Adelson 2005 HYPO 2.
| Methods | Randomised controlled trial, parallel group | |
| Participants |
Total number of participants: 27 Baseline characteristics: Therapeutic cooling Age: mean (SD) 7.17 (± 6.64) years Type of injury (closed/open): closed GCS on admission: mean (SD) 6.42 (± 1.2) No cooling Age: mean (SD) 5.6 (± 5.23) years Type of injury (closed/open): closed GCS on admission: mean (SD) 6.23 (± 1.2) Inclusion criteria: children 0 to 214 months of age, with non‐penetrating head injury, GCS ≤ 8, within 24 hours of admission Exclusion criteria: normal initial CT scan, penetrating brain injury, brain death on admission to emergency department, failure to obtain informed consent 24 hours from admission, uncorrectable coagulopathy (PT/PTT > 16/40 seconds), hypotensive episode for > 5 minutes defined as SBP < fifth percentile for age Country: USA Setting: hospital (single centre) |
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| Interventions |
Therapeutic cooling Number of participants: 14 Method of cooling: surface cooling using a hypothermia/heating blanket. Sedation and paralysis induced to prevent shivering Target temperature: 32 to 33 °C Time of cooling: < 6 hours Duration of cooling: 48 hours Rewarming details: after 48 hours, passive warming, 1 °C every 3 to 4 hours until 36.5 °C reached. Initiation of warming not stopped due to intracranial hypotension but slowed at times due to elevations in ICP Site of temperature measurement: rectal No cooling Number of participants: 13 Method of temperature management: participants were passively warmed if their initial presenting core temperature was < 36 °C Target temperature: 36.5 to 37.5 °C |
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| Outcomes | Outcomes measured in study: mortality, ventricular arrhythmias, delayed intracranial haemorrhage, intraabdominal/thoracic bleeding, coagulopathy infection (pneumonia), GOS, Infant Health Questionnaire, Vineland Adaptive Behaviour scale, ICP, other secondary clinical outcomes | |
| Notes |
Funding/declarations of interest: National Institute of Health grant, General Clinical Research Centre at Children's Hospital of Pittsburgh grant Study dates: August 2001 to December 2003 Note: HYPO 2 was a single‐centre trial set up later due to recruitment issues in HYPO 1, but running in parallel to HYPO 1 with a different inclusion criteria. All other methods and outcomes were the same as HYPO 1 |
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| Risk of bias | ||
| Bias | Authors' judgement | Support for judgement |
| Random sequence generation (selection bias) | Unclear risk | Described as randomised and stratification done by age of child at time of injury. No additional details |
| Allocation concealment (selection bias) | Unclear risk | Insufficient details provided |
| Blinding of participants and personnel (performance bias): mortality | Low risk | Not possible to blind personnel; unlikely to influence performance |
| Blinding of participants and personnel (performance bias): GOS | Unclear risk | Not possible to blind personnel; unclear if this would influence performance |
| Blinding of participants and personnel (performance bias): pneumonia | Unclear risk | Not possible to blind personnel; unclear if this would influence performance |
| Blinding of outcome assessment (detection bias): mortality; pneumonia | Low risk | Lack of blinding unlikely to influence outcome assessment |
| Blinding of outcome assessment (detection bias): GOS | Low risk | Neurocognitive tests (GOS) were performed by the site neuropsychologist or technician who were blinded to the therapeutic intervention |
| Incomplete outcome data (attrition bias) All outcomes | Low risk | Low for mortality and pneumonia. Small loss of follow‐up at 3 and 6 months for GOS data, not reported by treatment groups. |
| Selective reporting (reporting bias) | Unclear risk | Clinical trials registration or pre‐published protocol not reported. Insufficient information to make judgement |
| Other bias | Low risk | No other sources of bias identified |