04-4b57b4cc81b1
Sattar, Naveed
c81a1259-e177-4522-a732-52d8218384f6
Weir, Robin A.
22fdf7d8-99d5-4039-aea9-f1b2ccae218b
Fox, Keith A.
cb14d631-49e0-4eaa-9c31-bc8fa56bcf62
Ford, Ian
9fd64fa3-4f53-4b12-9536-4506f9759585
McConnachie, Alex
c930d8cf-ab00-47e9-a22d-dbcf7a26f039
Berry, Colin
106fbcaa-69ba-45ec-969f-6f18e06680cf

McCartney, Peter J., Eteiba, Hany, Maznyczka, Annette M., McEntegart, Margaret, Greenwood, John P., Muir, Douglas F., Chowdhary, Saqib, Gershlick, Anthony H., Appleby, Clare, Cotton, James M., Wragg, Andrew, Curzen, Nick, Oldroyd, Keith G., Lindsay, Mitchell, Rocchiccioli, J. Paul, Shaukat, Aadil, Good, Richard, Watkins, Stuart, Robertson, Keith, Malkin, Christopher, Martin, Lynn, Gillespie, Lynsey, Ford, Thomas J., Petrie, Mark C., Macfarlane, Peter W., Tait, R. Campbell, Welsh, Paul, Sattar, Naveed, Weir, Robin A., Fox, Keith A., Ford, Ian, McConnachie, Alex and Berry, Colin , T-TIME Group (2019) Effect of low-dose intracoronary alteplase during primary percutaneous coronary intervention on microvascular obstruction in patients with acute myocardial infarction: A randomized clinical trial. JAMA, 321 (1), 56-68. (doi:10.1001/jama.2018.19802).

Record type: Article

Abstract

Importance: Microvascular obstruction commonly affects patients with acute ST-segment elevation myocardial infarction (STEMI) and is associated with adverse outcomes.

Objective: To determine whether a therapeutic strategy involving low-dose intracoronary fibrinolytic therapy with alteplase infused early after coronary reperfusion will reduce microvascular obstruction.

Design, Setting, and Participants: Between March 17, 2016, and December 21, 2017, 440 patients presenting at 11 hospitals in the United Kingdom within 6 hours of STEMI due to a proximal-mid-vessel occlusion of a major coronary artery were randomized in a 1:1:1 dose-ranging trial design. Patient follow-up to 3 months was completed on April 12, 2018.

Interventions: Participants were randomly assigned to treatment with placebo (n = 151), alteplase 10 mg (n = 144), or alteplase 20 mg (n = 145) by manual infusion over 5 to 10 minutes. The intervention was scheduled to occur early during the primary PCI procedure, after reperfusion of the infarct-related coronary artery and before stent implant.

Main Outcomes and Measures: The primary outcome was the amount of microvascular obstruction (% left ventricular mass) demonstrated by contrast-enhanced cardiac magnetic resonance imaging (MRI) conducted from days 2 through 7 after enrollment. The primary comparison was the alteplase 20-mg group vs the placebo group; if not significant, the alteplase 10-mg group vs the placebo group was considered a secondary analysis.

Results: Recruitment stopped on December 21, 2017, because conditional power for the primary outcome based on a prespecified analysis of the first 267 randomized participants was less than 30% in both treatment groups (futility criterion). Among the 440 patients randomized (mean age, 60.5 years; 15% women), the primary end point was achieved in 396 patients (90%), 17 (3.9%) withdrew, and all others were followed up to 3 months. In the primary analysis, the mean microvascular obstruction did not differ between the 20-mg alteplase and placebo groups (3.5% vs 2.3%; estimated difference, 1.16%; 95% CI, -0.08% to 2.41%; P = .32) nor in the analysis of 10-mg alteplase vs placebo groups (2.6% vs 2.3%; estimated difference, 0.29%; 95% CI, -0.76% to 1.35%; P = .74). Major adverse cardiac events (cardiac death, nonfatal MI, unplanned hospitalization for heart failure) occurred in 15 patients (10.1%) in the placebo group, 18 (12.9%) in the 10-mg alteplase group, and 12 (8.2%) in the 20-mg alteplase group.

Conclusions and Relevance: Among patients with acute STEMI presenting within 6 hours of symptoms, adjunctive low-dose intracoronary alteplase given during the primary percutaneous intervention did not reduce microvascular obstruction. The study findings do not support this treatment.

Trial Registration: ClinicalTrials.gov Identifier: NCT02257294.

This record has no associated files available for download.

More information

Accepted/In Press date: 20 November 2018
Published date: 1 January 2019
Keywords: Aged, Area Under Curve, Cardiac Catheters, Combined Modality Therapy, Coronary Angiography, Coronary Occlusion/drug therapy, Coronary Vessels, Dose-Response Relationship, Drug, Female, Humans, Infusions, Intra-Arterial, Magnetic Resonance Imaging, Male, Middle Aged, Percutaneous Coronary Intervention, Quality of Life, ST Elevation Myocardial Infarction/drug therapy, Tissue Plasminogen Activator/administration & dosage, Treatment Failure, Troponin T/blood

Identifiers

Local EPrints ID: 436097
URI: http://eprints.soton.ac.uk/id/eprint/436097
DOI: doi:10.1001/jama.2018.19802
ISSN: 0098-7484
PURE UUID: e7b074b1-e01e-4ca0-8225-d53a1a708fe0
ORCID for Nick Curzen: ORCID iD orcid.org/0000-0001-9651-7829

Catalogue record

Date deposited: 27 Nov 2019 17:30
Last modified: 17 Mar 2024 03:02

Export record

Altmetrics

Contributors

Author: Peter J. McCartney
Author: Hany Eteiba
Author: Annette M. Maznyczka
Author: Margaret McEntegart
Author: John P. Greenwood
Author: Douglas F. Muir
Author: Saqib Chowdhary
Author: Anthony H. Gershlick
Author: Clare Appleby
Author: James M. Cotton
Author: Andrew Wragg
Author: Nick Curzen ORCID iD
Author: Keith G. Oldroyd
Author: Mitchell Lindsay
Author: J. Paul Rocchiccioli
Author: Aadil Shaukat
Author: Richard Good
Author: Stuart Watkins
Author: Keith Robertson
Author: Christopher Malkin
Author: Lynn Martin
Author: Lynsey Gillespie
Author: Thomas J. Ford
Author: Mark C. Petrie
Author: Peter W. Macfarlane
Author: R. Campbell Tait
Author: Paul Welsh
Author: Naveed Sattar
Author: Robin A. Weir
Author: Keith A. Fox
Author: Ian Ford
Author: Alex McConnachie
Author: Colin Berry
Corporate Author: T-TIME Group

Download statistics

Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.

View more statistics

Library staff additional information
Atom RSS 1.0 RSS 2.0

Contact ePrints Soton: eprints@soton.ac.uk

ePrints Soton supports OAI 2.0 with a base URL of http://eprints.soton.ac.uk/cgi/oai2

This repository has been built using EPrints software, developed at the University of Southampton, but available to everyone to use.

We use cookies to ensure that we give you the best experience on our website. If you continue without changing your settings, we will assume that you are happy to receive cookies on the University of Southampton website.

×