Permissive versus restrictive temperature thresholds in critically ill children with fever and infection: a multicentre randomized clinical pilot trial

The FEVER pilot trial was a pragmatic, open, parallel-group multicentre RCT in infants and children accepted for emergency admission to one of four participating paediatric intensive care units (PICUs). The units represented a geographical spread across England and a variety of common configurations for UK PICUs (general or combined general and cardiac units in general academic medical centres or within stand-alone children’s hospitals).

The trial was coordinated and sponsored by the Intensive Care National Audit & Research Centre (ICNARC) Clinical Trials Unit (CTU).

Health Research Authority and research ethics committee (17/LO/1139) approval was obtained. The protocol was registered (ISRCTN16022198) prior to recruitment of the first patient. A trial steering committee, with a majority of independent members, and an independent data monitoring and ethics committee were convened to oversee the trial on behalf of the funder.

The full trial protocol is available in the supplementary appendix.

Inclusion criteria were as follows: > 28 days and < 16 years of age, unplanned admission to a participating PICU, fever ≥ 37.5 °C in the first 48 h following contact with the paediatric retrieval service or PICU, new requirement for mechanical ventilation and the treating clinician presumed the cause of the fever was an infective process. Mechanical ventilation was considered to include invasive ventilation, non-invasive ventilation and high-flow humidified oxygen.

Exclusion criteria were as follows: acute encephalopathy, including convulsive status epilepticus; post-cardiopulmonary bypass or known/suspected cardiomyopathy/myocarditis; rhabdomyolysis (a serum creatine kinase concentration at least 10 times the upper limit of normal); malignant hyperthermia, neuroleptic malignant syndrome or drug-induced hyperthermia; receiving palliative care or death perceived as imminent; and previous recruitment to the FEVER pilot trial. These exclusions reflected populations that clinical staff were not in equipoise about the risks and benefits of fever control [16].

Potentially eligible infants and children were screened against the eligibility criteria by the paediatric retrieval team or PICU staff. Randomization took place as soon as eligibility was confirmed, including during transport. Participants were randomly allocated (1:1) via a secure web-based system.

Participants received antipyretic interventions at a temperature threshold of either 37.5 °C in the restrictive group or 39.5 °C in the permissive group, until they were no longer receiving any mechanical ventilator support. The 37.5 °C value was selected to represent usual care following extensive feasibility work demonstrating that approximately 60% of emergency PICU admissions receive antipyretic interventions at or below this temperature. The site and technique for temperature measurement and all other care were at the discretion of the treating clinical teams.

A secure, study-specific, web portal was developed containing an electronic case report form. These data were then combined with routinely collected UK Paediatric Intensive Care Audit Network (PICANet; www.​picanet.​org.​uk) data.

We employed a “research without prior consent” (RWPC) approach as is appropriate in emergency situations where it is not practically possible to obtain consent prospectively and any delay in commencing treatment allocation may be detrimental [17]. A member of the research team approached the parents/legal representatives as soon as it was possible and appropriate after randomization to discuss the trial, to provide a participant information sheet (supplementary material) and seek consent for continued inclusion in the trial. If the participant was discharged or died prior to their parents/legal representatives being approached, then they were approached by an appropriate team member at a later point either in person or by post with an option to opt out from the trial [17].

The following outcome measures were used to assess the specified objectives. Objective 1: the proportion of eligible patients recruited (target 50%). Objective 2: the number of eligible patients recruited per month (estimated at 6.25 per site per month). Objective 3: staff and parents’ views on the intervention thresholds and trial procedures and the proportion of parents/legal representatives refusing or withdrawing consent. Objective 4: the difference in maximum temperature between the restrictive and permissive groups in the first 48 h, proportion of 6-h time periods in which antipyretic interventions were used as directed in the trial protocol. Objectives 5: occurrence of serious adverse events in each group. Objective 6: characteristics and completeness of potential primary endpoints for a definitive trial including length of PICU stay, length of invasive ventilation, ventilator-free days at day 30, duration of organ support and PICU mortality.

As a pilot RCT, no formal sample size calculations were performed, instead a sample size of 100 was determined to be adequate to estimate candidate patient-centred outcome measures to a necessary degree of precision and to test the trial processes. It was anticipated that this sample size would give 90% power to demonstrate a separation of 0.5 °C in mean peak temperature between temperature groups allowing for 16% withdrawal. 0.5 °C was chosen on the basis of the HEAT trial [9] and our own observational work of the impact of antipyretics on fever in PICU [18].

All analyses were carried out by the randomized group. Continuous variables were summarized as mean (standard deviation) and median (interquartile range) whilst categorical variables were summarized as number (percentage). Analyses were conducted using Stata/SE Version 14.0 (StataCorp LP, College Station, US).

To explore key stakeholder perspectives on trial acceptability, approach to consent and participant information, we invited parents to complete a questionnaire following the FEVER pilot trial recruitment discussion and/or participate in an interview approximately a month after leaving hospital. We also invited staff involved in the pilot trial to take part in a focus group at the end of recruitment. Interviews and focus groups were audio recorded after consent was obtained. Questionnaire and topic guides were developed using previous research [19, 20] and pre-pilot trial qualitative study findings (reported separately) that explored staff and parent perspective on trial design. Qualitative data analysis was thematic and iterative [21]. Interviews continued until no new themes were identified (data saturation) [22]. Quantitative data were analysed using simple descriptive statistics. Data synthesis was pragmatic and drew on the constant comparative approach [23].

Between 25 September and 19 December, 2017, 154 patients were screened and met the inclusion criteria (Fig. 1). Of these, 15 (9.7%) were excluded. Of those eligible, 26 (18.7%) were missed and 12 (8.6%) were not randomized due to local clinical decisions. One hundred one (72.7%) children were randomized into the pilot trial. One patient was removed as a duplicate. 72.5% (100/138) of eligible patients were appropriately randomized. The recruitment rate of 11.1 (95% confidence interval 9.0–13.5) patients per site per month was almost double that estimated from PICANet data.

Of the 100 patients, five (four in the permissive group) were unable to be approached for consent. These included children in the care of social workers and parents who were felt to have insufficient understanding of trial information. Consent to continue in the trial was refused in eight out of the remaining 95 patients. Of these, seven had been allocated to the permissive treatment group. In addition, parents/legal representatives of seven patients (five permissive and two restrictive) refused consent to be treated according to the trial protocol, but consented for ongoing data collection, and a further three patients treated in the permissive group withdrew consent so as to allow an antipyretic intervention to be given. One hospital had seven out of their 10 patients randomized to the permissive group have consent either refused or withdrawn, which accounted for almost half (46.7%) of the total number across all four sites.

Therefore, 87 out of the 100 correctly randomized patients were included in the analysis of objectives 4–6.

A total of 60 parents (49 mothers, 11 fathers) of 57/100 (57%) randomized children took part in a questionnaire (41/60, 68%), an interview (12/60, 20%) or both (7/60, 12%). Eight (six questionnaire and two interview participants) had refused consent for their child’s involvement in the FEVER pilot trial. Forty-eight staff (9/48, 19% medical; 39/48, 81% nursing) participated in one of five focus groups held at the four participating PICUs. All parents interviewed described their support for the trial (see Table 1), which was viewed “an interesting trial” (P30, interview, mother, restrictive), involving a perceived low risk, non-invasive intervention, of which parents were familiar. Many of the questionnaire respondents (32/42, 76%) cited helping other children in the future as their main reason for providing consent, whilst during interviews parents emphasized how they trusted doctors to prioritize their child’s well-being whilst they were in the FEVER pilot trial. Reasons the eight parents provided for declining consent included concerns about their child being in pain or discomfort, increased physiological workload, pre-existing medical condition, risk of epileptic seizures due to family history and incapacity to make an informed decision (see Table 1). Two parents withdrew consent due to concerns about their child being in pain or discomfort during deintensification. Importantly, parents who declined consent to use data already collected, or for their child to continue in the FEVER pilot trial, also described their support for the proposed definitive RCT.

The majority (42/48, 89% of questionnaire respondents) indicated they were satisfied with the FEVER consent process. Four (4/48, 9%) indicated that they were not satisfied with the use of RWPC, although this had not influenced their decision to agree or decline consent. Those who took part in an interview also described how the consent discussion had been well timed and how staff had “clearly explained” (P74, interview, mother, permissive) the trial. Participant information materials were viewed as being “clear and understandable” (P80, interview, mother, permissive).

Overall, the two treatment groups were well matched at baseline (Table 2). Bronchiolitis was the most common diagnosis. Baseline temperature was the same in both groups; however, a greater proportion of patients in the restrictive temperature arm received pre-randomization paracetamol (Additional file 1: Table S3).

Over the first 48 h following randomization, patients in the restrictive group had a mean peak temperature of 38.4 °C (95% confidence interval 38.2–38.6 °C) compared with 38.8 °C (38.6–39.1 °C) in the permissive group. This resulted in a between-group difference in mean peak temperature over the first 48 h of 0.5 °C (0.2–0.8 °C). The separation of around 0.5 °C was maintained up to 84 h following randomization (Fig. 2). More patients received antipyretic interventions in the restrictive group (98%, 48/49) than in the permissive group (50%, 19/38) in the 48 h following randomization (Additional file 1: Table S6).

Protocol deviations were assessed for each patient during each 6-h time period from randomization until death or discharge from PICU. Either not receiving an antipyretic intervention when above the allocated threshold or receiving such an intervention without reaching the threshold were considered deviations. (These definitions are likely to represent overestimates of non-adherence because of interventions in previous, or immediately following, time periods not being considered). Deviations were reported in 39 of 628 6-h time periods (6.2%) in the permissive group and 60 out of 810 time periods (7.4%) in the restrictive group. Overall, 39% of patients in the permissive group and 55% in the restrictive group experienced at least one 6-h period containing a protocol deviation (Table 2).

The embedded qualitative work investigated staff attitudes that may have contributed to non-adherence. Staff had mixed views about the acceptability of the permissive temperature threshold. Focus group participants who did not find the permissive threshold acceptable described how they were unhappy about not administering paracetamol when they thought a child was uncomfortable or in pain. This led to protocol deviations. Suggestions were made to revise the proposed FEVER pilot trial protocol to exclude patients not on mechanical ventilation (e.g. high-flow nasal oxygen) or those close to being extubated when sedation is being weaned.

Overall, the majority of staff described their support for a definitive trial, often stating this trial was needed to provide an answer to an important research question.

“You’re never gonna know the answer if you don’t do a trial” (Staff 04, focus group 2).

There were no reported serious adverse events. Three adverse events in total were reported. One seizure was reported in the permissive group (an expected adverse event) that was deemed unlikely to be related to the trial intervention. There were two adverse events in the restrictive group: one seizure that was deemed unrelated and one rhabdomyolysis (an expected adverse event) (Additional file 1: Table S4).

For the 86 patients consenting to data collection and having left hospital at the time of data lock, all candidate outcome data were complete on consented patients. Characteristics of the outcome measures are outlined in Table 3, as expected for a pilot trial of this size, there were no significant differences between the groups in any of the outcomes.