Frequently asked questions
Hear you can find answers to frequently asked questions regarding everything from randomization to follow-up.
Yes, visit stepcaretrial.com to see the recruitment status at all sites.
OHCA: Arrest at the ER prior to final report from paramedics, non-admitted patients/relatives/care-givers whom have a cardiac arrest at the hospital or at a doctor’s appointment, patients with repeated cardiac arrests and non-sustained ROSC (<20 min) from the first OHCA at the arrival to the ER (continued events).
IHCA: Admitted patients to the hospital who have a cardiac arrest while at the hospital.
If the exact time of the cardiac arrest is unknown then use the time of call to the dispatch center. This time is recorded, it is accurate and included in the EMS forms.
Based on the intention to treat principle, data should be collected for this patient. However, the treatment goals for MAP, sedation and temperature will be up to the treating clinician. In these cases it may be an option to slightly delay the randomization until the performance of the CT brain, if there is a clear suspicion of an intracranial hemorrhage.
No, if the GCS was high and the patient clearly obeyed commands after the OHCA then the patient should not be enrolled into STEPCARE. It is unlikely for the patient to be completely conscious after the arrest and then develop severe hypoxic brain injury.
No the patient is not eligible and should be screened out using the criteria “Unconscious - NO”. This is because the reduced level of consciousness occurred due to a different event than the original OHCA
This is actually not a PD since the screening/inclusion presumably was decided before it was decided to withhold ICU-care. This will happen now and then in a trial like this. It happened in TTM1 and 2 and if you scrutinize the K-M curves they are part of the initial “drop” in survival. So please capture as much data as possible and the patient will remain in the ITT population for all analyses.
However, in a trial like this when it is not urgent to start the interventions it is reasonable to give a few minutes of observation and also consideration before screening and inclusion. Some patients on the margin will distinguish themselves as ineligible within the first half hour or so. That said, it is a generalizable population we are looking for, so rather include than exclude. And information that emerges downstream from the decision to randomize will never be considered PDs.
The aim is to start the interventions as soon as possible. If the interventions can be commenced where the patient was randomised such as Emergency Department, Angio or Cath Lab, otherwise the interventions can wait until the patient is admitted to ICU.
For unconscious patient who develop core temperature > 37.8°C within 72 h of being randomized to standard temperature management without device and for other clinical indications (anuric, acidic, hyperkalaemic etc) requires continuous renal replacement therapy (CRRT), the temperature goal should be as for other non-cardiac arrest ICU-patients (commonly CRRT with extracorporeal temperature management aimed at normothermia). If there is a refractory fever despite CRRT the temperature goal is to the discretion of the physician.
Yes, but this method of cooling should not be used routinely in place of a device. Instead, ice packs should only be used if the body temperature is sufficiently high that it would be of clinical concern outside the context of post cardiac arrest care.
Assess if the patient is possibly/likely ready for extubation within 1-2 hours and if the treating clinician therefore wishes to maintain no/light sedation. If this is the case and the patient is not tolerating the cooling device, the use of the device can be halted. If extubation does not occur within 1-2 hours restart the device and administer the level of sedation required for comfort, assess RASS regularly but aim to avoid deep sedation.
No, pain should be treated as per routine practice and the patient can receive opioids if pain is adequately assessed and detected. Opiate infusions are OK if low doses are used and they are titrated to correspond to patient´s needs.
The sedative medication is according to clinical routine in each unit.
Whenever possible the sedation should be kept minimal, but if clinically indicated, sedation can be increased temporarily.
No, this is perfectly acceptable and belongs to the nature of the condition.
Whenever possible the sedation should be kept minimal, but if clinically indicated, sedation can be increased temporarily.
If the patient has seizures and other forms of antiepileptic treatments are ineffective drugs such as propofol and benzos can be used as per the treating clinician. This will be recorded in the eCRF.
Assess if the patient is possibly/likely ready for extubation within 1-2 hours and if the treating clinician therefore wishes to maintain no/light sedation. If this is the case and the patient is not tolerating the cooling device, the use of the device can be halted. If extubation does not occur within 1-2 hours restart the device and administer the level of sedation required for comfort, assess RASS regularly but aim to avoid deep sedation.
Sedation can be used in the minimal sedation group if there is a clinical indication for it as defined in the study protocol. The reason for this must be documented- if there is no documentation or record this will be classed as a protocol deviation. The need for deep sedation should be reassessed every 4-6 hours and if possible the use of sedation should be minimized as soon as appropriate.
This patient should not be withdrawn from the study. We suggest changing to another sedative.
No, sedation is to be kept constantly deep until the end of the 36-hour period.
In general if the patient randomized to deep sedation continuous sedation should be started targeting a RASS of -4 to -5. Sedation holidays are not indicated before 36 hours from randomization. However if a participant is enrolled into the deep sedation arm and is found to be profoundly comatose without sedation, and their RASS is -4 to -5, then supplemental sedation is NOT required while their RASS is -4 to -5.
First check the volume status and cardiac function. When optimized, you may try another sedative medication. If the problem remains and the noradrenaline dose is at a very high level (approaching 1 microgram/kg/min) deemed unsafe by the treating clinician, the MAP target can be reduced at increments of 5mmHg.
The MAP intervention stops when the patient is extubated or at 72 hours whichever occurs first. If the patient is extubated but then need to be reintubated before 72 hours then the allocated MAP target should be used. When the intervention stops the MAP target will be up to the treating clinician.
If possible the MAP target should be reassessed every 4-6 hours and if the situarion allows (decreasing need of a vasopressor) then the allocated MAP target should be reintated.
We do not know this for sure and it may vary between patients. In the COMACARE and NEUROPROTECT trial there were patients who received up to 1 microgram/kg/min in order to achieve the higher MAP. There was no clear indication that these patients had more severe side-effect or a worse outcome. Nonetheless if the noradrenaline dose is high the patients should be assessed on a case by case basis.
Assess patient clinically and consider all correctable factors such as hypovolemia, systolic dysfunction etc. If clinically indicated, the MAP target can be decreased in increments of 5 mmHg. Document in medical notes the reason why MAP target can not be achieved- if there is no documentation or record this will be classed as a protocol deviation. Reassess the MAP target every 4-6 hours and if possible, increase the MAP target.
The ERC/ESICM Guidelines (https://pubmed.ncbi.nlm.nih.gov/33773827/) recommend targeting a MAP of higher than 65 mmHg. The American Heart Association and the Neurocritical Care Society target a MAP of higher than 80 mmHg (https://pubmed.ncbi.nlm.nih.gov/38040992/) unless the patient has invasive brain oxygen monitoring. Therefore there are currently no clear scientific consensus on how to manage these patients.
With an IABP the patient will have a pulse wave created by the heart and the pulse wave related to the inflation and deflation of the balloon. The IABP device will calculate a MAP which is a mean of the both the patients own beat and the one created by the IABP device. For MAP CARE aim to target a mean MAP of > 65 mmHg in the low MAP group and a mean MAP of > 85 mmHg in the high MAP group.
Aim to maintain the MAP target according to the randomization group of either >65 mmHg or >85 mmHg.
Prognostication for hypoxic brain injury should proceed according ESICM/ERC Guidelines. Indeed the WLST should not be applied before 72 hours. In rare cases WLST can be considered due to other reasons (family request, identification of terminal disease) before 72 hours. However this should be seen as a protocol violation and this must be documented. If the patient develops "brain death" before 72 hours this should not be seen as WLST or a protocol violation.
Protocol violations are reported through the eCRF.
This is actually not a PD since the screening/inclusion presumably was decided before it was decided to withhold ICU-care. This will happen now and then in a trial like this. It happened in TTM1 and 2 and if you scrutinize the K-M curves they are part of the initial “drop” in survival. So please capture as much data as possible and the patient will remain in the ITT population for all analyses.
However, in a trial like this when it is not urgent to start the interventions it is reasonable to give a few minutes of observation and also consideration before screening and inclusion. Some patients on the margin will distinguish themselves as ineligible within the first half hour or so. That said, it is a generalizable population we are looking for, so rather include than exclude. And information that emerges downstream from the decision to randomize will never be considered PDs.