The University of Southampton
University of Southampton Institutional Repository

Intracoronary abciximab and aspriration thrombectomy in patients with large anterior myocardial infarction: the INFUSE-AMI randomized trial

Intracoronary abciximab and aspriration thrombectomy in patients with large anterior myocardial infarction: the INFUSE-AMI randomized trial
Intracoronary abciximab and aspriration thrombectomy in patients with large anterior myocardial infarction: the INFUSE-AMI randomized trial
CONTEXT: Thrombus embolization during percutaneous coronary intervention (PCI) in ST-segment elevation myocardial infarction (STEMI) is common and results in suboptimal myocardial perfusion and increased infarct size. Two strategies proposed to reduce distal embolization and improve outcomes after primary PCI are bolus intracoronary abciximab and manual aspiration thrombectomy.

OBJECTIVE: To determine whether bolus intracoronary abciximab, manual aspiration thrombectomy, or both reduce infarct size in high-risk patients with STEMI.

DESIGN, SETTING, AND PATIENTS: Between November 28, 2009, and December 2, 2011, 452 patients presenting at 37 sites in 6 countries within 4 hours of STEMI due to proximal or mid left anterior descending artery occlusion undergoing primary PCI with bivalirudin anticoagulation were randomized in an open-label, 2 x 2 factorial design to bolus intracoronary abciximab delivered locally at the infarct lesion site vs no abciximab and to manual aspiration thrombectomy vs no thrombectomy.

INTERVENTIONS: A 0.25-mg/kg bolus of abciximab was administered at the site of the infarct lesion via a local drug delivery catheter. Manual aspiration thrombectomy was performed with a 6 F aspiration catheter.

MAIN OUTCOME MEASURES: Primary end point: infarct size (percentage of total left ventricular mass) at 30 days assessed by cardiac magnetic resonance imaging (cMRI) in the abciximab vs no abciximab groups (pooled across the aspiration randomization); major secondary end point: 30-day infarct size in the aspiration vs no aspiration groups (pooled across the abciximab randomization).

RESULTS: Evaluable cMRI results at 30 days were present in 181 and 172 patients randomized to intracoronary abciximab vs no abciximab, respectively, and in 174 and 179 patients randomized to manual aspiration vs no aspiration, respectively. Patients randomized to intracoronary abciximab compared with no abciximab had a significant reduction in 30-day infarct size (median, 15.1%; interquartile range [IQR], 6.8%-22.7%; n = 181, vs 17.9% [IQR, 10.3%-25.4%]; n = 172; P = .03). Patients randomized to intracoronary abciximab also had a significant reduction in absolute infarct mass (median, 18.7 g [IQR, 7.4-31.3 g]; n = 184, vs 24.0 g [IQR, 12.1-34.2 g]; n = 175; P = .03) but not abnormal wall motion score (median, 7.0 [IQR, 2.0-10.0]; n = 188, vs 8.0 [IQR, 3.0-10.0]; n = 184; P = .08). Patients randomized to aspiration thrombectomy vs no aspiration had no significant difference in infarct size at 30 days (median, 17.0% [IQR, 9.0%-22.8%]; n = 174, vs 17.3% [IQR, 7.1%-25.5%]; n = 179; P = .51), absolute infarct mass (median, 20.3 g [IQR, 9.7-31.7 g]; n = 178, vs 21.0 g [IQR, 9.1-34.1 g]; n = 181; P = .36), or abnormal wall motion score (median, 7.5 [IQR, 2.0-10.0]; n = 186, vs 7.5 [IQR, 2.0-10.0]; n = 186; P = .89).

CONCLUSION: In patients with large anterior STEMI presenting early after symptom onset and undergoing primary PCI with bivalirudin anticoagulation, infarct size at 30 days was significantly reduced by bolus intracoronary abciximab delivered to the infarct lesion site but not by manual aspiration thrombectomy.

TRIAL REGISTRATION: clinicaltrials.gov Identifier: NCT00976521.

0098-7484
1817-1826
Stone, G.W.
045ed82f-285e-48af-a334-c50844487890
Maehara, A.
26c22290-824f-4777-963d-a7b323e144d8
Witzenbichler, B.
4324a7fc-24e9-476b-8c6e-2d306b68803a
Parise, H.
e6de5f17-9469-440b-a0e5-a9279f7ef54b
Godlewski, J.
d5f1aafa-fc86-46a2-84a9-a9b6b6094540
Dambrink, J.H.
2f17e07d-f6ed-4476-b9bb-255787e0103a
Ochala, A.
f8e18ad8-223b-4472-a7d1-e0f2fdda9826
Carlton, T.W.
4b54bfc6-ead7-477f-ad33-62e2f71fcf53
Cristea, E.
8843e1ba-fac0-4f27-85c7-60f229eaebd2
Wolff, S.D.
546d638d-06fa-4ea6-a2a4-cbc99feadc15
Brener, S.J.
def9b40e-8ab1-4ed8-a951-129297fc7717
Chowdhary, S.
1f9a2be6-f844-435c-a490-64255b3783d9
El-Omar, M.
e51f6234-8856-4314-a0a1-b93979293529
Neunteufl, T.
ffc9d6e5-2367-48f9-9271-1180db9e768f
Metzger, D.C.
8b758223-bec4-4af6-beb7-b3fc414b7c05
Karwoski, T.
9319e068-9be6-4b76-8ee2-3db2aa275ca1
Dizon, J.M.
a38e9186-e359-4925-ade4-f73db70a469c
Mehran, R.
742c3166-2d13-4761-a300-3e0742129b01
Gibson, C.M.
f3e067ff-711c-4c80-9bfa-27fff2f5c127
Curzen, N.
70f3ea49-51b1-418f-8e56-8210aef1abf4
INFUSE-AMI Investigators
Stone, G.W.
045ed82f-285e-48af-a334-c50844487890
Maehara, A.
26c22290-824f-4777-963d-a7b323e144d8
Witzenbichler, B.
4324a7fc-24e9-476b-8c6e-2d306b68803a
Parise, H.
e6de5f17-9469-440b-a0e5-a9279f7ef54b
Godlewski, J.
d5f1aafa-fc86-46a2-84a9-a9b6b6094540
Dambrink, J.H.
2f17e07d-f6ed-4476-b9bb-255787e0103a
Ochala, A.
f8e18ad8-223b-4472-a7d1-e0f2fdda9826
Carlton, T.W.
4b54bfc6-ead7-477f-ad33-62e2f71fcf53
Cristea, E.
8843e1ba-fac0-4f27-85c7-60f229eaebd2
Wolff, S.D.
546d638d-06fa-4ea6-a2a4-cbc99feadc15
Brener, S.J.
def9b40e-8ab1-4ed8-a951-129297fc7717
Chowdhary, S.
1f9a2be6-f844-435c-a490-64255b3783d9
El-Omar, M.
e51f6234-8856-4314-a0a1-b93979293529
Neunteufl, T.
ffc9d6e5-2367-48f9-9271-1180db9e768f
Metzger, D.C.
8b758223-bec4-4af6-beb7-b3fc414b7c05
Karwoski, T.
9319e068-9be6-4b76-8ee2-3db2aa275ca1
Dizon, J.M.
a38e9186-e359-4925-ade4-f73db70a469c
Mehran, R.
742c3166-2d13-4761-a300-3e0742129b01
Gibson, C.M.
f3e067ff-711c-4c80-9bfa-27fff2f5c127
Curzen, N.
70f3ea49-51b1-418f-8e56-8210aef1abf4

Stone, G.W., Maehara, A., Witzenbichler, B., Parise, H., Godlewski, J., Dambrink, J.H., Ochala, A., Carlton, T.W., Cristea, E., Wolff, S.D., Brener, S.J., Chowdhary, S., El-Omar, M., Neunteufl, T., Metzger, D.C., Karwoski, T., Dizon, J.M., Mehran, R., Gibson, C.M. and Curzen, N. , INFUSE-AMI Investigators (2012) Intracoronary abciximab and aspriration thrombectomy in patients with large anterior myocardial infarction: the INFUSE-AMI randomized trial. JAMA, 307 (17), 1817-1826. (doi:10.1001/jama.2012.421). (PMID:22447888)

Record type: Article

Abstract

CONTEXT: Thrombus embolization during percutaneous coronary intervention (PCI) in ST-segment elevation myocardial infarction (STEMI) is common and results in suboptimal myocardial perfusion and increased infarct size. Two strategies proposed to reduce distal embolization and improve outcomes after primary PCI are bolus intracoronary abciximab and manual aspiration thrombectomy.

OBJECTIVE: To determine whether bolus intracoronary abciximab, manual aspiration thrombectomy, or both reduce infarct size in high-risk patients with STEMI.

DESIGN, SETTING, AND PATIENTS: Between November 28, 2009, and December 2, 2011, 452 patients presenting at 37 sites in 6 countries within 4 hours of STEMI due to proximal or mid left anterior descending artery occlusion undergoing primary PCI with bivalirudin anticoagulation were randomized in an open-label, 2 x 2 factorial design to bolus intracoronary abciximab delivered locally at the infarct lesion site vs no abciximab and to manual aspiration thrombectomy vs no thrombectomy.

INTERVENTIONS: A 0.25-mg/kg bolus of abciximab was administered at the site of the infarct lesion via a local drug delivery catheter. Manual aspiration thrombectomy was performed with a 6 F aspiration catheter.

MAIN OUTCOME MEASURES: Primary end point: infarct size (percentage of total left ventricular mass) at 30 days assessed by cardiac magnetic resonance imaging (cMRI) in the abciximab vs no abciximab groups (pooled across the aspiration randomization); major secondary end point: 30-day infarct size in the aspiration vs no aspiration groups (pooled across the abciximab randomization).

RESULTS: Evaluable cMRI results at 30 days were present in 181 and 172 patients randomized to intracoronary abciximab vs no abciximab, respectively, and in 174 and 179 patients randomized to manual aspiration vs no aspiration, respectively. Patients randomized to intracoronary abciximab compared with no abciximab had a significant reduction in 30-day infarct size (median, 15.1%; interquartile range [IQR], 6.8%-22.7%; n = 181, vs 17.9% [IQR, 10.3%-25.4%]; n = 172; P = .03). Patients randomized to intracoronary abciximab also had a significant reduction in absolute infarct mass (median, 18.7 g [IQR, 7.4-31.3 g]; n = 184, vs 24.0 g [IQR, 12.1-34.2 g]; n = 175; P = .03) but not abnormal wall motion score (median, 7.0 [IQR, 2.0-10.0]; n = 188, vs 8.0 [IQR, 3.0-10.0]; n = 184; P = .08). Patients randomized to aspiration thrombectomy vs no aspiration had no significant difference in infarct size at 30 days (median, 17.0% [IQR, 9.0%-22.8%]; n = 174, vs 17.3% [IQR, 7.1%-25.5%]; n = 179; P = .51), absolute infarct mass (median, 20.3 g [IQR, 9.7-31.7 g]; n = 178, vs 21.0 g [IQR, 9.1-34.1 g]; n = 181; P = .36), or abnormal wall motion score (median, 7.5 [IQR, 2.0-10.0]; n = 186, vs 7.5 [IQR, 2.0-10.0]; n = 186; P = .89).

CONCLUSION: In patients with large anterior STEMI presenting early after symptom onset and undergoing primary PCI with bivalirudin anticoagulation, infarct size at 30 days was significantly reduced by bolus intracoronary abciximab delivered to the infarct lesion site but not by manual aspiration thrombectomy.

TRIAL REGISTRATION: clinicaltrials.gov Identifier: NCT00976521.

This record has no associated files available for download.

More information

e-pub ahead of print date: 25 March 2012
Published date: May 2012
Organisations: Human Development & Health

Identifiers

Local EPrints ID: 355262
URI: http://eprints.soton.ac.uk/id/eprint/355262
ISSN: 0098-7484
PURE UUID: 0f7cffea-5b00-4425-acfe-668151cc7d3a
ORCID for N. Curzen: ORCID iD orcid.org/0000-0001-9651-7829

Catalogue record

Date deposited: 19 Aug 2013 13:31
Last modified: 15 Mar 2024 03:23

Export record

Altmetrics

Contributors

Author: G.W. Stone
Author: A. Maehara
Author: B. Witzenbichler
Author: H. Parise
Author: J. Godlewski
Author: J.H. Dambrink
Author: A. Ochala
Author: T.W. Carlton
Author: E. Cristea
Author: S.D. Wolff
Author: S.J. Brener
Author: S. Chowdhary
Author: M. El-Omar
Author: T. Neunteufl
Author: D.C. Metzger
Author: T. Karwoski
Author: J.M. Dizon
Author: R. Mehran
Author: C.M. Gibson
Author: N. Curzen ORCID iD
Corporate Author: INFUSE-AMI Investigators

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

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.

×