Target Temperature Management After Cardiac Arrest (TTM)
Primary Purpose
Out-of-hospital Cardiac Arrest
Status
Completed
Phase
Not Applicable
Locations
International
Study Type
Interventional
Intervention
Target temperature 36°C
Target Temperature 33°C
Sponsored by
About this trial
This is an interventional treatment trial for Out-of-hospital Cardiac Arrest focused on measuring Induced hypothermia, Mild induced hypothermia, Therapeutic hypothermia, Cardiac arrest, Out-of-hospital cardiac arrest, Mortality, Neurological function, Randomised clinical trial
Eligibility Criteria
Inclusion Criteria:
- Age ≥ 18 years old
- Out-of-hospital cardiac arrest (OHCA) of presumed cardiac cause
- Return of spontaneous circulation (ROSC)
- Unconsciousness (Glasgow Coma Score < 8) (patients not able to obey verbal commands)after sustained ROSC
Exclusion Criteria:
- In-hospital cardiac arrest
- OHCA of presumed non-cardiac cause, e.g. after trauma or dissection/rupture of major artery OR Cardiac arrest caused by initial hypoxia (i.e. drowning, suffocation, hanging).
- Known bleeding diathesis (medically induced coagulopathy (e.g warfarin, clopidogrel) does not exclude the patient).
- Suspected or confirmed acute intracranial bleeding
- Suspected or confirmed acute stroke
- Unwitnessed asystole
- Known limitations in therapy and Do Not Resuscitate-order
- Known disease making 180 days survival unlikely
- Known pre-arrest CPC 3 or 4
- Temperature < 30°C on admission
- > 4 hours (240 minutes) from ROSC to screening
Systolic blood pressure < 80 mm Hg in spite of fluid loading/vasopressor and/or inotropic medication/intra aortic balloon pump#
- If the systolic blood pressure (SBP) is recovering during the inclusion window (220 minutes) the patient can be included.
Sites / Locations
- Liverpool Hospital
- North Shore Hospital
- St George Hospital
- General University Hospital
- Copenhagen University Hospital, Rigshospitalet
- San Martino Hospital
- Santa Maria degli Angeli Hospital
- Ospedale Universitario di Cattinaria
- Centre Hospitalier de Luxembourg
- Academisch Medisch Centrum, AMC
- Onze Lieve Vrouwe Gasthuis
- Rijnstate Hospital
- Leeuwarden Hospital
- Haukeland University Hospital
- Oslo University Hospital, Rikshospitalet
- Sahlgrenska University Hospital, Östra
- Sahlgrenska University Hospital
- Helsingborgs Hospital
- Karlstad Central Hospital
- Kungälv Hospital
- Linköping University Hospital
- Skåne University Hospital
- Skåne University Hospital
- Vrinnevi Hospital
- Norra Älvsborgs Läns Sjukhus
- Örebro University Hospital
- University Hospital of Geneva
- Kantonspital St Gallen
- Royal Bournemouth Hospital
- University Hospital of Wales
- Guy's and St Thomas NHS Trust
- St Georges' Hospital
- Royal Berkshire NHS Foundation Trust
Arms of the Study
Arm 1
Arm 2
Arm Type
Experimental
Active Comparator
Arm Label
Target Temperature 33°C
Target Temperature 36°C
Arm Description
Outcomes
Primary Outcome Measures
All-cause mortality
Secondary Outcome Measures
Composite outcome of all-cause mortality and poor neurological function (CPC 3 and 4) and composite outcome of all-cause mortality and poor neurological function (modified Rankin Scale 4 and 5)
Bleeding
Neurological function
Cerebral Performance Category, Modified Rankin Scale
Pneumonia
Electrolyte disorders
Hyperglycaemia > 10 mmol/l
Hypoglycemia < 3mmol/l
Cardiac arrhythmia
The need for renal replacement therapy
Landmark all-cause mortality
Cerebral Performance Category (CPC)
CPC 1,2,3,4,5
Modified Rankin Scale (mRS)
mRS 1,2,3,4,5,6
Full Information
NCT ID
NCT01020916
First Posted
November 25, 2009
Last Updated
July 8, 2013
Sponsor
Niklas Nielsen
Collaborators
Scandinavian Critical Care Trials Group, Copenhagen Trial Unit, Center for Clinical Intervention Research, Lund University, The George Institute for Global Health, Australia
1. Study Identification
Unique Protocol Identification Number
NCT01020916
Brief Title
Target Temperature Management After Cardiac Arrest
Acronym
TTM
Official Title
Target Temperature Management 33°C Versus 36°C After Out-of-hospital Cardiac Arrest, a Randomised, Parallel Groups, Assessor Blinded Clinical Trial
Study Type
Interventional
2. Study Status
Record Verification Date
July 2013
Overall Recruitment Status
Completed
Study Start Date
November 2010 (undefined)
Primary Completion Date
July 2013 (Actual)
Study Completion Date
July 2013 (Actual)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor-Investigator
Name of the Sponsor
Niklas Nielsen
Collaborators
Scandinavian Critical Care Trials Group, Copenhagen Trial Unit, Center for Clinical Intervention Research, Lund University, The George Institute for Global Health, Australia
4. Oversight
Data Monitoring Committee
Yes
5. Study Description
Brief Summary
Experimental studies and previous clinical trials suggest an improvement in mortality and neurological function with hypothermia after cardiac arrest. However, the accrued evidence is inconclusive and associated with risks of systematic error, design error and random error. Elevated body temperature after cardiac arrest is associated with a worse outcome. Previous trials did not treat elevated body temperature in the control groups. The optimal target temperature for post-resuscitation care is not known. The primary purpose with the TTM-trial is to evaluate if there are differences in all-cause mortality, neurological function and adverse events between a target temperature management at 33°C and 36°C for 24 hours following return of spontaneous circulation after cardiac arrest.
Detailed Description
Detailed statistical analysis plan for the Target Temperature Management after Out-of-hospital Cardiac Arrest trial
Introduction The Target temperature management after out-of-hospital cardiac arrest, a randomised, parallel-group, assessor-blinded clinical trial (the TTM-trial) is the largest trial to date in post-cardiac arrest treatment and in temperature management in the intensive care setting.
To prevent outcome reporting bias and data driven analysis results, the International Conference on Harmonisation of Good Clinical Practice and others have recommended that clinical trials should be analysed according to a pre-specified plan [1]. Leading experts in the critical care community have advocated that this should not only be a recommendation but rather a prerequisite [2]. Here we describe the statistical analysis plan that has been finalised while data collection in the TTM-trial still is on going, and to which all data analyses in the main publication of the TTM-trial results will adhere. The steering group of the TTM-trial unanimously approved the statistical analysis plan December 3rd 2012, patient recruitment at 950 patients was completed January 10th 2013, and the final follow-up is predicted to occur in the beginning of July 2013, after which the database will be locked and then analysed.
Trial overview The TTM-trial is a multicentre, multinational, outcome assessor-blinded, parallel group, randomised clinical trial comparing two strict target temperature regimens of 33°C and 36°C in adult patients, who have sustained return of spontaneous circulation and are unconscious after out-of-hospital cardiac arrest, when admitted to hospital. The study background, design, and rationale have previously been published [3, 4]. The TTM-trial protocol (current version 3.3) has been available online on www.ttm-trial.org since the start of the trial. The trial is registered at clinicaltrials.gov NCT01020916 and is endorsed by the European Clinical Research Infrastructure Network and the Scandinavian Critical Care Trials Group.
Objective The primary aim of the TTM-trial is to compare the effects of two strict target temperature protocols for the first 36 hours of hospital stay after resuscitation from out-of-hospital cardiac arrest (4 hours for achieving the target temperature, 24 hours of maintenance of target temperature, and 8 hours of rewarming). The null hypothesis is that there is no difference in survival until the end of trial (180 days from randomisation of the last patient) with a target temperature of 33°C compared to 36°C. To demonstrate or reject a Hazard Ratio difference of 20% between the groups, equivalent to approximately one months difference in median survival time assuming proportional hazards in the groups during the observation time, a sample size of 900 patients would be necessary with a type-1 error risk of 5% and a type-2 error risk of 10%. To allow for patients lost-to-follow up the target population is set to 950 patients.
Stratification and design variables The only stratification variable used is trial site (hospital). Pre-defined design variables allowing for an adjusted analysis of the primary outcome, and pre-defined subgroup analyses are: age, gender, first presenting cardiac rhythm (shockable or non-shockable), duration of cardiac arrest, and presence of shock at admission.
Definition of the efficacy variables The outcomes are defined as primary, secondary and exploratory (tertiary in the trial protocol). Only primary and secondary outcomes will be analysed for the first published report of the TTM-trial due to the complexity of the exploratory outcomes, and thus a need for separate publications.
Primary outcome The primary outcome is survival until end of trial, which will be 180 days from randomisation of the last patient.
Secondary outcomes including adverse events The main secondary outcomes are the composite outcomes of
poor neurological function defined as Cerebral Performance Category (CPC) 3 or 4, or death (CPC 5); and
poor neurological function defined as modified Rankin Scale (mRS) 4 or 5, or death (mRS 6)
evaluated at 180 days (+/- 14 days) from randomisation.
The number of study participants in each category of CPC and mRS will be reported separately.
The following adverse events are included in the secondary outcomes: bleeding, pneumonia, electrolyte disorders, hyperglycemia, hypoglycaemia, cardiac arrhythmia, myoclonic or tonic-clonic seizures, renal replacement therapy. Definitions for the adverse events have been described earlier [4].
Other secondary outcomes are Cerebral Performance Category at intensive care unit and hospital discharge, and best Cerebral Performance Category during entire trial period.
Exploratory outcomes Neurological function at 180 days defined with CPC, mRS, Informant Questionnaire on Cognitive Decline in the Elderly (IQCODE), Mini mental state exam (MMSE) and two simple questions: 1a. In the last two weeks, did you require help from another person for your every day activities? (If yes: 1b. Is this a new situation following the heart arrest?), and 2. Do you feel you have made a complete mental recovery after your heart arrest? [4].
Quality of life defined with Short-Form 36.
6. Data points Baseline variables
Sex
Age
Comorbidities*
Chronic heart failure (NYHA 3 or worse)
Previous acute myocardial infarction
Ischaemic heart disease
Previous cardiac arrhythmia
Previous cardiac arrest
Arterial hypertension
Previous transient ischaemic attack or stroke
Epilepsy
Diabetes mellitus
Asthma or chronic obstructive pulmonary disease
Chronic hemo- or peritoneal dialysis
Hepatic cirrhosis
Haematological malignancy
Other malignancy
Acquired immune deficiency syndrome
Alcoholism
Intravenous drug abuse
Other immunodeficiency
Pre-morbid Cerebral Performance Category (CPC)
Previous percutaneous coronary intervention
Previous coronary bypass grafting
Previous valvular surgery
Implantable cardioverter-defibrillator and or pacemaker
Age
Pre-hospital variables
Location of cardiac arrest
Bystander witnessed arrest
Bystander cardiopulmonary resuscitation (CPR)
First monitored rhythm at arrival of emergency medical service
Use of active compression-decompression device
Time from cardiac arrest to start of basic life support
Time from arrest to start of advanced life support
Time from arrest to return of spontaneous circulation
Data on admission
First measured temperature (tympanic)
Glasgow Coma Scale (combined score)
pH
Lactate
Shock on admission
Acute ST-elevation infarction or novel left bundle branch block
A comorbidity will only be reported if the frequency is above or equal to 5% in any of the intervention groups. Pre-morbid CPC will be reported regardless of the frequency.
Intervention period variables Core temperature primarily measured in the urinary bladder will be reported per hour during the 36 hours of the intervention period.
Neurological prognostication and withdrawal of care Number and proportion of patients still comatose at 72 hours after the end of the intervention period that underwent neurological prognostication by a blinded physician. Number of patients, who did not survive until neurological prognostication and their presumed cause of death, including limitations in care and reasons for that. Number of patients with electroencephalogram, somatosensory evoked potentials, magnetic resonance imaging, computed tomography of the head.
Concomitant cardiological treatments Number of patients receiving coronary angiography, percutaneous coronary intervention and coronary bypass grafting, divided in three time groups (immediately after admission, during intervention or when sedated in the intensive care unit, and after regaining consciousness. Number of patients receiving intra aortic balloon pump, other mechanical assist device, temporary pacemaker, permanent pacemaker and implantable cardioverter-defibrillator.
Other descriptive variables Number of days in intensive care unit and days on mechanical ventilation during the index ICU-admission and days in hospital within the index admission will be reported.
7. General analysis principles
Analyses will be conducted according to the modified intention-to-treat principle [5] if not otherwise stated.
All tests of significance will be two-sided with a maximal type-1 error risk of 5%
The primary analyses of primary and secondary outcomes will be those of the modified intention-to-treat population adjusted for the protocol specified stratification variable [6] and if necessary using data sets generated using multiple imputations (see below). An unadjusted analysis and an analysis adjusting for both stratification and predefined design variables will be carried out as sensitivity analyses. Other analyses may also be done using e.g. a slightly different population. If the results of these analyses are not consistent with the primary analyses this will be discussed. Nevertheless, the conclusions of the study will still be those based on the primary analyses.
The tests for interaction between the intervention and each design variable used to identify subgroups are exploratory.
Risks will be reported as hazard ratios or risk ratios with 95% confidence interval (CI) or with limits as stated under point 6.
If there is data missingness for a specified primary or secondary outcome of less than 5% we will perform a complete case analysis without imputing missing values. If there is a missingness of more than 5% we will perform Little's test. If the test indicates that the complete case data set is a random sample we will continue without imputing missing values and analyse the complete cases. If Little's test indicates that the data set of complete cases is not a random sample of the total data set we will report the point estimates and their 95% confidence limits applying a worst/best scenario imputation for the missing values. If the worst/best case analyses allow for the same conclusion we will not perform multiple imputation. However, if the worst/best case imputation provides different conclusions, multiple imputation will be performed, creating 10 imputed data sets under the assumption of missingness at random. The result of the trial will be the pooled intervention effect and 95% CI of the analyses of the data sets after multiple imputation.
Primarily the observed P-values of the primary and five secondary outcomes will be presented. However, multiplicity, a possibly reason for spurious statistically significant P-values, may be a problem when the result of several outcomes are presented. We therefore want to present a supplemental analysis being the result with P-values adjusted for multiplicity according to the fall-back procedure [7]. The P-values adjusted for multiplicity will be presented and discussed in relation to the unadjusted P-values. This adjustment may be needed to control the overall probability of a type 1 error (rejection of a null hypothesis that is actually true) and keep the family wise error rate below 0.05 as required by most regulatory agencies. This will be done by specifying the weights of the hypotheses assigned to them according to their importance. The sequence in which the hypotheses will be tested and their individual weights (in parentheses) will be: the primary outcome (0.50), first secondary outcome (0.25), second secondary outcome (0.0625), third secondary outcome (0.0625), fourth secondary outcome (0.0625), and fifth secondary outcome (0.0625). The multiplicity problem is further illuminated in the Discussion section.
8. Statistical analyses Trial profile Flow of study participants will displayed in a CONSORT diagram as shown in Box 1 [8]. Number of screened patients who fulfilled study inclusion criteria and the number included in the primary and secondary analyses as well as all reasons for exclusions in primary and secondary analyses will be reported.
Primary outcome Frequencies and percentages per group, as well as hazard ratios with 95% CI will be reported. The primary outcome will be analysed using Cox-regression with adjusting variables indicated below. The proportional hazard assumption across treatment groups will be checked by testing if there is an interaction between intervention and time and by plotting cumulative hazard functions for intervention groups.
The first analysis of the primary outcome, adjusted for the stratification variable, will be on the patients that met the inclusion criteria and did not meet the exclusion criteria at time of randomisation. Patients who did not meet inclusion criteria and did not receive the intervention (temperature management) and was erroneously randomised will be excluded according to the modified intention to treat principle.
The second analysis on the primary outcome will be on patients that met the inclusion criteria and did not meet the exclusion criteria and did not have any major protocol violations (per-protocol analysis).
The third analysis on the primary outcome will be an analysis adjusted for both the stratification variable and the design variables.
The above analyses will be repeated with sites grouped as a variable indicating whether the patient has been allocated by the 2 sites having allocated most patients or one of the other sites (which would be approximately ¼ of the trial population).
Secondary outcomes including adverse events Frequencies and percentages per group, as well as risk ratios with 95% CI will be reported. A standard Chi2-test will be used to assess the effect of treatment on binary and categorical outcomes. For the adjusted primary analyses logistic regression analysis will be used. Wilcoxon-Mann-Whitney's test will be used for continuous outcomes. There will only be reported significance testing on the composite outcomes mortality and poor neurological outcome versus survival with good neurological outcome; not on the individual sub-scores of CPC and mRS. For adverse events there will be a Chi2-test on having one or more adverse events versus having no adverse events. If there is a significant difference between treatment groups in occurrence of adverse events we will try to delineate which of the events that drive this difference. However we acknowledge the low power for performing analyses in this case.
Characteristics of patients with baseline comparisons Description of baseline characteristics listed above will be presented by treatment group. Discrete variables will be summarized by frequencies and percentages. Percentages will be calculated according to the number of patients where data are available. Where values are missing, the actual denominator will be stated.
Continuous variables will be summarised using standard measures of central tendency and dispersion, either using mean +/- standard deviation for data with normal distribution or median and inter quartile range for non-normally distributed data.
Intervention period variables The mean values of the actual measured temperature in the two intervention groups will be displayed in a graph with mean, +/- 2 standard deviations.
Neurological prognostication and withdrawal of care, concomitant cardiological treatments and other descriptive variables
Description of baseline characteristics listed above will be presented by treatment group without significance testing. Discrete variables will be summarized by frequencies and percentages. Percentages will be calculated according to the number of patients where data are available. Where values are missing, the actual denominator will be stated.
Continuous variables will be summarised using standard measures of central tendency and dispersion, either using mean +/- standard deviation for data with normal distribution or median and inter quartile range for non-normally distributed data.
9. Outline of figures and tables Figure 1 will be a CONSORT flow chart as specified above. Figure 2 will be a temperature graph for the two groups with hour 0 to 36 on the x-axis and mean temperature with +/- 2 standard deviations on the y-axis.
Figure 3 will be a Kaplan-Meier plot of survival in the two groups during the trial period (32 months).
Figure 4 will be a Forest plot of intervention effects stratified for the design variables: age dichotomised around the median, gender, duration of cardiac arrest dichotomised around the median, initial cardiac rhythm shockable or non-shockable, and presence or absence of cardiogenic shock at admission to hospital.
All tables will report variable according to randomisation groups:
Table 1 and 2 will report background variables. Table 3 will report intensive care unit and hospital stay variables. Table 4 will report adverse events. Table 5 will report 180-day outcomes for survival/mortality and neurological function with CPC and mRS.
10. Discussion With this statistical analysis plan we present the different analyses in the main publication of the TTM-trial to avoid risks of outcome reporting bias and data driven results. Of the pre-specified outcomes in the trial we choose to report only primary and secondary in the main publication, because of the complexity of the detailed neurological outcomes and quality of life that constitutes the exploratory outcomes, requiring separate publications.
We would like to emphasise that the main secondary outcome being the composite outcome of poor neurological function and mortality at 180 days after cardiac arrest will be of great importance in a situation of a neutral outcome in the primary outcome, when interpreting the results and deriving clinical implications from the TTM-trial. As survival is an outcome with low risk of bias, not prone to competing risks, and earlier trials and registry data indicate a lower sample size needed to show the same risk reduction when the composite outcome of mortality and poor neurological function is used (compared to mortality/survival), this was the fundament for the order of the outcomes. The composite outcome of poor neurological function and mortality will hopefully benefit by an increased power with respect to the possibility of finding or rejecting a significant signal when the trial is powered for survival, which would require a larger sample size.
Comments on the multiplicity problem
There are one primary and 5 secondary outcomes to be assessed:
Primary outcome: survival
Secondary outcomes
Neurological (CPC): binary quantity
Neurological (mRS): binary quantity
Adverse event: binary quantity
Cerebral performance category measured at specified point in time: binary quantity
Best cerebral performance during specified period: binary quantity Thus there are six significance tests. These have to be adjusted for multiplicity to control the probability of a type-1-error (rejection of a null hypothesis that is true). One way to diminish this risk would be to deal with the six outcomes as one group using a data driven adjustment of the P-values. The most powerful procedure based on the raw P-values is probably that of Hommel [7].
An alternative (the fixed sequence procedure) would be to specify the sequence of the hypotheses testing in advance. (Primary outcome, first secondary outcome, second secondary outcome, - - -, fifth secondary outcome.) In this latter case no multiplicity adjustment will be needed. Then each test will be done at the 0.05 level of significance in the specified order. However, as soon as a test is non-significant the remaining null hypotheses will be accepted without test.
For instance if the primary outcome and the first secondary outcome are significant at the 0.05 level and the second secondary outcome (neurological function measured with mRS) is insignificant, the null hypotheses corresponding to the secondary outcomes 3, 4 and 5 will be accepted without test.
A third approach is the so-called fall back procedure where the fixed hypothesis testing sequence is also used. However, if a test is insignificant, the procedure does not stop but the next hypothesis is tested at a reduced level of significance. This procedure also allows one to weight the hypotheses according to their importance and likelihood of being rejected.
Hommel's procedure is sensitive to the P-values of the last three tests while the fall back procedure is not. Since the first and second of the secondary outcomes probably will produce similar P-values it appears logical to place most of the weights on the primary and the first secondary outcome.
Based on these considerations the analyses in the TTM-trial will be presented with unadjusted P-values as well as adjusted for multiplicity using the fall back procedure.
11. Conclusion To conclude this article describes the principle for how the TTM-trial will be analysed and presented in the first and main publication. With this we minimise the risk for data driven results and outcome reporting bias.
References
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Nielsen N, Wetterslev J, al-Subaie N, Andersson B, Bro-Jeppesen J, Bishop G, Brunetti I, Cranshaw J, Cronberg T, Edqvist K, Erlinge D, Gasche Y, Glover G, Hassager C, Horn J, Hovdenes J, Johnsson J, Kjaergaard J, Kuiper M, Langørgen J, Macken L, Martinell L, Martner P, Pellis T, Pelosi P, Petersen P, Persson S, Rundgren M, Saxena M, Svensson R, Stammet P, Thorén A, Undén J, Walden A, Wallskog J, Wanscher M, Wise MP, Wyon N, Aneman A, Friberg H: Target temperature management after out-of-hospital cardiac arrest-a randomized, parallel-group, assessor-blinded clinical trial-rationale and design. Am Heart J. 2012, 163:541-548.
Fergusson D, Aaron SD, Guyatt G, Hérbert P: Post-randomisation exclusions: the intention-to-treat principle and excluding patients from analysis. BMJ 2002, 325:652-654
Kahan BC, Morris TP: Reporting and analysis of trials using stratified randomisation in leading medical journals: review and reanalysis. BMJ 2012, 344:e5840
Dmitrienko A, Tamhane AC, Bretz F (editors): Multiple testing Problems in Pharmaceutical Statistics. New York: CRC Press/Chapman & Hall; 2010
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6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Out-of-hospital Cardiac Arrest
Keywords
Induced hypothermia, Mild induced hypothermia, Therapeutic hypothermia, Cardiac arrest, Out-of-hospital cardiac arrest, Mortality, Neurological function, Randomised clinical trial
7. Study Design
Primary Purpose
Treatment
Study Phase
Not Applicable
Interventional Study Model
Parallel Assignment
Masking
ParticipantInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
950 (Anticipated)
8. Arms, Groups, and Interventions
Arm Title
Target Temperature 33°C
Arm Type
Experimental
Arm Title
Target Temperature 36°C
Arm Type
Active Comparator
Intervention Type
Procedure
Intervention Name(s)
Target temperature 36°C
Intervention Description
In hospital target temperature management to achieve a core body temperature of 36°C for 24 hours
Intervention Type
Procedure
Intervention Name(s)
Target Temperature 33°C
Intervention Description
In hospital target temperature management to achieve a core body temperature of 33°C for 24 hours
Primary Outcome Measure Information:
Title
All-cause mortality
Time Frame
Maximum follow-up with a minimum of 180 days
Secondary Outcome Measure Information:
Title
Composite outcome of all-cause mortality and poor neurological function (CPC 3 and 4) and composite outcome of all-cause mortality and poor neurological function (modified Rankin Scale 4 and 5)
Time Frame
180 days
Title
Bleeding
Time Frame
During day 1-7 of intensive care treatment
Title
Neurological function
Description
Cerebral Performance Category, Modified Rankin Scale
Time Frame
180 days
Title
Pneumonia
Time Frame
During day 1-7 of intensive care treatment
Title
Electrolyte disorders
Time Frame
During day 1-7 of intensive care treatment
Title
Hyperglycaemia > 10 mmol/l
Time Frame
During day 1-7 of intensive care treatment
Title
Hypoglycemia < 3mmol/l
Time Frame
During day 1-7 of intensive care treatment
Title
Cardiac arrhythmia
Time Frame
During day 1-7 of intensive care treatment
Title
The need for renal replacement therapy
Time Frame
During day 1-7 of intensive care treatment
Title
Landmark all-cause mortality
Time Frame
180 days
Title
Cerebral Performance Category (CPC)
Description
CPC 1,2,3,4,5
Time Frame
180 days
Title
Modified Rankin Scale (mRS)
Description
mRS 1,2,3,4,5,6
Time Frame
180 days
Other Pre-specified Outcome Measures:
Title
Quality of life
Description
SF-36
Time Frame
180 days
Title
Neurological function including "Complete neurological recovery"*
Description
Mini mental state exam (MMSE), Informant Questionnaire on Cognitive Decline in the Elderly (IQCODE) and two questions*
*Survivors with complete recovery defined by: MMSE ≥27 (or ≥19 on MMSE-Adult Lifestyle Functioning Interview by telephone interview), modified IQCODE ≤78, answer "No" to question 1a or "No" to question 1b, answer "Yes" to question 2.
1a. "In the last 2 weeks, did you require help from another person for your every day activities?" (If yes, 1b. "Is this a new situation following the heart arrest?") and 2. "Do you feel that you have made a complete mental recovery after your heart arrest?
Time Frame
180 days
Title
Neurological function at hospital discharge and best neurological function during follow up period
Description
CPC at hospital discharge and best CPC during the first 180 days after cardiac arrest
Time Frame
Hospital discharge and 1-180 days
10. Eligibility
Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
Age ≥ 18 years old
Out-of-hospital cardiac arrest (OHCA) of presumed cardiac cause
Return of spontaneous circulation (ROSC)
Unconsciousness (Glasgow Coma Score < 8) (patients not able to obey verbal commands)after sustained ROSC
Exclusion Criteria:
In-hospital cardiac arrest
OHCA of presumed non-cardiac cause, e.g. after trauma or dissection/rupture of major artery OR Cardiac arrest caused by initial hypoxia (i.e. drowning, suffocation, hanging).
Known bleeding diathesis (medically induced coagulopathy (e.g warfarin, clopidogrel) does not exclude the patient).
Suspected or confirmed acute intracranial bleeding
Suspected or confirmed acute stroke
Unwitnessed asystole
Known limitations in therapy and Do Not Resuscitate-order
Known disease making 180 days survival unlikely
Known pre-arrest CPC 3 or 4
Temperature < 30°C on admission
> 4 hours (240 minutes) from ROSC to screening
Systolic blood pressure < 80 mm Hg in spite of fluid loading/vasopressor and/or inotropic medication/intra aortic balloon pump#
If the systolic blood pressure (SBP) is recovering during the inclusion window (220 minutes) the patient can be included.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Niklas Nielsen, MD, PhD
Organizational Affiliation
Helsingborgs lasarett, Region Skåne, Sweden
Official's Role
Study Chair
First Name & Middle Initial & Last Name & Degree
Janneke Horn, MD, PhD
Organizational Affiliation
Academisch Medisch Centrum, Amsterdam, the Netherlands
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Hans Friberg, MD, PhD
Organizational Affiliation
Lund University Hospital, Lund, Sweden
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Tobias Cronberg, MD, PhD
Organizational Affiliation
Lund University Hospital, Lund, Sweden
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Michael Wanscher, MD, PhD
Organizational Affiliation
Copenhagen University Hospital, Copenhagen, Denmark
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Christian Hassager, MD, DMSc
Organizational Affiliation
Copenhagen University Hospital, Copenhagen, Denmark
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Jesper Kjaergaard, MD, PhD
Organizational Affiliation
Copenhagen University Hospital, Copenhagen, Denmark
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Jan Hovdenes, MD, PhD
Organizational Affiliation
Oslo University Hospital, Oslo, Norway
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Pascal Stammet, MD
Organizational Affiliation
Centre Hospitalier du Luxembourg
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Yvan Gasche, MD, PhD
Organizational Affiliation
Geneva University Hospital, Geneva, Switzerland
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Thomas Pellis, MD, PhD
Organizational Affiliation
Santa Maria degli Angeli Hospital, Pordenone, Italy
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Matt Wise, MD, DPhil
Organizational Affiliation
University Hospital of Wales, Cardiff, UK
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Anders Åneman, MD, PhD
Organizational Affiliation
Liverpool Hospital, Sydney, Australia
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Jørn Wetterslev, MD, PhD
Organizational Affiliation
Copenhagen Trial Unit, Copenhagen University Hospital, Copenhagen, Denmark
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
Michael Kuiper, MD, PhD
Organizational Affiliation
Leeuwarden Hospital, Leeuwarden, the Netherlands
Official's Role
Principal Investigator
First Name & Middle Initial & Last Name & Degree
David Erlinge, MD, PhD
Organizational Affiliation
Lund University Hospital, Lund, Sweden
Official's Role
Principal Investigator
Facility Information:
Facility Name
Liverpool Hospital
City
Sydney
Country
Australia
Facility Name
North Shore Hospital
City
Sydney
Country
Australia
Facility Name
St George Hospital
City
Sydney
Country
Australia
Facility Name
General University Hospital
City
Prague
Country
Czech Republic
Facility Name
Copenhagen University Hospital, Rigshospitalet
City
Copenhagen
ZIP/Postal Code
DK2100
Country
Denmark
Facility Name
San Martino Hospital
City
Genova
Country
Italy
Facility Name
Santa Maria degli Angeli Hospital
City
Pordenone
Country
Italy
Facility Name
Ospedale Universitario di Cattinaria
City
Trieste
Country
Italy
Facility Name
Centre Hospitalier de Luxembourg
City
Luxembourg
Country
Luxembourg
Facility Name
Academisch Medisch Centrum, AMC
City
Amsterdam
Country
Netherlands
Facility Name
Onze Lieve Vrouwe Gasthuis
City
Amsterdam
Country
Netherlands
Facility Name
Rijnstate Hospital
City
Arnhem
Country
Netherlands
Facility Name
Leeuwarden Hospital
City
Leeuwarden
Country
Netherlands
Facility Name
Haukeland University Hospital
City
Bergen
Country
Norway
Facility Name
Oslo University Hospital, Rikshospitalet
City
Oslo
Country
Norway
Facility Name
Sahlgrenska University Hospital, Östra
City
Gothenburg
Country
Sweden
Facility Name
Sahlgrenska University Hospital
City
Gothenburg
Country
Sweden
Facility Name
Helsingborgs Hospital
City
Helsingborg
ZIP/Postal Code
251 87
Country
Sweden
Facility Name
Karlstad Central Hospital
City
Karlstad
Country
Sweden
Facility Name
Kungälv Hospital
City
Kungälv
Country
Sweden
Facility Name
Linköping University Hospital
City
Linköping
Country
Sweden
Facility Name
Skåne University Hospital
City
Lund
Country
Sweden
Facility Name
Skåne University Hospital
City
Malmö
Country
Sweden
Facility Name
Vrinnevi Hospital
City
Norrköping
Country
Sweden
Facility Name
Norra Älvsborgs Läns Sjukhus
City
Trollhättan/Vänersborg
Country
Sweden
Facility Name
Örebro University Hospital
City
Örebro
Country
Sweden
Facility Name
University Hospital of Geneva
City
Geneva
Country
Switzerland
Facility Name
Kantonspital St Gallen
City
St Gallen
Country
Switzerland
Facility Name
Royal Bournemouth Hospital
City
Bournemouth
Country
United Kingdom
Facility Name
University Hospital of Wales
City
Cardiff
Country
United Kingdom
Facility Name
Guy's and St Thomas NHS Trust
City
London
Country
United Kingdom
Facility Name
St Georges' Hospital
City
London
Country
United Kingdom
Facility Name
Royal Berkshire NHS Foundation Trust
City
Reading
Country
United Kingdom
12. IPD Sharing Statement
Citations:
PubMed Identifier
20591514
Citation
Nielsen N, Friberg H, Gluud C, Herlitz J, Wetterslev J. Hypothermia after cardiac arrest should be further evaluated--a systematic review of randomised trials with meta-analysis and trial sequential analysis. Int J Cardiol. 2011 Sep 15;151(3):333-41. doi: 10.1016/j.ijcard.2010.06.008. Epub 2010 Jul 1.
Results Reference
background
PubMed Identifier
19549271
Citation
Nielsen N, Hovdenes J, Nilsson F, Rubertsson S, Stammet P, Sunde K, Valsson F, Wanscher M, Friberg H; Hypothermia Network. Outcome, timing and adverse events in therapeutic hypothermia after out-of-hospital cardiac arrest. Acta Anaesthesiol Scand. 2009 Aug;53(7):926-34. doi: 10.1111/j.1399-6576.2009.02021.x. Epub 2009 Jun 22.
Results Reference
background
PubMed Identifier
35470143
Citation
Grindegard L, Cronberg T, Backman S, Blennow K, Dankiewicz J, Friberg H, Hassager C, Horn J, Kjaer TW, Kjaergaard J, Kuiper M, Mattsson-Carlgren N, Nielsen N, van Rootselaar AF, Rossetti AO, Stammet P, Ullen S, Zetterberg H, Westhall E, Moseby-Knappe M. Association Between EEG Patterns and Serum Neurofilament Light After Cardiac Arrest: A Post Hoc Analysis of the TTM Trial. Neurology. 2022 Jun 14;98(24):e2487-e2498. doi: 10.1212/WNL.0000000000200335. Epub 2022 Apr 25.
Results Reference
derived
PubMed Identifier
34415801
Citation
Grand J, Kjaergaard J, Hassager C, Moller JE, Bro-Jeppesen J. Comparing Doppler Echocardiography and Thermodilution for Cardiac Output Measurements in a Contemporary Cohort of Comatose Cardiac Arrest Patients Undergoing Targeted Temperature Management. Ther Hypothermia Temp Manag. 2022 Sep;12(3):159-167. doi: 10.1089/ther.2021.0008. Epub 2021 Aug 20.
Results Reference
derived
PubMed Identifier
34271131
Citation
Thomsen JH, Hassager C, Erlinge D, Nielsen N, Lindholm MG, Bro-Jeppesen J, Grand J, Pehrson S, Graff C, Kober LV, Kjaergaard J. Repolarization and ventricular arrhythmia during targeted temperature management post cardiac arrest. Resuscitation. 2021 Sep;166:74-82. doi: 10.1016/j.resuscitation.2021.07.004. Epub 2021 Jul 14.
Results Reference
derived
PubMed Identifier
32345356
Citation
During J, Annborn M, Cronberg T, Dankiewicz J, Devaux Y, Hassager C, Horn J, Kjaergaard J, Kuiper M, Nikoukhah HR, Stammet P, Unden J, Wanscher MJ, Wise M, Friberg H, Nielsen N. Copeptin as a marker of outcome after cardiac arrest: a sub-study of the TTM trial. Crit Care. 2020 Apr 28;24(1):185. doi: 10.1186/s13054-020-02904-8.
Results Reference
derived
PubMed Identifier
31068215
Citation
Rundgren M, Ullen S, Morgan MPG, Glover G, Cranshaw J, Al-Subaie N, Walden A, Joannidis M, Ostermann M, Dankiewicz J, Nielsen N, Wise MP. Renal function after out-of-hospital cardiac arrest; the influence of temperature management and coronary angiography, a post hoc study of the target temperature management trial. Crit Care. 2019 May 8;23(1):163. doi: 10.1186/s13054-019-2390-0.
Results Reference
derived
PubMed Identifier
28629472
Citation
Stammet P, Dankiewicz J, Nielsen N, Fays F, Collignon O, Hassager C, Wanscher M, Unden J, Wetterslev J, Pellis T, Aneman A, Hovdenes J, Wise MP, Gilson G, Erlinge D, Horn J, Cronberg T, Kuiper M, Kjaergaard J, Gasche Y, Devaux Y, Friberg H; Target Temperature Management after Out-of-Hospital Cardiac Arrest (TTM) trial investigators. Protein S100 as outcome predictor after out-of-hospital cardiac arrest and targeted temperature management at 33 degrees C and 36 degrees C. Crit Care. 2017 Jun 20;21(1):153. doi: 10.1186/s13054-017-1729-7.
Results Reference
derived
PubMed Identifier
28099439
Citation
Wiberg S, Hassager C, Stammet P, Winther-Jensen M, Thomsen JH, Erlinge D, Wanscher M, Nielsen N, Pellis T, Aneman A, Friberg H, Hovdenes J, Horn J, Wetterslev J, Bro-Jeppesen J, Wise MP, Kuiper M, Cronberg T, Gasche Y, Devaux Y, Kjaergaard J. Single versus Serial Measurements of Neuron-Specific Enolase and Prediction of Poor Neurological Outcome in Persistently Unconscious Patients after Out-Of-Hospital Cardiac Arrest - A TTM-Trial Substudy. PLoS One. 2017 Jan 18;12(1):e0168894. doi: 10.1371/journal.pone.0168894. eCollection 2017.
Results Reference
derived
PubMed Identifier
27887653
Citation
Glover GW, Thomas RM, Vamvakas G, Al-Subaie N, Cranshaw J, Walden A, Wise MP, Ostermann M, Thomas-Jones E, Cronberg T, Erlinge D, Gasche Y, Hassager C, Horn J, Kjaergaard J, Kuiper M, Pellis T, Stammet P, Wanscher M, Wetterslev J, Friberg H, Nielsen N. Intravascular versus surface cooling for targeted temperature management after out-of-hospital cardiac arrest - an analysis of the TTM trial data. Crit Care. 2016 Nov 26;20(1):381. doi: 10.1186/s13054-016-1552-6.
Results Reference
derived
PubMed Identifier
27667713
Citation
Gilje P, Koul S, Thomsen JH, Devaux Y, Friberg H, Kuiper M, Horn J, Nielsen N, Pellis T, Stammet P, Wise MP, Kjaergaard J, Hassager C, Erlinge D; TTM study group. High-sensitivity troponin-T as a prognostic marker after out-of-hospital cardiac arrest - A targeted temperature management (TTM) trial substudy. Resuscitation. 2016 Oct;107:156-61. doi: 10.1016/j.resuscitation.2016.06.024.
Results Reference
derived
PubMed Identifier
27523954
Citation
Bro-Jeppesen J, Johansson PI, Hassager C, Wanscher M, Ostrowski SR, Bjerre M, Kjaergaard J. Endothelial activation/injury and associations with severity of post-cardiac arrest syndrome and mortality after out-of-hospital cardiac arrest. Resuscitation. 2016 Oct;107:71-9. doi: 10.1016/j.resuscitation.2016.08.006. Epub 2016 Aug 11.
Results Reference
derived
PubMed Identifier
27438111
Citation
Devaux Y, Dankiewicz J, Salgado-Somoza A, Stammet P, Collignon O, Gilje P, Gidlof O, Zhang L, Vausort M, Hassager C, Wise MP, Kuiper M, Friberg H, Cronberg T, Erlinge D, Nielsen N; for Target Temperature Management After Cardiac Arrest Trial Investigators. Association of Circulating MicroRNA-124-3p Levels With Outcomes After Out-of-Hospital Cardiac Arrest: A Substudy of a Randomized Clinical Trial. JAMA Cardiol. 2016 Jun 1;1(3):305-13. doi: 10.1001/jamacardio.2016.0480.
Results Reference
derived
PubMed Identifier
26525271
Citation
Bro-Jeppesen J, Kjaergaard J, Stammet P, Wise MP, Hovdenes J, Aneman A, Horn J, Devaux Y, Erlinge D, Gasche Y, Wanscher M, Cronberg T, Friberg H, Wetterslev J, Pellis T, Kuiper M, Nielsen N, Hassager C; TTM-Trial Investigators. Predictive value of interleukin-6 in post-cardiac arrest patients treated with targeted temperature management at 33 degrees C or 36 degrees C. Resuscitation. 2016 Jan;98:1-8. doi: 10.1016/j.resuscitation.2015.10.009. Epub 2015 Oct 23.
Results Reference
derived
PubMed Identifier
26433116
Citation
Lilja G, Nilsson G, Nielsen N, Friberg H, Hassager C, Koopmans M, Kuiper M, Martini A, Mellinghoff J, Pelosi P, Wanscher M, Wise MP, Ostman I, Cronberg T. Anxiety and depression among out-of-hospital cardiac arrest survivors. Resuscitation. 2015 Dec;97:68-75. doi: 10.1016/j.resuscitation.2015.09.389. Epub 2015 Oct 9.
Results Reference
derived
PubMed Identifier
25975474
Citation
Stammet P, Collignon O, Hassager C, Wise MP, Hovdenes J, Aneman A, Horn J, Devaux Y, Erlinge D, Kjaergaard J, Gasche Y, Wanscher M, Cronberg T, Friberg H, Wetterslev J, Pellis T, Kuiper M, Gilson G, Nielsen N; TTM-Trial Investigators. Neuron-Specific Enolase as a Predictor of Death or Poor Neurological Outcome After Out-of-Hospital Cardiac Arrest and Targeted Temperature Management at 33 degrees C and 36 degrees C. J Am Coll Cardiol. 2015 May 19;65(19):2104-14. doi: 10.1016/j.jacc.2015.03.538. Erratum In: J Am Coll Cardiol. 2015 Aug 25;66(8):983. J Am Coll Cardiol. 2017 Apr 25;69(16):2104.
Results Reference
derived
PubMed Identifier
25886727
Citation
Devaux Y, Stammet P, Friberg H, Hassager C, Kuiper MA, Wise MP, Nielsen N; Biomarker subcommittee of TTM trial (Target Temperature Management After Cardiac Arrest, NCT01020916). MicroRNAs: new biomarkers and therapeutic targets after cardiac arrest? Crit Care. 2015 Feb 11;19(1):54. doi: 10.1186/s13054-015-0767-2.
Results Reference
derived
PubMed Identifier
25844993
Citation
Cronberg T, Lilja G, Horn J, Kjaergaard J, Wise MP, Pellis T, Hovdenes J, Gasche Y, Aneman A, Stammet P, Erlinge D, Friberg H, Hassager C, Kuiper M, Wanscher M, Bosch F, Cranshaw J, Kleger GR, Persson S, Unden J, Walden A, Winkel P, Wetterslev J, Nielsen N; TTM Trial Investigators. Neurologic Function and Health-Related Quality of Life in Patients Following Targeted Temperature Management at 33 degrees C vs 36 degrees C After Out-of-Hospital Cardiac Arrest: A Randomized Clinical Trial. JAMA Neurol. 2015 Jun;72(6):634-41. doi: 10.1001/jamaneurol.2015.0169.
Results Reference
derived
PubMed Identifier
25789868
Citation
Johansson PI, Bro-Jeppesen J, Kjaergaard J, Wanscher M, Hassager C, Ostrowski SR. Sympathoadrenal activation and endothelial damage are inter correlated and predict increased mortality in patients resuscitated after out-of-hospital cardiac arrest. a post Hoc sub-study of patients from the TTM-trial. PLoS One. 2015 Mar 19;10(3):e0120914. doi: 10.1371/journal.pone.0120914. eCollection 2015.
Results Reference
derived
PubMed Identifier
25756419
Citation
Bro-Jeppesen J, Kjaergaard J, Wanscher M, Nielsen N, Friberg H, Bjerre M, Hassager C. Systemic Inflammatory Response and Potential Prognostic Implications After Out-of-Hospital Cardiac Arrest: A Substudy of the Target Temperature Management Trial. Crit Care Med. 2015 Jun;43(6):1223-32. doi: 10.1097/CCM.0000000000000937.
Results Reference
derived
PubMed Identifier
25365723
Citation
Bro-Jeppesen J, Annborn M, Hassager C, Wise MP, Pelosi P, Nielsen N, Erlinge D, Wanscher M, Friberg H, Kjaergaard J; TTM Investigators. Hemodynamics and vasopressor support during targeted temperature management at 33 degrees C Versus 36 degrees C after out-of-hospital cardiac arrest: a post hoc study of the target temperature management trial*. Crit Care Med. 2015 Feb;43(2):318-27. doi: 10.1097/CCM.0000000000000691.
Results Reference
derived
PubMed Identifier
25270900
Citation
Bro-Jeppesen J, Hassager C, Wanscher M, Ostergaard M, Nielsen N, Erlinge D, Friberg H, Kober L, Kjaergaard J. Targeted temperature management at 33 degrees C versus 36 degrees C and impact on systemic vascular resistance and myocardial function after out-of-hospital cardiac arrest: a sub-study of the Target Temperature Management Trial. Circ Cardiovasc Interv. 2014 Oct;7(5):663-72. doi: 10.1161/CIRCINTERVENTIONS.114.001556. Epub 2014 Sep 30.
Results Reference
derived
PubMed Identifier
25267568
Citation
Westhall E, Rosen I, Rossetti AO, van Rootselaar AF, Kjaer TW, Horn J, Ullen S, Friberg H, Nielsen N, Cronberg T. Electroencephalography (EEG) for neurological prognostication after cardiac arrest and targeted temperature management; rationale and study design. BMC Neurol. 2014 Aug 16;14:159. doi: 10.1186/s12883-014-0159-2.
Results Reference
derived
PubMed Identifier
25078879
Citation
Beurskens CJ, Horn J, de Boer AM, Schultz MJ, van Leeuwen EM, Vroom MB, Juffermans NP. Cardiac arrest patients have an impaired immune response, which is not influenced by induced hypothermia. Crit Care. 2014 Jul 30;18(4):R162. doi: 10.1186/cc14002.
Results Reference
derived
PubMed Identifier
24237006
Citation
Nielsen N, Wetterslev J, Cronberg T, Erlinge D, Gasche Y, Hassager C, Horn J, Hovdenes J, Kjaergaard J, Kuiper M, Pellis T, Stammet P, Wanscher M, Wise MP, Aneman A, Al-Subaie N, Boesgaard S, Bro-Jeppesen J, Brunetti I, Bugge JF, Hingston CD, Juffermans NP, Koopmans M, Kober L, Langorgen J, Lilja G, Moller JE, Rundgren M, Rylander C, Smid O, Werer C, Winkel P, Friberg H; TTM Trial Investigators. Targeted temperature management at 33 degrees C versus 36 degrees C after cardiac arrest. N Engl J Med. 2013 Dec 5;369(23):2197-206. doi: 10.1056/NEJMoa1310519. Epub 2013 Nov 17.
Results Reference
derived
PubMed Identifier
24188226
Citation
Ferreira Da Silva IR, Frontera JA. Targeted temperature management in survivors of cardiac arrest. Cardiol Clin. 2013 Nov;31(4):637-55, ix. doi: 10.1016/j.ccl.2013.07.010.
Results Reference
derived
PubMed Identifier
24044764
Citation
Nielsen N, Winkel P, Cronberg T, Erlinge D, Friberg H, Gasche Y, Hassager C, Horn J, Hovdenes J, Kjaergaard J, Kuiper M, Pellis T, Stammet P, Wanscher M, Wise MP, Aneman A, Wetterslev J. Detailed statistical analysis plan for the target temperature management after out-of-hospital cardiac arrest trial. Trials. 2013 Sep 17;14:300. doi: 10.1186/1745-6215-14-300.
Results Reference
derived
PubMed Identifier
23688929
Citation
Cronberg T, Nielsen N. Fever after therapeutic hypothermia - does rebound pyrexia matter? Resuscitation. 2013 Aug;84(8):1011-2. doi: 10.1016/j.resuscitation.2013.05.006. Epub 2013 May 17. No abstract available.
Results Reference
derived
PubMed Identifier
23499577
Citation
Nielsen N, Friberg H. Can we conclude anything yet about the effect of hypothermia for patients arresting in-hospital? Resuscitation. 2013 May;84(5):535-6. doi: 10.1016/j.resuscitation.2013.02.009. Epub 2013 Mar 13. No abstract available.
Results Reference
derived
PubMed Identifier
22520518
Citation
Nielsen N, Wetterslev J, al-Subaie N, Andersson B, Bro-Jeppesen J, Bishop G, Brunetti I, Cranshaw J, Cronberg T, Edqvist K, Erlinge D, Gasche Y, Glover G, Hassager C, Horn J, Hovdenes J, Johnsson J, Kjaergaard J, Kuiper M, Langorgen J, Macken L, Martinell L, Martner P, Pellis T, Pelosi P, Petersen P, Persson S, Rundgren M, Saxena M, Svensson R, Stammet P, Thoren A, Unden J, Walden A, Wallskog J, Wanscher M, Wise MP, Wyon N, Aneman A, Friberg H. Target Temperature Management after out-of-hospital cardiac arrest--a randomized, parallel-group, assessor-blinded clinical trial--rationale and design. Am Heart J. 2012 Apr;163(4):541-8. doi: 10.1016/j.ahj.2012.01.013.
Results Reference
derived
PubMed Identifier
21458906
Citation
Nielsen N, Friberg H. Insights from the evidence evaluation process--do we have the answers for therapeutic hypothermia? Resuscitation. 2011 May;82(5):501-2. doi: 10.1016/j.resuscitation.2011.02.041. Epub 2011 Mar 10. No abstract available.
Results Reference
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Learn more about this trial
Target Temperature Management After Cardiac Arrest
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