ICare-ACS (Improving Care Processes for Patients with Suspected Acute Coronary Syndrome): A study of cross-system implementation of a National Clinical Pathway

Than, Martin P., Pickering, John W., Dryden, Jeremy M., Lord, Sally J., Aitken, S. Andrew, Aldous, Sally J., Allan, Kate E., Ardagh, Michael W., Bonning, John W.N., Callender, Rosie, Chapman, Laura R.E., Christiansen, Jonathan P., Cromhout, Andre P.J., , Deely, Joanne M., Devlin, Gerard P., Ferrier, Katherine A., Florkowski, Christopher M., Frampton, Christopher M.A., George, Peter M., Hamilton, Gregory J., Jaffe, Allan S., Kerr, Andrew J., Larkin, G. Luke, Makower, Richard M., Matthews, Timothy J.E., , Peacock, W. Frank, Peckler, Bradley F., Van Pelt, Niels C., Poynton, Louise, Richards, A. Mark, Scott, Anthony G., Simmonds, Mark B., Smyth, David, Thomas, Oliver P., To, Andrew C.Y., Du Toit, Stephen A., Troughton, Richard W., & Yates, Kim M. (2018) ICare-ACS (Improving Care Processes for Patients with Suspected Acute Coronary Syndrome): A study of cross-system implementation of a National Clinical Pathway. Circulation, 137(4), pp. 354-363.

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Description

Background: Efforts to safely reduce length of stay for emergency department patients with symptoms suggestive of acute coronary syndrome (ACS) have had mixed success. Few system-wide efforts affecting multiple hospital emergency departments have ever been evaluated. We evaluated the effectiveness of a nationwide implementation of clinical pathways for potential ACS in disparate hospitals.

Methods: This was a multicenter pragmatic stepped-wedge before-and-after trial in 7 New Zealand acute care hospitals with 31 332 patients investigated for suspected ACS with serial troponin measurements. The implementation was a clinical pathway for the assessment of patients with suspected ACS that included a clinical pathway document in paper or electronic format, structured risk stratification, specified time points for electrocardiographic and serial troponin testing within 3 hours of arrival, and directions for combining risk stratification and electrocardiographic and troponin testing in an accelerated diagnostic protocol. Implementation was monitored for >4 months and compared with usual care over the preceding 6 months. The main outcome measure was the odds of discharge within 6 hours of presentation

Results: There were 11 529 participants in the preimplementation phase (range, 284-3465) and 19 803 in the postimplementation phase (range, 395-5039). Overall, the mean 6-hour discharge rate increased from 8.3% (range, 2.7%-37.7%) to 18.4% (6.8%-43.8%). The odds of being discharged within 6 hours increased after clinical pathway implementation. The odds ratio was 2.4 (95% confidence interval, 2.3-2.6). In patients without ACS, the median length of hospital stays decreased by 2.9 hours (95% confidence interval, 2.4-3.4). For patients discharged within 6 hours, there was no change in 30-day major adverse cardiac event rates (0.52% versus 0.44%; P=0.96). In these patients, no adverse event occurred when clinical pathways were correctly followed.

Conclusions: Implementation of clinical pathways for suspected ACS reduced the length of stay and increased the proportions of patients safely discharged within 6 hours. Clinical Trial Registration: URL: https://www.anzctr.org.au/ (Australian and New Zealand Clinical Trials Registry). Unique identifier: ACTRN12617000381381.

Impact and interest:

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ID Code: 197672
Item Type: Contribution to Journal (Journal Article)
Refereed: Yes
ORCID iD:
Parsonage, William A.orcid.org/0000-0002-0223-5378
Measurements or Duration: 10 pages
Keywords: acute coronary syndrome, clinical protocols, critical pathways, emergency service, hospital, troponin
DOI: 10.1161/CIRCULATIONAHA.117.031984
ISSN: 0009-7322
Pure ID: 46540930
Divisions: Past > QUT Faculties & Divisions > Faculty of Health
Funding Information: Funding was provided by a grant from the Health Research Council of New Zealand (HRC 14/711). Emergency Department (M.P.T., J.W.P., M.W.A., R.C., J.M.D., O.P.T., J.M.D.) and Department of Cardiology (S.J.A., D.S., R.W.T.), Christchurch Hospital, New Zealand. Department of Medicine, Christchurch Heart Institute, University of Otago, New Zealand (J.W.P., C.M.A.F., P.M.G., A.M.R., R.W.T.). Department of Cardiology (N.C.v.P.), Middlemore Hospital, Auckland, New Zealand. Department of Epidemiology and Medical Statistics, University of Notre Dame, Sydney Campus, New South Wales, Australia (S.J.L.). National Health and Medical Research Council Clinical Trials Centre, University
Copyright Owner: 2017 American Heart Association, Inc
Copyright Statement: This work is covered by copyright. Unless the document is being made available under a Creative Commons Licence, you must assume that re-use is limited to personal use and that permission from the copyright owner must be obtained for all other uses. If the document is available under a Creative Commons License (or other specified license) then refer to the Licence for details of permitted re-use. It is a condition of access that users recognise and abide by the legal requirements associated with these rights. If you believe that this work infringes copyright please provide details by email to qut.copyright@qut.edu.au
Deposited On: 17 Mar 2020 05:13
Last Modified: 28 Jun 2024 21:14

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