A Randomized Trial of Drug Route in Out-of-Hospital Cardiac Arrest

Keith Couper; Chen Ji; Charles D Deakin; Rachael T Fothergill; Jerry P Nolan; John B Long; James M Mason; Felix Michelet; Chloe Norman; Henry Nwankwo; Tom Quinn; Anne-Marie Slowther; Michael A Smyth; Kath R Starr; Alison Walker; Sara Wood; Steve Bell; Gemma Bradley; Martina Brown; Shona Brown; Emma Burrow; Karl Charlton; Andrew Claxton Dip; Victoria Dra'gon; Christine Evans; Jakob Falloon; Theresa Foster; Justin Kearney; Nigel Lang; Matthew Limmer; Adam Mellett-Smith; Joshua Miller; Carla Mills; Ria Osborne; Nigel Rees; Robert E S Spaight; Gemma L Squires; Belinda Tibbetts; Michelle Waddington; Gregory A Whitley; Jason V Wiles; Julia Williams; Sarah Wiltshire; Adam Wright; Ranjit Lall; Gavin D Perkins; PARAMEDIC-3 Collaborators

doi:10.1056/NEJMoa2407780

A Randomized Trial of Drug Route in Out-of-Hospital Cardiac Arrest

N Engl J Med. 2024 Oct 31:10.1056/NEJMoa2407780. doi: 10.1056/NEJMoa2407780. Online ahead of print.

Authors

Keith Couper¹, Chen Ji¹, Charles D Deakin¹, Rachael T Fothergill¹, Jerry P Nolan¹, John B Long¹, James M Mason¹, Felix Michelet¹, Chloe Norman¹, Henry Nwankwo¹, Tom Quinn¹, Anne-Marie Slowther¹, Michael A Smyth¹, Kath R Starr¹, Alison Walker¹, Sara Wood¹, Steve Bell¹, Gemma Bradley¹, Martina Brown¹, Shona Brown¹, Emma Burrow¹, Karl Charlton¹, Andrew Claxton Dip¹, Victoria Dra'gon¹, Christine Evans¹, Jakob Falloon¹, Theresa Foster¹, Justin Kearney¹, Nigel Lang¹, Matthew Limmer¹, Adam Mellett-Smith¹, Joshua Miller¹, Carla Mills¹, Ria Osborne¹, Nigel Rees¹, Robert E S Spaight¹, Gemma L Squires¹, Belinda Tibbetts¹, Michelle Waddington¹, Gregory A Whitley¹, Jason V Wiles¹, Julia Williams¹, Sarah Wiltshire¹, Adam Wright¹, Ranjit Lall¹, Gavin D Perkins¹; PARAMEDIC-3 Collaborators

Affiliation

¹ From the Warwick Medical School, Clinical Trials Unit, University of Warwick (K.C., C.J., J.P.N., J.B.L., J.M.M., F.M., C.N., H.N., A.-M.S., M.A.S., K.R.S., S.W., R.L., G.D.P.), and the Critical Care Unit, University Hospital Coventry and Warwickshire NHS Trust (M.A.S.), Coventry, Devon Air Ambulance (N.L., B.T.) and South Western Ambulance Service NHS Foundation Trust (R.O., S.W.), Exeter, East Midlands Ambulance Service NHS Trust, Nottingham (R.E.S.S., G.L.S., G.A.W.), East of England Ambulance Service NHS Trust, Cambridge (S.B., T.F.), Kingston University (T.Q.) and London Ambulance Service NHS Trust (R.T.F., J.K., J.F., A.M.-S.), London, North East Ambulance Service NHS Foundation Trust, Newcastle upon Tyne (K.C., E.B., M.L.), North West Ambulance Service NHS Trust, Bolton (S.B., A. Wright, M.W.), South Central Ambulance Service NHS Foundation Trust, Bicester (C.D.D., M.B., A.C., V.D.), South East Coast Ambulance Service NHS Foundation Trust, Crawley (G.B., J.W.), Welsh Ambulance Services University NHS Trust, Cwmbran (C.M., N.R.), West Midlands Ambulance Service University NHS Foundation Trust, Brierley Hill (A. Walker, C.E., J.M., J.V.W.), the Critical Care Unit, University Hospitals Birmingham NHS Foundation Trust, Birmingham (G.D.P., K.C.), the Emergency Department, Harrogate and District NHS Foundation Trust, Harrogate (A. Walker), the Department of Anaesthesia, Royal United Hospitals Bath NHS Foundation Trust, Bath (J.P.N.), University Hospital Southampton NHS Foundation Trust, Southampton (C.D.D.), and the University of Bristol, Bristol (J.P.N.) - all in the United Kingdom.

Abstract

Background: In patients with out-of-hospital cardiac arrest, the effectiveness of drugs such as epinephrine is highly time-dependent. An intraosseous route of drug administration may enable more rapid drug administration than an intravenous route; however, its effect on clinical outcomes is uncertain.

Methods: We conducted a multicenter, open-label, randomized trial across 11 emergency medical systems in the United Kingdom that involved adults in cardiac arrest for whom vascular access for drug administration was needed. Patients were randomly assigned to receive treatment from paramedics by means of an intraosseous-first or intravenous-first vascular access strategy. The primary outcome was survival at 30 days. Key secondary outcomes included any return of spontaneous circulation and favorable neurologic function at hospital discharge (defined by a score of 3 or less on the modified Rankin scale, on which scores range from 0 to 6, with higher scores indicating greater disability). No adjustment for multiplicity was made.

Results: A total of 6082 patients were assigned to a trial group: 3040 to the intraosseous group and 3042 to the intravenous group. At 30 days, 137 of 3030 patients (4.5%) in the intraosseous group and 155 of 3034 (5.1%) in the intravenous group were alive (adjusted odds ratio, 0.94; 95% confidence interval [CI], 0.68 to 1.32; P = 0.74). At the time of hospital discharge, a favorable neurologic outcome was observed in 80 of 2994 patients (2.7%) in the intraosseous group and in 85 of 2986 (2.8%) in the intravenous group (adjusted odds ratio, 0.91; 95% CI, 0.57 to 1.47); a return of spontaneous circulation at any time occurred in 1092 of 3031 patients (36.0%) and in 1186 of 3035 patients (39.1%), respectively (adjusted odds ratio, 0.86; 95% CI, 0.76 to 0.97). During the trial, one adverse event, which occurred in the intraosseous group, was reported.

Conclusions: Among adults with out-of-hospital cardiac arrest requiring drug therapy, the use of an intraosseous-first vascular access strategy did not result in higher 30-day survival than an intravenous-first strategy. (Funded by the National Institute for Health and Care Research; PARAMEDIC-3 ISRCTN Registry number, ISRCTN14223494.).

Associated data

ISRCTN/ISRCTN14223494

Abstract

Associated data

Grants and funding