Efficacy and Mechanism Evaluation

Intravenous immunoglobulin treatment for encephalitis in children aged 6 months to 16 years: the IgNiTE RCT

  • Type:
    Extended Research Article
  • Authors:
    Mildred A IroMildred A Iro on ORCiD,
    Manish SadaranganiManish Sadarangani on ORCiD,
    Michael AbsoudMichael Absoud on ORCiD,
    Liberty CantrellLiberty Cantrell on ORCiD,
    Wui K ChongWui K Chong on ORCiD,
    Christopher ClarkChristopher Clark on ORCiD,
    Ava EastonAva Easton on ORCiD,
    Victoria GrayVictoria Gray on ORCiD,
    Matilda HillMatilda Hill on ORCiD,
    Rachel KneenRachel Kneen on ORCiD,
    Ming LimMing Lim on ORCiD,
    Xinxue LiuXinxue Liu on ORCiD,
    Mike PikeMike Pike on ORCiD,
    Tom SolomonTom Solomon on ORCiD,
    Angela VincentAngela Vincent on ORCiD,
    Louise WillisLouise Willis on ORCiD,
    Ly-Mee YuLy-Mee Yu on ORCiD,
    Andrew J PollardAndrew J Pollard on ORCiD,
    IgNiTE Study Team
    Detailed Author information

    Mildred A Iro1,*, Manish Sadarangani1,2,3,4, Michael Absoud5,6, Liberty Cantrell1, Wui K Chong7, Christopher Clark8, Ava Easton9,10, Victoria Gray11, Matilda Hill1, Rachel Kneen12,13, Ming Lim5,6, Xinxue Liu1, Mike Pike14, Tom Solomon12,15,16, Angela Vincent17, Louise Willis1, Ly-Mee Yu18, Andrew J Pollard1,2, IgNiTE Study Team

    • 1 Oxford Vaccine Group, Department of Paediatrics, University of Oxford and NIHR Biomedical Research Centre, Oxford University Hospitals NHS Foundation Trust, Oxford, UK
    • 2 Department of Paediatrics, Oxford University Hospitals NHS Foundation Trust, Oxford, UK
    • 3 Vaccine Evaluation Center, BC Children’s Hospital Research Institute, University of British Columbia, Vancouver, BC, Canada
    • 4 Department of Pediatrics, University of British Columbia, Vancouver, BC, Canada
    • 5 Department of Children’s Neurosciences, Evelina London Children’s Hospital at Guy’s and St Thomas’ NHS Foundation Trust, King’s Health Partners Academic Health Science Centre, London, UK
    • 6 Department of Women and Children’s Health, Faculty of Life Sciences and Medicine, King’s College London, London, UK
    • 7 Department of Radiology, Great Ormond Street Hospital for Children, London, UK
    • 8 Institute of Child Health, University College London, London, UK
    • 9 The Encephalitis Society, Malton, UK
    • 10 Department of Clinical Infection, Microbiology and Immunology, University of Liverpool, Liverpool, UK
    • 11 Psychological services (Paediatrics), Alder Hey Children’s NHS Foundation Trust, Liverpool, UK
    • 12 Institute of Infection, Veterinary and Ecological Sciences, University of Liverpool, Liverpool, UK
    • 13 Littlewoods Neuroscience Foundation, Department of Neurology, Alder Hey Children’s NHS Foundation Trust, Liverpool, UK
    • 14 Department of Paediatric Neurology, Oxford University Hospitals NHS Trust, Oxford, UK
    • 15 National Institute for Health Research Health Protection Research Unit in Emerging and Zoonotic Infections, University of Liverpool, Liverpool, UK
    • 16 Walton Centre NHS Foundation Trust, Liverpool, UK
    • 17 Nuffield Department of Clinical Neurosciences, Weatherall Institute of Molecular Medicine, University of Oxford, Oxford, UK
    • 18 Nuffield Department of Primary Care Health Sciences, University of Oxford, Oxford, UK
    • * Corresponding author email: mildred.iro@nhs.net
    • Disclosure of interests

      Full disclosure of interests: Completed ICMJE forms for all authors, including all related interests, are available in the toolkit on the NIHR Journals Library report publication page at https://doi.org/10.3310/YJWQ4299.

      Primary conflicts of interest: Mildred A Iro was a trainee member of the NIHR Efficacy and Mechanism Evaluation Funding Committee from October 2020 to October 2021. Michael Absoud has received a grant from the NIHR in the last 36 months, for research unrelated to the submitted work. Manish Sadarangani has been an investigator on projects funded by GlaxoSmithKline, Merck, Moderna, Pfizer, Sanofi-Pasteur, Seqirus, Symvivo and VBI Vaccines; all funds have been paid to his institute. Ava Easton is Chief Executive of the Encephalitis Society, which has previously received grants from CSL Behring (UK). Ming Lim has received grants from the GOSH charity, Boston Children’s Hospital Research Fund and Action Medical Research in the last 36 months, all for research unrelated to the submitted work. Ming Lim is co-chair of the European Paediatric Neurology Education and Training Board and works for an institution which holds research accounts with Roche (Switzerland), Octapharma (Switzerland) and Novartis (Switzerland). Tom Solomon is supported by the NIHR Health Protection Research Unit in Emerging and Zoonotic Infections, NIHR Programme Grant for Applied Research, NIHR Global Health Research on Brain Infections and the European Union’s Horizon 2020 research and innovation program ZikaPLAN. Tom Solomon is a consultant for the Medicines and Healthcare products Regulatory Agency (MHRA) Vaccine Benefit Risk Expert Working Group. Angela Vincent is a consultant for Aspen NewCo Inc and has received honoraria from UCB and Alexion. Ly-Mee Yu had membership with NIHR HTA Efficient Study Designs from November 2015 to July 2016. Andrew J Pollard is chair of the Department of Health and Social Care’s Joint committee on Vaccines and Immunisation (JCVI) and was a member of WHO’s SAGE until 1 January 2022. Oxford University has entered a partnership with AstraZenenca on COVID-19 vaccines, but Andrew J Pollard does not participate in the JCVI COVID-19 committee.

  • Funding:
    Efficacy and Mechanism Evaluation programme
  • Journal:
    Efficacy and Mechanism Evaluation
  • Issue:
    Volume: 11, Issue: 6
  • Published:
  • Citation:
    Iro MA, Sadarangani M, Absoud M, Cantrell L, Chong WK, et al. Intravenous immunoglobulin treatment for encephalitis in children aged 6 months to 16 years: the IgNiTE RCT. Efficacy Mech Eval 2024;11(06). https://doi.org/10.3310/YJWQ4299
  • DOI:
    https://doi.org/10.3310/YJWQ4299
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Background

There are data suggesting that intravenous immunoglobulin treatment has some benefit for certain forms of encephalitis but robust evidence from large randomised controlled trials in children with all-cause encephalitis is lacking.

Objective

To evaluate whether intravenous immunoglobulin treatment improves neurological outcomes in childhood encephalitis when given early in the illness.

Design

Phase 3b, investigator-initiated, randomised, double-blind, placebo-controlled trial of intravenous immunoglobulin for the treatment of encephalitis in children.

Setting

Twenty-one NHS Hospitals in the UK.

Participants

Children aged 6 months to 16 years with a diagnosis of acute or sub-acute encephalitis.

Intervention

Two doses (1 g/kg/dose) of either intravenous immunoglobulin or matching placebo, given 24–36 hours apart, in addition to standard treatment.

Main outcome measure

Participants were followed up for 12 months (+/– 4 weeks) after randomisation. The primary outcome measure was a ‘good recovery’ defined as a score of ≤ 2 on the Paediatric Glasgow Outcome Score Extended at 12 months after randomisation.

Secondary outcomes

The secondary outcomes were clinical, neurological, neuroimaging and neuropsychological results, identification of the proportion of children with immune-mediated encephalitis, and intravenous immunoglobulin safety data.

Results

We planned to recruit 308 children over a 42-month period. After enrolment of 18 participants (8 male; 44%) over 21 months (from December 2015 to September 2017), funding was withdrawn due to slow recruitment and the study was terminated. Ten participants were randomised to the intravenous immunoglobulin group, and eight to the placebo group, and all 18 participants were included in the analysis. At 12 months after randomisation, 9 participants [50%; intravenous immunoglobulin n = 5 (50%), placebo n = 4 (50%)] made good recovery and 5 participants [28%; intravenous immunoglobulin n = 3 (30%), placebo n = 2 (25%)] made a poor recovery. Three participants in the placebo group (43%) experienced a total of 10 serious adverse events compared with none in the intravenous immunoglobulin group but none of the adverse events were judged to be related to the study treatment. No deaths occurred during the study period.

Conclusion

ImmunoglobuliN in the Treatment of Encephalitis (IgNiTE) was halted prematurely due to slow recruitment. Given the small sample size, the study was underpowered to evaluate the effect of intravenous immunoglobulin when compared with placebo in childhood encephalitis. The study findings, albeit from a small sample size, support existing evidence that encephalitis results in poor neurological outcomes for many children. Lessons learned from the ImmunoglobuliN in the Treatment of Encephalitis trial would be valuable for the success of future trials set up to address the efficacy of early treatment with intravenous immunoglobulin in all-cause encephalitis in children.

Study limitations and future work

The study was underpowered to evaluate the efficacy of intravenous immunoglobulin in the treatment of childhood encephalitis due to the small sample size achieved. Future trials should seek to address this important question.

Trial registration

This trial is registered as Clinical Trials.gov (NCT02308982) and ISRCTN15791925.

Funding

This award was funded by the National Institute for Health and Care Research (NIHR) Efficacy and Mechanism Evaluation (EME) programme (NIHR award ref: 12/212/15) and is published in full in Efficacy and Mechanism Evaluation; Vol. 11, No. 6. See the NIHR Funding and Awards website for further award information.

Notes

Article history

The research reported in this issue of the journal was funded by the EME programme as award number 12/212/15. The contractual start date was in January 2015. The final report began editorial review in October 2022 and was accepted for publication in July 2023. The authors have been wholly responsible for all data collection, analysis and interpretation, and for writing up their work. The EME editors and production house have tried to ensure the accuracy of the authors’ manuscript and would like to thank the reviewers for their constructive comments on the final manuscript document. However, they do not accept liability for damages or losses arising from material published in this manuscript.

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Copyright statement

Copyright © 2024 Iro et al. This work was produced by Iro et al. under the terms of a commissioning contract issued by the Secretary of State for Health and Social Care. This is an Open Access publication distributed under the terms of the Creative Commons Attribution CC BY 4.0 licence, which permits unrestricted use, distribution, reproduction and adaptation in any medium and for any purpose provided that it is properly attributed. See: https://creativecommons.org/licenses/by/4.0/. For attribution the title, original author(s), the publication source – NIHR Journals Library, and the DOI of the publication must be cited.

2024 Iro et al.

Chapter 1 Introduction

Background

Encephalitis is a rare condition that can result in serious consequences for those affected and their families. Encephalitis can result from an infection of the brain (infectious encephalitis) or from autoantibodies that affect the brain (immune‐mediated encephalitis), or both. 1 Immune‐mediated disorders, such as acute disseminated encephalomyelitis contribute to a significant proportion of cases where no infective cause is identified. 2 Nonetheless, despite routine investigations, no aetiology is found in up to approximately 40–60% of cases of encephalitis. 2,3

Irrespective of the cause, the final common pathway in the pathophysiology in encephalitis is brain inflammation, which leads to changes in neurological function. Therefore, a paradigm for intervention with the greatest presumptive benefit centres on the early attenuation of the extensive inflammation, which is the primary cause of fatality and neurological sequelae and underpins the pathogenesis of most forms of encephalitis.

Direct evidence of efficacy of intravenous immunoglobulin (IVIG) is suggested by the successful outcomes from both its therapeutic and prophylactic use in enteroviral encephalitis in the immunocompromised and in outbreaks in Southeast and East Asia. There is also evidence from case reports that seem to support the use of IVIG in other infectious causes of encephalitis, including infections with West Nile virus, coxsackie viruses and Mycoplasma pneumoniae, where its use has been associated with rapid improvement and reduced morbidity. The authors of one previous study of IVIG in children with Japanese encephalitis (JE) suggest that IVIG may be an effective treatment for JE and other flaviviral encephalitis due to its anti-inflammatory effects, immune augmentation and neutralisation of the JE virus. 4 However, the result of a Cochrane systematic review of IVIG in infective encephalitis was inconclusive due to the risk of bias and quality of evidence of the included studies. 5

Immunotherapy, often in the form of IVIG, also appears to benefit both adults and children with autoimmune encephalitis, resulting in improved outcomes. Further evidence exists to support the benefit of IVIG in various autoimmune neurological conditions that share similar underlying inflammatory mechanisms to encephalitis, including primary inflammatory myopathies, inflammatory neuropathies and multiple sclerosis. Furthermore, given its disease-modifying properties, there is theoretical evidence of benefit from IVIG treatment even in encephalitis patients who appear to have made an initial full recovery since they can still develop persisting symptoms later.

However, in clinical practice the use of IVIG in encephalitis varies. 6 In the immune-mediated forms of encephalitis, IVIG is typically used after inevitable delay (by weeks in some cases) while alternative diagnoses are being excluded, or until a definitive diagnosis is obtained. In other cases, IVIG is used as a last treatment option where clinical improvement is slow; this is usually after several days from hospital admission. Delay in diagnosis and institution of appropriate treatment in encephalitis may contribute to the high rate of morbidity and mortality, prolonged hospitalisation and associated costs from encephalitis. Given the available evidence of a possible beneficial role of IVIG, there is a strong case for the prospective assessment of the potential role of early intervention with IVIG for all children presenting with evidence of inflammatory encephalitis.

Hypothesis

Our hypothesis was that early treatment with IVIG in addition to standard care could improve neurological outcomes in children with encephalitis.

Study objectives

Primary objective

To determine whether early treatment with IVIG improves neurological outcomes at 12 months after randomisation in children with encephalitis, compared with placebo.

Secondary objectives

  • To evaluate whether IVIG is associated with improved clinical outcomes relating to the hospital admission, including duration of ventilation, length of stay on intensive care unit (ICU), and length of hospitalisation.

  • To evaluate whether early IVIG is associated with improved neurological outcomes including motor and behavioural outcomes, and quality of life.

  • To assess whether IVIG has impact on the development of epilepsy in children affected by encephalitis.

  • To evaluate the impact of IVIG on neuropsychological outcomes of patients with encephalitis.

  • To evaluate whether IVIG treatment is associated with improved neuroradiological outcomes.

  • To identify what adverse effects are experienced with IVIG treatment.

  • To evaluate what proportion of recruited children with encephalitis have an autoantibody mediated disease.

Exploratory objectives

  • To correlate neuroimaging findings with primary and secondary outcomes.

  • To correlate clinical and laboratory parameters with neurological outcomes.

  • To compare brain magnetic resonance imaging (MRI) findings with aetiological diagnosis.

  • Analysis of gene expression in whole blood before and after study treatment.

  • Identification of specific DNA sequence and structural genetic variants in patients with encephalitis.

Encephalitis

In this section, we describe the burden of encephalitis, established treatment options and the role that IVIG might have in the treatment of affected patients.

Encephalitis is a syndrome of neurological dysfunction that results from inflammation of the brain parenchyma. The worldwide annual incidence ranges from 3.5 to 7.4 per 100,000, rising to 16 per 100,000 in children, with the highest incidence in infants under 1 year of age. 7 In England, the incidence of childhood encephalitis is 4.02 per 100,000 per year. 8

Pathophysiology

The inflammation that occurs in encephalitis causes the brain parenchyma to swell leading to altered level of consciousness, and often seizures.

Impact of encephalitis

Encephalitis survivors suffer long-term sequelae and around 30–50% of patients fail to make a full recovery, experiencing impairments in concentration, behaviour, speech and memory, and seizures. 9 Affected patients also experience persisting physical, psychological, cognitive, behavioral and social impairments which can be significant. Even those children who appear to have made an initial recovery experience some degree of disability later. 10,11

Across paediatric encephalitis studies, case fatality of 2–16% has been reported,9,1217 with individual studies reporting an overall long-term morbidity of 30–60%. 11,13,14,16,1823 In a 10-year Israeli study of 46 children with all-cause encephalitis, 33% of affected children had focal motor deficit at discharge while 15% showed varying levels of cognitive impairment. 10 In the same study, half of affected children had persisting symptoms, including behavioural problems (52%), recurrent headache (22%) and problems with sleep (19%) after a mean follow-up period of 6 years. Children with encephalitis have a significantly higher prevalence of learning disability (20%) compared to the general population (10%), and even those who appear to have made full recovery demonstrate lower intelligence scores when compared with the general population. 10,24 In a prospective study of Malaysian children with JE, 13% of affected children who were of school age never returned to school due to severe physical disabilities from the illness, while 38% had marked deterioration in school performance which resulted in discontinuation of schooling. 14 In an Indian study of JE, 10% of 39 children had Parkinsonian features at discharge and about 30% had residual symptoms at 14 month follow up. 25 A meta-analysis comprising 890 children with infectious encephalitis from 15 studies showed that 10–20% of children with had abnormal behaviour, motor and cognitive impairment at follow-up 1 to 12 years later while a third of patients had developmental delay. 26

Following herpes simplex encephalitis (HSE), 40–65% of affected children develop seizures. 20 In an Australian study of 147 children followed up for a median duration of 7 years, post-encephalitic epilepsy and drug-resistant epilepsy were reported in 31 (21%) and 15 (10%) children respectively. 27

Treatments for encephalitis

Following suspicion of an encephalitis diagnosis, antibiotics and antiviral (aciclovir) treatment are usually commenced and subsequently rationalised based on microbiological results and clinical progress. Aciclovir is widely used for the treatment of confirmed herpes simplex and varicella zoster virus encephalitis. For bacterial infections causing encephalitis, an appropriate antibiotic is used, based on microbiological sensitivity testing. For autoimmune encephalitis, treatment strategies including IV methylprednisolone, plasma exchange and IVIG are commonly used.

Intravenous immunoglobulin

Intravenous immunoglobulin is a blood product made from pooled collections of human plasma collected from thousands of blood donors. The efficacy of IVIG has been demonstrated for a range of neurological conditions. 28 Licensed indications include as replacement therapy for people with primary and secondary antibody deficiency states, Kawasaki disease, haematological conditions (idiopathic immune thrombocytopenic purpura, B‐cell chronic lymphocytic leukaemia) and neurological conditions (multifocal motor neuropathy and chronic demyelinating polyneuropathy). 29 At the time of running the trial, IVIG was sometimes used off‐label for the treatment of children with encephalitis, but has since been commissioned (2021) for use in autoimmune encephalitis. 30

Dosing

The dose of IVIG for each indication varies. 31 For primary and secondary antibody deficiency states, the starting dose is between 0.4 g/kg and 0.6 g/kg of bodyweight with subsequent adjustments made based on clinical outcome. For neurological diseases, two doses of 2 g/kg of bodyweight over 5 days are typically given, 6 weeks apart. For haematological conditions, a dose of 0.8 g/kg to 1 g/kg is used.

Adverse effects

Intravenous immunoglobulin treatment is generally considered safe and well tolerated; however, adverse events (AEs) such as chills, headache, fever, vomiting, allergic reaction, nausea, arthralgia, low blood pressure and low back pain may occur. Rarely, sudden fall in blood pressure, anaphylactic shock, and thromboembolic reactions could occur. Cases of reversible aseptic meningitis and isolated cases of haemolytic anaemia have been observed as well as acute renal failure. Since IVIG is a blood product, there is the risk of transmission of infectious agents such as HIV and viral hepatitis by contaminated products. 32

How IVIG might work

Intravenous immunoglobulin has multiple actions which may operate in concert with each other. For a particular disease, there may be one predominant mechanism of action depending on the underlying disease pathogenesis. The most relevant actions of IVIG include the following:

  1. inhibition of complement binding and prevention of membrane attack complex formation3336

  2. neutralisation of certain pathogenic cytokines37,38

  3. regulation of autoantibodies or cytokines by anti‐idiotypic or anticytokine antibodies39,40

  4. blockade of Fc gamma receptors on macrophages41,42

  5. modulation of T‐cell function and antigen recognition. 4347

Additional actions include the effect of IVIG on superantigens and enhancement of remyelination. 44 Antiviral functions of IVIG and its potential to inhibit viral infection has been demonstrated in vitro. 4850

Literature

The literature review was first carried out in PubMed in 2017 and updated in August 2022 (search terms: ‘intravenous immunoglobulin’ or ‘IVIG’ and ‘encephalitis’).

Intravenous immunoglobulin in infectious encephalitis

There are reports of successful outcomes following treatment with IVIG in children with M. pneumoniae encephalitis,51,52 in immunocompromised patients with echovirus meningoencephalitis,53 and in children with JE. 54 Clinical observation following an outbreak of brainstem encephalitis in Catalonia support a beneficial role of IVIG – all but 3 of 34 children who received IVIG showed good clinical response and had no significant sequelae. 55 In a quasi-controlled Indian trial of 83 children with acute encephalitis syndrome complicated by myocarditis, Bhatt et al. demonstrated that who received IVIG treatment demonstrated a borderline significant lower rate of mortality and an improvement in ejection fraction compared with those treated with standard care alone. 56 However, a retrospective review of 35 paediatric patients with confirmed or suspected encephalitis showed similar clinical and neurological outcomes between IVIG treated versus non-treated patients. 57

Intravenous immunoglobulin in autoimmune encephalitis

The largest available evidence suggesting a positive effect of IVIG in anti-N-methyl-D-aspartate receptor (NMDAR) encephalitis is from a Philadelphia multi-institutional observational cohort study in which 577 patients (211 children) were enrolled. 58 Of the 472 patients who underwent first-line immunotherapy (which included any combination of steroids, IVIG and plasmapheresis) or tumour removal, 53% had symptom improvement within 4 weeks; good recovery was observed in 221 patients at 3 months and in 97% of these at 24 months. A retrospective case series of 20 children with N-methyl D aspartate receptor antibody encephalitis (NMDAR-AbE) demonstrated an 85% recovery rate with immunomodulatory treatment including IVIG. 59 A North Indian study of 11 children with NMDAR-AbE reported significant response to steroids and immunoglobulin in 58% of patients. 60 In a prospective Indian study of 15 patients aged 2–64 years with AIE, 67% of patients who were treated with IVIG, steroids or both showed significant improvement, with no further seizures or clinical relapse years at follow-up. 61 A single-arm, open-label study of 41 adult patients with possible autoimmune encephalitis demonstrated a clinical benefit from IVIG with significant improvement in neurological functional outcomes following IVIG treatment. 62 Nosadini et al. 63 carried out a systematic review and meta-analysis of 1550 adults and children from 652 articles with NMDAR-AbE the use of immunotherapy in NMDAR-AbE, which showed that a combination of immunotherapy including IVIG was associated with good functional outcome in affected patients and lack of immunotherapy within the first 30 days of illness onset was associated with poor functional outcomes. Bien and et al. 64 performed a randomised controlled trial (RCT) of 21 patients in which 16 were randomised to either tacrolimus or IVIG and were compared historical untreated controls. They found that immunotreated patients had a longer survival than historical controls. Contrarily, a retrospective case series of 10 children with limbic encephalitis, a form of AIE, failed to show benefit from IVIG treatment,65 and a case series of 10 Taiwanese children with limbic encephalitis showed that all enrolled patients had neuropsychiatric symptoms and 90% developed refractory epilepsy at a mean follow-up of 5.6 years, despite receiving high dose corticosteroid or IVIG treatment. 66

Intravenous immunoglobulin in acute demyelinating encephalomyelitis

Efficacy of IVIG treatment in acute demyelinating encephalomyelitis (ADEM) is suggested by several single case reports and case series. 6771 In a retrospective case series of 15 children with ADEM admitted to a single institution in Turkey, all 3 children who made poor response with subsequent IVIG treatment. 72 A similar finding was reported in a single-centre Turkish study of 15 children. 73 One study in Japan showed rapid recovery of consciousness and complete clinical improvement in three children with ADEM treated with IVIG. 74 Pradhan et al. reported on four patients with steroid refractory ADEM and also reported quick recovery following IVIG treatment. 75 A prospective observational study of 18 children with ADEM indicated that outcomes were better in children who received IVIG in the first week than those who did so in the second week of the illness. 76 The findings of a single centre Israeli study of 16 children with ADEM suggested a possible beneficial effect from IVIG when either given separately or combined with high dose methylprednisolone. 77 An Australian study demonstrated an improvement in disability scores in 11 children with infectious encephalitis, 8 children with NMDAR antibody encephalitis and 16 children with other immune mediated encephalitis. 78 In the same study, the proportion of children treated with IVIG who had a good outcome at follow-up (mean duration of 52 months) increased from baseline by 88% and 11% for NMDAR antibody encephalitis and other immune-mediated encephalitis respectively.

Summary

Although there is evidence that IVIG benefits some patients with encephalitis, the studies described above have several limitations. Most of the evidence from IVIG use in infectious encephalitis is from single case reports. The largest evidence of IVIG in infectious encephalitis is from a prospective study of children with acute encephalitis complicated by myocarditis, which was a non-randomised study where the study investigators were aware of treatment allocation. 56 In addition, this study was conducted in a developing setting, and it is unclear how the generalisable are the study findings. The evidence from the studies of AIE are compelling. However, the study by Titulaer et al. was not a RCT and enrolled patients received other immunomodulatory treatment alongside IVIG, which makes it impossible to attribute the observed clinical efficacy to IVIG treatment alone. 58 Furthermore, the study by Lee et al. is limited by the small sample size and also lack of a control arm.

The rising use of IVIG in patients with encephalitis in the absence of robust evidence is not without cost implications. In a previously described single-centre study of IVIG use in Australia,79 the total cost of IVIG was US$ 2,595,907 (median $3538/patient, range $544–260,766). In the UK, IVIG costs £18–22 per gram, equivalent to £2100–£3080 per 2 g/kg for a 70-kg patient. 80 Given the high cost associated with IVIG use and its limited availability, and the crucial need to improve outcomes from encephalitis, robust evidence of efficacy from IVIG treatment is imperative.

Chapter 2 Methods

Trial design

ImmunoglobuliN in the Treatment of Encephalitis (IgNiTE) was a randomised, double-blinded, parallel arm, placebo-controlled study to compare early IVIG treatment with placebo in the treatment of childhood encephalitis in individuals aged 6 months to 16 years.

Research governance

This IgNiTE trial was conducted in compliance with the principles of the Declaration of Helsinki (1996), in full conformity with the International Conference on Harmonisation of Technical Requirements for Registration of Pharmaceuticals for Human Use (ICH) Guidelines for Good Clinical Practice (CPMP/ICH/135/95 July 1996), the Research Governance Framework and the Medicines for Human Use (Clinical Trial) Regulations 2004. Ethics approval was granted by the UK National Research Ethics Service (NRES) committee (South Central – Oxford A; REC 14/SC/1416). Clinical trial (CT) authorisation granted via the Medicines and Healthcare Products Regulatory Agency (MHRA) notification scheme (Ref: 21584/0337/001-0001). Written approval from local Research and Development (R&D) departments at each participating site was obtained before recruitment was commenced at each site. This trial was sponsored by the University of Oxford and was adopted on the UK children Research Network portfolio (co-adopted by Infectious Diseases and Neurological) UKCRN ID 18993. Quality assurance strategies were in place to ensure compliance with the CT regulations. The trial was registered for an International Standard Randomised Controlled Trial Number (ISRCTN), which was assigned on 24 June 2015 (ISRCTN 15791925). The study was assigned a European Clinical Trials Database number (2014-002997-35) and was registered with ClinicalTrials.gov (identifier NCT 02308982) on 5 December 2014. The trial protocol was published on 3 November 2016. 81 The study database OpenClinicaTM was designed and delivered by the Oxford Vaccine Group Clinical Trials Unit. A Trial Steering Committee (TSC) was set up to oversee the trial. The committee comprised an independent chairperson, an independent patient and public involvement (PPI) member, two independent clinicians, the chief investigator (CI), co-investigators and trial statisticians. The TSC met regularly to monitor and advise on study progress and conduct. An independent Data Monitoring and Ethics Committee (DMEC) was set up to monitor the main outcome measures and to ensure the safety of trial participants. The committee comprised an independent chairperson, a statistician and an expert clinician. The DMEC met regularly throughout the trial to monitor safety, efficacy and the overall conduct of the study.

The protocol was amended after the trial was terminated early to remove endpoints which could not be derived from the data collected and to update the statistical analysis section; this is reflected in this report.

Funding

The study was funded by the National Institute for Health and Care Research (NIHR) Efficacy and Mechanism Evaluation programme (reference 12/212/15). The investigational medicinal product (IMP), IVIG (Privigen) was provided by CSL Behring. The matching placebo (0.9% saline and 0.1% albumin) was manufactured at the Royal Liverpool and Broadgreen Aseptic Manufacturing Unit under its manufacturing license; funds for this were provided by CSL Behring.

Inclusion and exclusion criteria

The inclusion criteria were adapted from the International Encephalitis Consortium case definition. 82

Inclusion criteria

  1. Age 6 weeks to 16 years old.

  2. Acute (within 24 hours) or subacute (24 hours to 4 weeks) onset of altered mental state (reduced or altered conscious level, irritability, altered personality or behaviour, lethargy) not attributable to a metabolic cause.

  3. At least two of:

    • fever ≥38°C within 72 hours before or after presentation to hospital

    • new or acute onset brain imaging consistent with encephalitis or immune-mediated encephalopathy

    • cerebrospinal fluid (CSF) white cell count (WCC) >4/microlitre

    • generalised or partial seizures not fully attributable to a pre-existing seizure disorde;

    • new-onset focal neurological signs (including movement disorders) for >6 hours

    • EEG abnormality that is consistent with encephalitis and not clearly attributable to another cause.

  4. Parent/guardian/legal representative consent to the patient participating in the trial.

Exclusion criteria

Children and young people were not eligible to participate if any of the following applied:

  • high clinical suspicion of bacterial meningitis or TB meningitis (e.g. presence of frankly purulent CSF; CSF WCC > 1000/microlitre; bacteria on Gram stain and/or culture)

  • prior receipt of any IVIG product during the index admission

  • traumatic brain injury

  • known metabolic encephalopathy

  • toxic encephalopathy

  • hypertensive encephalopathy/posterior reversible encephalopathy syndrome

  • pre-existing demyelinating disorder; pre-existing antibody-mediated central nervous system disorder; pre-existing CSF diversion

  • ischaemic or haemorrhagic stroke

  • children with a contraindication to IVIG or albumin

  • known hypercoagulable state

  • significant renal impairment defined as glomerular filtration rate of 29 ml/min/1.73 m2 and below (Chronic Kidney Disease Stage 4)

  • known hyperprolinaemia

  • known to be pregnant

  • any other significant disease or disorder which, in the opinion of the investigator, may either put the participants at risk because of participation in the trial or may influence the result of the trial, or the participant’s ability to participate in the trial

  • participants who were being actively followed up in another research trial involving an IMP which had a potential immunomodulatory or neuroprotective effect.

Study procedures

Informed consent

Written informed consent was obtained from all participants before enrolment to the study. Parents and guardians had the opportunity to review the participant information sheet and participant consent form prior to participation. Informed consent was taken by a suitably qualified and experienced medical doctor, as delegated by the CI. Information sheets and assent forms for different age groups were available and where possible, verbal assent and consent from participants was obtained.

Study flow chart

Figure 1 shows the study flow chart.

FIGURE 1.

Study flow chart

Randomisation and allocation procedure

Randomisation was performed using a secure web-based randomisation system (Sortition®) which was developed by the Clinical Trials Unit in the Nuffield Department of Primary Care Health Sciences, University of Oxford. Randomisation was performed soon as possible after consent was obtained, and within the time window for administration of the first dose of study drug. Allocation sequence was generated by the trial statistician. Stratification variables accounted for at randomisation were age group (<1 year, 1–4 years, 5–9 years, 10–14 years and ≥15 years) and steroid treatment at the time of randomisation, using stratified block randomisation with randomly varying block sizes. Participants were allocated in a 1 : 1 ratio to receive 2 doses (1 g/kg/dose) of either IVIG or matching placebo, in addition to standard care. Confirmation of randomisation was electronically delivered to the investigator performing the randomisation, core members of the central coordinating team, and the independent pharmacy team at each study site.

A rigid blinding process was in place all throughout the study. Participants, their parents/guardians/authorised legal representative, in addition to study staff and clinical staff who were actively involved in the conduct of the study (including recruitment, administration of study treatment, data collection and entry, laboratory analyses) were blind to the treatment allocation through the entire study period. Study monitors who were independent of the study and all site pharmacists were unblinded. The latter was to ensure robust IMP management at each study site. Performance and ascertainment bias were minimised by measures designed to maintain the blinding including identical packaging of IVIG and matched placebo. Dispensing of the correct allocation was performed by the independent pharmacy team who had to be unblinded for this purpose.

Treatment

The IVIG used in the study was Privigen (100 mg/ml solution), with a shelf life of 3 years. The placebo was a mixture of 0.9% saline +0.1 human albumin solution, which had a shelf life of 6 months. The addition of albumin to saline was necessary to make the placebo visually identical to IVIG. Also, similar packaging and labelling were applied to both study treatments. A tear-off label distinguishing both treatments was taken off at the time of dispensing by the unblinded pharmacist at each recruiting site. A dosing guide based on weight band was provided to avoid IMP wastage.

Outcome measures

Primary outcome: Glasgow Outcome Score extended, paediatric version

The primary outcome measure was the Glasgow Outcome Score-Extended, paediatric version (GOS-E Peds) at 12 months after randomisation. The GOS-E Peds is a modified version of the GOS-E, a gold standard for measuring outcomes in adults with traumatic brain injury. The GOS-E Peds provides a developmentally appropriate structured interview necessary to evaluate children across different age groups. Its use has been validated and found to be sensitive to both severity of injury and to recovery over time, at least 6 months after brain injury and has been suggested as useful in guiding treatment in the early phases of recovery from brain injury.

Based on responses provided to the questions contained in the GOS-E Peds, participants were assigned to one of eight categories: 1-Upper Good Recovery, 2-Lower Good Recovery, 3-Upper Moderate Disability, 4-Lower Moderate Disability, 5-Upper Severe Disability, 6-Lower Severe Disability, 7-Vegetative State, and 8-Death. ‘Good recovery’ was defined as a GOS-E Peds score of two or lower and a score of >2 indicated ‘poor recovery’.

Secondary outcomes
Clinical

Secondary clinical outcomes were obtained from routinely collected medical information. These included the need for admission to ICU, invasive ventilation requirement and the length of hospital stay, which was defined as the number of days from admission to a recruiting site to discharge from acute care (i.e. not including days in hospital for neurorehabilitation). At 6 and 12 months after randomisation, information on new diagnosis of epilepsy and need for anti-epileptic treatment since discharge were collected.

Neurological

Secondary neurological outcomes were assessed using various age-appropriate questionnaires and outcome scores, which included the GOS-E Peds (assessed at 6 months after randomisation), Liverpool Outcome Score (LOS), Pediatric Quality of Life Score (PedsQL), Gross Motor Function Classification System (GMFCS), SDQ and Adaptive Behaviors Assessment System, second edition (ABAS-II), all assessed at 4–8 weeks after discharge from acute care and 12 months after randomisation. In addition, a blinded neuropsychology assessment was performed at 12 months after randomisation during which cognitive function was assessed using the following age-appropriate scales: (1) Bayley Scales of Infant and Toddler Development, third edition (1 to 2 years 5 months); (2) Wechsler Preschool Primary Scale of Intelligence IV (2 years 6 months to 5 years 11 months), and (3) Wechsler Intelligence Scale for Children V (6 years to 16 years 11 months).

The LOS is a validated tool for assessing level of disability after encephalitis in infants and children. It was originally designed to assess disease burden following JE and its use has been extended to other forms of encephalitis. For each participant, a total score (sum of scores for all questions) and an outcome score (the lowest score for any single question) were documented. Based on the outcome score only, participants were assigned to one of five outcome categories: 5-Full recovery, 4-Minor sequelae, 3-Moderate sequelae, 2-Severe sequelae, and 1-Death. ‘Good recovery’ was defined as a LOS of 5 and a score of ≤4 indicated ‘poor recovery’.

The PedsQL is a brief measure of health-related quality of life comprised of 23 items assessing quality of life in 4 domains: physical functioning (8 items), emotional functioning (5 items), social functioning (5 items) and school functioning (5 items). Based on the scores in each domain, two summary scores (physical health and psychosocial health summary scores) as well as a total scale score were computed. Total scale scores are presented. A higher total scale score indicates better quality of life.

The GMFCS is an assessment tool based on self-initiated movement and assesses motor function in three areas – walking, sitting and standing. It uses five levels to describe the motor function limitations, taking into consideration age, the use of mobility aids and the quality of movement. The GMFCS is rated from Level 1 (walks without limitations) to Level 5 (transported in a manual wheelchair). Levels 1 and 2 indicate independent mobility. Level 3 indicates ability to move with assistive devices while Levels 4 and 5 indicate significant limitation and dependence on helpers for minor movements. Gross motor function was categorised as mild (Levels 1 and 2), moderate (Level 3) and severe (Levels 4 and 5).

The SDQ is a 25-item questionnaire comprising 5 scales of 5 items each focusing on difficulties relating to emotional functioning, conduct, hyperactivity and interaction with peers. Scale scores and a total difficulties score (generated by summing the scores from all the scales except the prosocial scale) were documented. Based on the total difficulties score, SDQ scores were categorised into four bands: close to average, slightly lower, low and very low, based on a UK community sample. For 2–4-year-old children, the close to average category contains 80%, the slightly raised category contains 12%, the high category contains 4% and the very high category contains 4% of the population. For 4–17-year-old parent-completed questionnaires, the close to average category contains 80%, the slightly raised category contains 10%, the high category contains 5% and the very high category contains 5% of the sampled UK population.

The ABAS-II is an instrument used to evaluate adaptive skills that are important to everyday living and assesses three main domains: (1) Conceptual (summarises performance in the following skill areas – communication, functional academics and self-direction), (2) Social (leisure and social), and (3) Practical (community use, home living, health and safety, self-care). The individual response provided for each skill area question was assigned a score. The total score allocated to each domain was obtained by summing up the skills scores in that domain. Raw scores were converted into composite scores, with a population mean of 100 and a standard deviation of 15, with a lower score signifying worse adaptive behavior. Composite scores were divided into the following categories based on percentiles (%) of the normative population: very superior >130 (≥ 98%); superior 120–129 (91–97%); above average 110–119 (75–90%); average 90–109 (25–74%); below average 80–89 (9–24%); borderline 71–79 (3–8%); extremely low 70 or less (≤2%).

The Bayley Scales of Infant and Toddler Development (BSID-III) is a widely used and validated measure of cognitive functioning which produces three composite scores: cognitive scale, language scale (receptive and expressive) and motor scale (fine and gross). The Wechsler Preschool Primary Scale of Intelligence IV produces scores for: Verbal Comprehension Index (VCI), Visual Spatial Index (VSI), Fluid Reasoning, Working Memory Index (WMI), Processing Speed Index (PSI) and Full-Scale IQ (FSIQ). The Wechsler Intelligence Scale for Children IV assesses general thinking and reasoning skills and is made up of 10 subtests, yielding 4 composite scores (Verbal Comprehension, Perceptual Reasoning Index (PRI), Working Memory, and Processing Speed). The Full-Scale IQ (composite score) is an average of these four scales. Composite standard scores have a mean of 100 and SD of 15. Neurodevelopmental outcome was classified as (1) severe impairment (composite score of <70, >2SD below the mean), (2) mild impairment (score of 70–84, >1SD below the mean) and (3) normal neurodevelopmental (score of ≥85).

Neuroimmunology

Auto-antibody testing was performed by the clinical neuroimmunology service at the Nuffield Department of Clinical Neurosciences, Oxford. Testing was done for antibodies against live neurons, Aquaporin 4, NMDAR, Myelin oligodendrocyte glycoprotein (MOG), leucine-rich, glioma inactivated 1 (LGI1) and Contactin-associated protein-like 2 (CASPR2).

Neuroimaging

Neuroimaging findings were obtained from clinical scans (i.e. scans performed as part of routine clinical care). In addition, an optional follow-up research scan was performed in a subset of participants, where consent was provided. Anonymised research scans provided on a compact disc were analysed by a neuroradiologist at University College London who reported the following:

Initial clinical scan(s):

  • proportion of participants with an abnormal scan

  • distribution of disease – structural and functional anatomy of lesion

  • subset of radiological features (mass effect, hydrocephalus, enhancement, other).

Follow up scan(s):

  • proportion of participants with an abnormal scan

  • lesion resolution/persisting disease

  • presence of new lesions

  • distribution of disease – structural and functional anatomy of lesion

  • subset of radiological features (mass effect, hydrocephalus, enhancement, other).

Mortality

Information on any deaths occurring up to 12 months after randomisation was collected.

Safety

Safety outcomes were obtained throughout the study (see Safety monitoring). In addition, a mandatory full blood count check was performed for all participants 24–48 hours following the second dose of the study treatment to monitor for haemolysis which has previously been described with high concentrations of IVIG treatment. 83

Schedule of visits

A schedule of visits is shown in Appendix 1.

Screening

The purpose of the screening visit was to fully assess the child’s eligibility for the study. Parents/Legal guardians of potential patients were then approached to explain the study and address any queries. The participant information sheet was provided to families who were given sufficient time to decide on whether they wanted their child to participate in the study. Where interest was indicated, written consent was obtained and relevant clinical information was collected. A screening log was maintained throughout the study.

T0: enrolment and randomisation

After obtaining written consent, participants were enrolled to the study and allocated a study number. They were then randomised using the online randomisation system. Following randomisation, electronic confirmation was sent to research staff performing the randomisation, the site Principal Investigator (PI), the site pharmacist and the coordinating team in Oxford. The electronic confirmation specified an allocation number which the site pharmacist used to dispense the study treatment, using an allocation list that was held securely by the pharmacy team and the trial statisticians only.

T1 and T2: IMP administration visits

T1 was the day of administration of the first dose of study treatment. This was as soon as possible after enrolment and within five working days from when a diagnosis of encephalitis was suspected. For participants transferred from a non-participating site during the illness, an additional three working days from admission to the IgNiTE site was allowable if this gave more time for enrolment than five working days from suspicion of a diagnosis of encephalitis. The second dose was administered 24 hours after the first dose (T2).

Each dose of study treatment was based on the participant’s weight (1 g/kg/dose). To avoid wastage a dose-banding guide based on the participant’s weight, which rounded up the total dose of study treatment to be administered to a whole number, was used.

T1 + 24h: research sampling

This visit occurred 24 hours after the first dose of study treatment. Where consent was provided, research specific blood samples were obtained at this time point.

T2 + 24–48 hours

This visit occurred between 24 and 48 hours after receipt of the second dose of study treatment. At this time point, a mandatory full blood count was obtained from all participants to assess for evidence of haemolysis.

T2 + 7 days

This visit occurred 7 days after receipt of the second dose of study treatment. Where consent was provided, research specific blood sample was obtained at this time point.

T3: prior to discharge from medical care

This visit occurred up to 48 hours prior to discharge from medical care. Clinical and laboratory investigation results were collected.

T4: 4–8 weeks after discharge from acute care

At this timepoint, participants completed the study questionnaires.

T5: 6 months after randomisation (+/– 4 weeks)

The GOS-E Peds (secondary outcome) was completed by participants and a research specific MRI scan was performed where consent was provided. Research sampling was also performed at this timepoint, where consent was provided.

T6: 12 months (+/– 4 weeks) after randomisation

Participants were assessed for the primary outcome during a face-to-face visit at this time point. The study questionnaires were completed at this timepoint. A neuropsychology assessment of cognitive function using age-appropriate assessment tools (see section Chapter 2, Secondary outcomes) was performed by a study neuropsychologist who was unaware of the participants’ treatment allocation.

At each study visit time point, eligibility and consent were re-affirmed before any study procedures were performed, relevant clinical information and information regarding serious adverse events (SAEs) were obtained and entered onto an electronic case report form (eCRF).

Collection of research samples and storage

Where specific consent was provided, blood was taken for autoantibody testing, RNA and DNA analysis in line with the study protocol.

Concomitant medication

Details of concomitant medications were collected throughout the study. These included antimicrobials, steroids, anticonvulsants, immunomodulatory treatment (commenced after randomisation), hyperosmolar treatment such as Mannitol and 3% saline, IVIG (as part of routine care and not administered before study treatment), and blood transfusion.

Safety monitoring

Participants were monitored during, and 20 minutes after administration of the study treatment for AEs. The following were reportable in this study:

  • AEs and adverse events of special interest (AESIs) occurring in the first 5 days following receipt of each dose of the study drug

  • SAEs occurring up until 6 months after randomisation

  • serious adverse reactions (SARs) occurring throughout the study period.

An AE was defined as an untoward medical occurrence in a participant that was not necessarily caused by or related to the IMP and was assessed as ‘not related’ or ‘unlikely related’. An adverse reaction (AR) was defined as an untoward and unintended response to the IMP related to any dose administered and was assessed as ‘definitely, likely or possibly related’. An unexpected AR was defined as an AR, the nature and severity of which was not consistent with known information about the IMP. The Summary of Product Characteristics for Privigen was used to assess relatedness of ARs to the study treatment. A SAR was defined as an AE that was both serious and, in the opinion of the reporting Investigator, believed with reasonable probability to be due to one of the trial treatments, based on the information provided. An AESI was defined as any AE of significant scientific, medical, and public interest, relating to an IMP and for which ongoing monitoring and rapid communication by the investigator to the study sponsor could be appropriate.

For each AE, the following information were recorded: description, date of onset and end date, severity and assessment of relatedness to the trial treatment, other suspect drug or device and action taken. The severity was assessed based on the degree to which these affect routine care using the following scale: 1 = mild, 2 = moderate, 3 = severe, 4 = life-threatening, 5 = death. Assessment of causality (i.e. the relationship between an AE and the trial treatment) was performed by a medically qualified investigator at each study site. AEs or ARs that were assessed to be serious (i.e. fatal, life-threatening, resulting in inpatient hospitalisation or prolongation of hospitalisation, resulted in persistent/significant disability or incapacity, or congenital anomaly/birth defect) were reviewed by a delegated medical doctor and reported to the CI, the study sponsor, and CSL Behring within 24 hours after the study team became aware of the event. All AESIs, SAEs and SARS were followed either until resolution, or the event was considered stable. AESIs included the following: (1) anaphylaxis, (2) new onset seizure or abnormal movements not thought to be due to the encephalitis illness, (3) thromboembolism, (4) aseptic meningitis unrelated to the encephalitis illness, (5) acute renal failure, (6) acute haemolysis and (7) other medically significant event as determined by the investigator. The CI and trial manager provided an annual report of all SAEs and SARs (expected and unexpected), which were distributed to the sponsor, and the Research Ethics Committee (REC). The Sponsor reported all SAEs and SARs to the MHRA as part of the annual Drug Safety Update Report. In addition, throughout the duration of the trial, the DMEC reviewed safety data on an ongoing basis to rule out any significant safety concerns.

Data collection and management

Data were collected by clinical staff using paper-based source documents and were subsequently transcribed onto a secure web-based password-protected eCRF, OpenClinicaTM. The paper and electronic data-collection forms were created in accordance with the requirements of the trial protocol. The eCRF was hosted and maintained by the Oxford Vaccine Group Clinical Trials Unit. All participants were identified using a unique trial-specific number and participant-identifiable data were not included in either the paper or eCRF. At the end of the study, the eCRF system was locked and the data were exported for final analysis after data cleaning. All trial data will be stored and archived in line with the Medicines for Human Use (Clinical Trials) Amended Regulations 2006. All study documents will be retained after the completion or discontinuation of the trial for 3 years after the youngest participant turns 18 years.

Management of the study

The trial was coordinated through the Oxford Vaccine Group, a UK Clinical Research Collaboration registered CTs unit working in collaboration with the Primary Care trials unit at the University of Oxford (registration number: 52). The study coordinating team were responsible for the overall management of the trial and comprised the CI, a study lead doctor and nurse, a trial manager and a quality assurance manager. A study team was set up at each recruiting site to oversee the day-to-day running of the trial and publicise the study within the site. Close communication lines were maintained between individual study teams and the coordinating team. In addition, a Trial Management Group was set up to address and discuss clinical queries and the scientific aspects of the study.

The trial master file (TMF) contained all essential documents for the conduct of the trial: approved trial protocols, regulatory approvals, financial and legal documents, the delegation of trial duties log, copies of approved participant information sheets, participant consent forms, screening logs, standard operating procedures, pharmacy/IMP, safety monitoring, etc. The trial manager was responsible for maintaining the TMF.

Monitoring was performed in line with a trial-specific monitoring plan and comprised remote monitoring of the eCRF data and self-monitoring questionnaires completed by each site. A triggered site visit was necessary for sites that either provided a significant proportion of study data or if queries raised during remote monitoring were not resolved. Review of monitoring activity was conducted by a representative of the study sponsor. After each monitoring visit, the trial manager provided a report summarising the documents that had been reviewed and actions required by the study team which was reviewed by the sponsor and CI.

Recruitment and retention

Participant identification and recruitment

Participants were recruited from NHS Hospitals in the UK, as shown in Appendix 2. At each site, potential participants were identified through various routes which included review of medical handover notes, checking the wards for new admissions with a suspected diagnosis of encephalitis, and review of routine clinical investigation results. Following identification of a potentially eligible patient, their clinical presentation was matched against the study inclusion criteria. Parents/guardians of the patients meeting the study criteria were approached by a member of the clinical team to seek their interest in the study. If interest was indicated, a member of the research team approached the family to confirm eligibility and to seek consent. Assent from the participant was also required if they were ≥6 years of age and judged to have sufficient mental capacity to provide this.

Retention of participants

The study team maintained an approachable relationship with participants and provided contact via telephone to discuss any aspect of the study and to remind them of follow-up.

Patient and public involvement

The Encephalitis Society were actively involved in preparing the proposal for this study. The Society agreed that there is the pressing need for improved treatments to address the serious problem of encephalitis, and fully supported the study. A representative of The Encephalitis Society was on the Trial Management Group and provided a patient-centred research perspective to the study design and conduct. The Encephalitis Society was heavily involved in training research nurses and study recruiters. PPI groups were consulted in the development of the essential documents for the study including the participant information sheet and consent forms. Three PPI representatives with previous personal experiences of encephalitis sat on the TSC and contributed to providing overall oversight of the study. Study update meetings were held to which patients previously affected by encephalitis were invited to share their experiences with study teams, thus highlighting the importance of the study. Preliminary blinded results from the study were presented at various national level meetings and conferences. The Plain language summary of this report was reviewed by the Encephalitis Society. The Encephalitis Society will be actively involved in dissemination of the study findings.

Equality, diversity and inclusion

This trial involved individuals with a rare disease; this patient group is often under-served in clinical research. We sought to enrol all eligible children, regardless of their age, gender or ethnicity. The trial was conducted across 21 NHS sites across the UK, serving different local populations. We involved PPI groups in the design and conduct of this study. Children were actively involved in the consent process; children aged ≥6 years and judged to have sufficient mental capacity were required to give assent.

Chapter 3 Statistics

Sample size

At the time of conception of the IgNiTE trial, there were insufficient data from previous studies for sample size calculation. Detection of at least 20% treatment difference from 43% in the ‘good recovery’ rate (i.e. GOS-E Peds score 2 or lower) by 12 months after randomisation was deemed clinically significant. This was based on the results of a large observational study on autoimmune encephalitis by Titulaer et al. 58 A sample size of 308 (154 per group, including an approximate 10% attrition rate) was needed to achieve 90% power (at 5% level of significance, 2-sided) at detecting a difference in the primary outcome between the study groups.

Statistical methods

The analyses were performed on the intention-to-treat (ITT) population; this included all 18 participants who were randomised. In the analysis of the AEs, the population analysed were the 16 participants who received study treatment.

Since only 20% of participants were recruited before the trial was halted, all analyses are descriptive. Hypothesis testing of outcomes has not been conducted, as these analyses would be severely underpowered. Furthermore, no subgroup comparisons or sensitivity analyses were conducted due to the small number of participants.

Descriptive analysis

A Consolidated Standards of Reporting Trials (CONSORT) flow chart was constructed to summarise the flow of participants through the study. Baseline characteristics are summarised by randomised arm to examine balance between the arms at baseline. All outcomes are presented by time point and randomised group, using descriptive statistics. The proportion of participants lost to follow-up or with missing objective are summarised by treatment arm and at each time point. For continuous variables, the mean (normally distributed data) and standard deviation or the median (skewed data) and inter-quartile range (IQR), or range are presented. Binary and categorical variables are presented as counts and percentages.

Statistical software

All analyses were carried out in R version 4.1.1.

Chapter 4 Results

Here we describe the recruitment process and describe results of the primary and secondary outcomes of the study. The exploratory laboratory endpoints were not analysed due to lack of funding to undertake the relevant testing.

Recruitment and participant flow

Recruitment took place between 23 December 2015 and 26 September 2017. During this time, a total of 18 participants were recruited from 21 NHS sites. Appendix 2 shows the recruitment sites and number of participants enrolled from each site. Figure 2 is the CONSORT flow diagram for the trial, which summarises the participant flow through the trial.

FIGURE 2.

CONSORT diagram.

Baseline characteristics

Table 1 summarises the key baseline demographics by treatment arm. The mean age of the participants was 4.09 years (IQR 2.0–11.8), 44% were male, and 89% were of white ethnicity.

IVIG (n = 10) Placebo (n = 8) All (n = 18)
Age at randomisation (years) Median (IQR) 5.55 (1.52–11.8) 4.09 (2.71–9.64) 4.09 (2.0–11.8)
Sex (%) Male 4 (40) 4 (50) 8 (44.4)
Female 6 (60) 4 (50) 10 (55.6)
Ethnicity (%) White 8 (80) 8 (100) 16 (88.9)
Asian 1 (10) 0 (0) 1 (5.6)
Missing 1 (10) 0 (0) 1 (5.6)
History of immunocompromise (%) No 9 (90) 7 (87.5) 16 (88.9)
Missing 1 (10) 1 (12.5) 2 (11.1)
Previous diagnosis of encephalitis (%) No 9 (90) 7 (87.5) 16 (88.9)
Missing 1 (10) 1 (12.5) 2 (11.1)
History of encephalopathic illness (%) No 9 (90) 7 (87.5) 16 (88.9)
Missing 1 (10) 1 (12.5) 2 (11.1)
Pre-existing diagnosis of epilepsy (%) No 9 (90) 7 (87.5) 16 (88.9)
Missing 1 (10) 1 (12.5) 2 (11.1)

Ten participants were randomised to IVIG treatment, and eight participants were randomised to the placebo treatment. Baseline characteristics were balanced between the study groups, although there was a tendency towards lower age in the placebo group and the IVIG arm had slightly more females.

Withdrawal from treatment and from the study

The retention rate of the study was high and comparable between both groups at 12 months after randomisation: 80% (IVIG group) versus 75% (placebo group). Two participants (one in each study group) were withdrawn from the study before receipt of the first dose of study treatment; this was due to one participant being transferred urgently to a non-IgNiTE participating hospital and study treatment being unavailable for another participant. One participant in the IVIG group withdrew consent prior to the 12 months after randomisation time point.

Adherence and compliance with treatment

One participant in the placebo group received only one dose of study treatment due to refusal of the second dose.

Loss to follow-up and missing data

At the 12-month visit for primary endpoint, there were two withdrawals from the IVIG group and one withdrawal and one loss to follow up from the placebo group. The median age for these four participants who had missing data at the 12-month visit for primary endpoint was 8.5 years and 3 (75%) were female. The median age for those with no missing data at the same timepoint was 4.1 years, and 50% were female. Due to small numbers, formal comparison of the two groups was not conducted.

All 18 randomised participants were included in the ITT analysis for primary and secondary outcomes, and all 16 participants who received study treatment were included in the safety analysis.

Primary outcome: GOS-E Peds at 12 months

The primary outcome was assessed using the GOS-E Peds, an outcome scale used to assess level of disability, at 12 months after randomisation. The proportion of participants who made good recovery was similar between both study groups, as shown in Table 2.

IVIG (N = 10) (%) Placebo (N = 8) (%) Overall (N = 18)
GOS-E Peds Scorea
 1. Upper good recovery 4 (40) 4 (50) 8 (44%)
 2. Lower good recovery 1 (10) 0 (0) 1 (6%)
 5. Upper severe disability 1 (10) 1 (13) 2 (11%)
 6. Lower severe disability 2 (20) 1 (13) 3 (17%)
Participants with missing data due to being withdrawn or lost to follow-up 2 (20) 2 (25) 4 (22%)

Participants were assigned to one of 8 categories: 1-Upper Good Recovery, 2-Lower Good Recovery, 3-Upper Moderate Disability, 4-Lower Moderate Disability, 5-Upper Severe Disability, 6-Lower Severe Disability, 7-Vegetative State, and 8-Death. ‘Good recovery’ was defined as a GOS-E Peds score of two or lower and a score of >2 indicated ‘poor recovery’.

Primary analysis

Nine participants [50%; IVIG n = 5 (50%); placebo n = 4 (50%)] made a good recovery, defined as a GOS-E Peds score of <2. Five participants [28%; IVIG n = 3 (30%), placebo n = 2 (25%)] made a poor recovery and four participants [22%; IVIG n = 2 (20%), placebo n = 2 (25%)] did not undergo a GOS-E Peds assessment at 12 months after randomisation.

Secondary outcomes

Clinical outcomes

Table 3 summarises results of the clinical outcomes assessed in the study.

Outcome IVIG

(N = 10)		 Placebo

(N = 8)		 Overall

(N = 18)
During hospital stay
 Duration of ventilation Median (IQR) 2.5 (2.0–3.5)

(n = 4)		 2.0 (2.0–3.0)

(n = 5)		 2.0 (2.0–3.0)

(n = 9)
 Length of ICU stay Median (IQR) 4.0 (3.0–6.0)

(n = 5)		 5.0 (2.0–10.0)

(n = 5)		 4.5 (3.0–6.8)

(n = 10)
 Length of hospitalisation for acute care Median (IQR) 12.0 (8.0–27.0)

(n = 9)		 8.0 (6.5–14.0)

(n = 7)		 11.0 (7.8–19.5)

(n = 16)
6 months post randomisation
 New diagnosis of epilepsy since discharge n (%) 1 (10) 1 (13) 2 (11)
 Anti-epileptic treatment since discharge n (%) 1 (10) 1 (13) 2 (11)
12 months post randomisation
 New diagnosis of epilepsy since discharge n (%) 0 (0) 1 (13) 1 (6)
 Anti-epileptic treatment since discharge n (%) 0 (0) 0 (0) 0 (0)
Duration of ventilation

Ten participants [56%; IVIG n = 5 (50%), placebo = 5 (63%)] were admitted to the ICU during the admission and nine of these (IVIG n = 4, placebo n = 5) required invasive ventilation. The median duration of invasive ventilation was similar between both study groups: 2.5 days (IQR 2–3.5) for the IVIG group versus 2 days (IQR 2–3) for the placebo group.

Length of ICU stay

The median length of stay on ICU did not differ between both study groups and was 4 days (IQR 3–6) for the IVIG group and 5 days (IQR 2–10) for the placebo group.

Length of hospitalisation

The median length of hospitalisation was 12 days (IQR 8–27) for the IVIG group versus 8 days (IQR 6.5–14) for the placebo group.

New diagnosis of epilepsy

At 6 months after randomisation, two participants [11%; IVIG n = 1 (10%), placebo n = 1 (13%)] had a new diagnosis of epilepsy. At 12 months after randomisation, one additional participant in the placebo group (13%) had a new diagnosis of epilepsy versus none of the participants in the IVIG group. Five participants [28%; IVIG n = 2 (20%), placebo n = 3 (38%)] had incomplete data for this outcome.

Neurological outcomes

Table 4 summarises the secondary neurological outcomes.

Outcome 4–8 weeks post discharge 12 months post randomisation
IVIG (N = 10) Placebo (N = 8) IVIG (N = 10) Placebo (N = 8)
LOS
 2. Severe sequelae (%) 2 (20) 2 (25) 2 (20) 2 (25)
 3. Moderate sequelae (%) 2 (20) 3 (38) 1 (10) 1 (13)
 4. Minor sequelae (%) 1 (10) 0 (0) 1 (10) 1 (13)
 5. Full recovery (%) 3 (30) 2 (25) 4 (40) 2 (25)
 Missing data due to withdrawal or loss to follow-up of participant (%) 1 (10) 1 (13) 2 (20) 2 (25)
 Missing data – assessment not performed (%) 1 (10) 0 (0) 0 0
PedsQL
 Mean (SD) 77.9 (11.1) 56.5 (7.8) 79.9 (21.6) 63.7 (30.1)
 Missing data due to withdrawal or loss to follow-up of participant (%) 1 (10) 1 (13) 2 (20) 2 (25)
 Missing data – assessment not performed (%) 4 (40) 5 (63) 2 (20) 4 (50)
SDQ
 Close to average (%) 4 (40) 1 (13) 4 (40) 1 (13)
 Slightly raised (%) 1 (10) 0 (0) 1 (10) 0 (0)
 Very high (%) 0 (0) 1 (13) 1 (10) 1 (13)
 Missing data due to withdrawal or loss to follow-up of participant (%) 1 (10) 1 (13) 2 (20) 2 (25)
 Missing data – assessment not performed (%) 4 (40) 5 (63) 2 (20) 4 (50)
ABAS
 Very superior (%) 0 (0) 0 (0) 1 (10) 0 (0)
 Superior (%) 1 (10) 0 (0) 1 (10) 0 (0)
 Above average (%) 1 (10) 0 (0) 1 (10) 0 (0)
 Average (%) 2 (20) 1 (13) 0 (0) 1 (13)
 Below average (%) 0 (0) 1 (13) 1 (10) 0 (0)
 Borderline (%) 1 (10) 0 (0) 0 (0) 0 (0)
 Extremely low (%) 1 (10) 0 (0) 1 (10) 1 (13)
 Missing data due to withdrawal or loss to follow-up of participant (%) 1 (10) 1 (13) 2 (20) 2 (25)
 Missing data – assessment not performed (%) 3 (30) 5 (63) 3 (30) 4 (50)
GMFCSa
 Mild (%) 5 (50) 2 (25) 6 (60) 1 (13)
 Severe (%) 0 (0) 1 (13)
 Missing data due to withdrawal or loss to follow-up of participant (%) 1 (10) 1 (13) 2 (20) 2 (25)
 Missing data – assessment not performed (%) 4 (40) 5 (63) 2 (20) 4 (50)
GOSE-Peds at 6 months post randomisation
IVIG (N = 10) Placebo ( N  = 8)
 1. Upper good recovery (%) 4 (40) 4 (50)
 3. Upper moderate disability (%) 1 (10) 1 (13)
 5. Upper severe disability (%) 0 (0) 1 (13)
 6. Lower severe disability (%) 3 (30) 1 (13)
 Missing data due to withdrawal or loss to follow-up of participant (%) 2 (20) 1 (13)
 Missing data – assessment not performed (%) 0 (0) 0 (0)

GMFCS was categorised as mild (Levels 1 and 2), moderate (Level 3) and severe (Levels 4 and 5).

Glasgow Outcome Score-Extended, paediatric at 6 months after randomisation

At 6 months after randomisation, four participants in the IVIG group (40%) versus four participants in the placebo group (50%) made a good recovery, while four participants in the IVIG group (40%) versus 3 participants in the placebo group (38%) made poor recovery on the GOS-E Peds assessment. Three participants [17%; IVIG n = 2 (20%), placebo n = 1 (13%)] did not undergo a GOS-E Peds assessment at 6 months after randomisation.

Liverpool Outcome Score

At 4–8 weeks after discharge from acute care, three participants in the IVIG group (30%) versus two participants in the placebo group (25%) made full recovery (i.e. LOS > 4) while five participants in the IVIG group (50%) versus five participants in the placebo group (63%) made a poor recovery, reporting minor to severe sequelae. Three participants [17%; IVIG n = 2 (20%); placebo n = 1 (13%)] did not have LOS data collected at this timepoint.

At 12 months after randomisation, four participants in the IVIG group (40%) versus two participants in the placebo group (25%) made full recovery while four participants in the IVIG group (40%) versus four participants in the placebo group (50%) made poor recovery, reporting minor to severe sequelae. Four participants [22%; IVIG n = 2 (20%); placebo n = 2 (25%)] did not have LOS data collected at this timepoint.

Paediatric quality of life

Paediatric quality of life scores were available for seven participants [39%; IVIG n = 5 (50%), placebo n = 2 (25%)] at 4–8 weeks after discharge from acute care and for eight participants [44%; IVIG n = 6 (60%), placebo n = 2 (25%)] at 12 months post randomisation.

At 4–8 weeks after discharge from acute care, mean PedsQL scores were 77.9 (SD 11.10) for the IVIG group versus 56.5 (SD 7.8) for the placebo group. At 12 months after randomisation, PedsQL scores were 79.9 (SD 21.6) for the IVIG group versus 63.7 (SD 30.1) for the placebo group.

Gross motor function classification system

At 4–8 weeks after discharge from acute care, five participants in the IVIG group (50%) versus two participants in the placebo group (25%) had mild impairment of gross motor functioning. These data were not available for 11 participants [61%; IVIG n = 5 (50%), placebo n = 6 (75%)] at this timepoint.

At 12 months after randomisation, six participants (60%) versus two participants (25%) in the IVIG and placebo groups, respectively, experienced either mild or severe impairment of gross motor function. These data were not available for 10 participants [56%; IVIG n = 4 (40%), placebo n = 6 (75%)] at this timepoint.

Strengths and Difficulty Questionnaire

At 4–8 weeks after discharge from acute care, four participants in the IVIG group (40%) versus one participant in the placebo group (13%) had a score that was close to the average of the normative population, one participant in the IVIG group (10%) and none in the placebo group had a slightly raised score, while no participants in the IVIG group versus one participant in the placebo group (13%) had a very high score. These data were not available for 11 participants [61%; IVIG n = 5 (50%), placebo n = 6 (75%)] at this timepoint.

At 12 months after randomisation, four participants in the IVIG group (40%) versus one participant in the placebo group (13%) had a score that was close to the average for the normative population, one participant in the IVIG group (10%) versus none in the placebo group had a slightly raised score, and one participant each in the IVIG and placebo groups (10% vs. 13% respectively) had a high score when compared with the normative population. These data were not available for 10 participants [56%; IVIG n = 4 (40%), placebo n = 6 (75%)] at this timepoint.

Adaptive Behaviors Assessment System-second edition

At 4–8 weeks after discharge from acute care, four participants in the IVIG group (40%) versus one participant in the placebo group (13%) had a score that was either similar or higher than the average score for the normative population while two participants in the IVIG group (20%) versus one participant in the placebo group (13%) had a score that was lower than the average for the normative population. Ten participants [56%; IVIG n = 4 (40%), placebo n = 6 (75%)] did not have ABAS-II assessment at this timepoint.

At 12 months after randomisation, three participants in the IVIG group (30%) versus one participant in the placebo group (13%) had a score that was similar or higher when compared with the average score for the normative population, while two participants in the IVIG group (20%) versus one participant in the placebo group (13%) had a score that was below the average of the normative population. Eleven participants [61%; IVIG n = 5 (50%), placebo n = 6 (75%)] did not have ABAS-II assessment at this timepoint.

Neuropsychology assessment

The results of neuropsychology assessment at 12 months after randomisation are summarised in Table 5.

Participant Age at assessment Bayley cognitive score FSIQ VCI VSI/PRI WMI PSI
Placebo arm
 1 4y 8m - a a a a
 2 5y 6m - 79 95 79 75 71
 3 2y 10m - a a a a a
 4 2y 0m 110 - - - - -
 5 16y 10m - 89 99 88 83 94
IVIG arm
 6 4y 5m - a a a a a
 7 9y 2m - 104 92 111 107 116
 8 14y 1m - 95 102 90 99 91
 9 8y 8m - 88 93 96 91 83
 10 2y 2m 55 - - - - -
 11 3y 9m - 65 60 75 72 -
 12 2y 1m - a a a a a
 13 14y 6m - 119 108 110 110 131

Note

Young person unable to complete full battery due to attention or behavioural needs.

Green = normal neurodevelopmental score, Yellow = mild impairment, Red = severe impairment.

Thirteen participants [72%; IVIG n = 8 (80%); placebo n = 5 (63%)] had blinded neuropsychology assessment performed at 12 months after randomisation; four [30%; IVIG n = 2 (25%), placebo n = 2 (40%)] of these participants were unable to complete the full battery of assessments due to attention or behavioural needs. Five participants [28%; IVIG n = 2 (20%), placebo n = 3 (38%)] did not undergo neuropsychology assessment.

The proportion of participants (IVIG vs. placebo) with a score of ≥85 (indicating normal development) for each of the main composite scores were as follows: four (40%) versus one (13%) for FSIQ, four (40%) versus two (25%) for VCI, four (40%) versus one (13%) for VSI, four (40%) versus 0 (0%) for WMI; and three (30%) versus one (13%); for PRI. Two participants (one in each treatment arm) were assessed using the Bayley scale of infant development, one participant (IVIG arm) had severe neurodevelopmental outcome while the other (placebo arm) had a normal neurodevelopmental outcome.

Neuroimaging

Tables 68 summarise the neuroimaging results.

At baseline, 5 out of 19 acute scans (26%) were abnormal; 4 of these (80%) showed bilateral changes and one showed unilateral changes. There were nine follow-up scans for eight unique participants of which six (67%) were normal and unchanged from the acute scan while two (25%) scans showed abnormal changes.

Participant number Age at time of acute scan Type of scan Overall assessment Laterality of abnormality
1 3 years 7 months MRI Abnormal Bilateral
2 14 years MRI Normal N/A
3 1 year 9 months MRI Abnormal Unilateral (Right)
4 13 years CT scan Normal N/A
4 13 years MRI Abnormal Bilateral
5 8 years 2 months MRI Normal N/A
6 15 years 9 months CT scan Normal N/A
6 15 years 9 months MRI Normal N/A
7 1 year MRI Not available Not available
8 2 years 8 months MRI Normal N/A
8 2 years 8 months MRI Normal N/A
9 4 years 6 months MRI Abnormal Bilateral
10 7 years 8 months CT scan Normal N/A
10 7 years 8 months MRI Abnormal Bilateral
11 7 years 9 months MRI Normal N/A
12 1 year CT scan Normal N/A
12 1 year CT scan Normal N/A
12 1 year MRI Normal N/A
13 1 year 1 month CT scan Normal N/A

N/A, not applicable.

Participant number TEM FR PAR OCC INS BS CBL COR WM DGM DGM - BG DGM-TH DGM - Other SUN SN
1 Y N Y Y Y Y Y Y Y Y Y Y Y Y Y
3 N N N N N N N N N Y N Y N NA NA
4 Y Y Y Y Y N N Y N N N N N N N
9 N Y Y Y N Y N N Y N NA NA NA NA NA
10 Y Y Y Y Y Y Y N Y Y Y Y N NA NA

TEM, temporal; FR, frontal; PAR, parietal; OCC, occipital; INS, insular; BS, brainstem; CBL, cerebellum; COR, cortex; WM, white matter; DGM, deep gray matter; BG, basal ganglia; TH, thalamus; SUN, sub thalamic nuclei; SN, substantial nigra; Y, yes (lesion present); N, normal; NA, not assessed.

Participant Number Somatomotor/sensory Visual Auditory Limbic Extrapyr system Radiological pattern (A/V/I) Mass Hydro Enhc
1 N Y N Y Y V N N Y
3 N N N N N Non-specific N N N
4 N N N N N V Y N N
9 N N N N N V & I N N N
10 Y Y Y N N A & I N N N

Autoantibody testing

The results of autoantibody testing are shown in Table 9. Two participants (both in the placebo arm) were identified to have specific autoantibodies; one participant was positive for LGI1 antibodies, and one participant was positive for MOG antibodies. Two additional participants (both in the IVIG arm) were positive for IgG to live neurons, but negative for antibodies to the specific antigens tested for.

Participant number NEURONS NR1 (NMDAR-Ab) MOG-FL IgG1 AQP4 LGI1 CASPR2
1 Negative Negative Negative Negative Negative Negative
2 Negative Negative Negative Negative Negative Negative
3 Negative Negative Negative Negative Positive Negative
4 Positive Negative Negative Negative Negative Negative
5 Negative Negative Negative Negative Negative Negative
6 Positive Negative Negative Negative Negative Negative
7 Negative Negative Negative Negative Negative Negative
8 Negative Negative Negative Negative Negative Negative
9 Negative Negative Negative Negative Negative Negative
10 Negative Negative Negative Negative Negative Negative
11 Negative Negative Positive Negative Negative Negative
12 Negative Negative Negative Negative Negative Negative

Note

NR1, NMDA receptor subunit 1; NMDAR-Ab, N-methyl-D-aspartate receptor antibody; MOG-FL, full length myelin oligodendrocyte glycoprotein; LGI1, leucine-rich glioma-inactivated 1; CASPR2, contactin-associated protein-like 2.

Safety reporting

Safety outcomes are summarised in Table 10. One participant in the IVIG group (11%) versus none in the placebo group experienced an AESI within 5 days of receiving the study treatment. The participant developed a fever during infusion of IVIG, which was judged to be unrelated to the study treatment. Ten SAEs were reported in three participants in the placebo group (43%) versus none in the IVIG group. None of the SAEs were judged to be related to the study treatment. None of the participants experienced haemolysis following receipt of two doses of study treatment and there were no deaths reported during the study period.

Outcome IVIG (N = 9) Placebo (N = 7)
AEs of special interest (AESI) in the first 5 days from each dose
 AESIs reported No. participants 1 (11%) 0 (0%)
No. events 1 0
 Relationship to study treatment Related 0 (0%) -
Not related 1 (100%) -
SAEs up to 6 months post randomisation
 SAEs reported No. participants 0 (0%) 3 (43%)
No. events 0 10
 Relationship to study treatment Related - 0 (0%)
Not related - 10 (100%)
Haemolysis (drop in haemoglobin of >3 g/dl)
 Haemolysis present Yes (%) 0 (0) 0 (0)
No (%) 9 (100) 4 (57)
Missing data (%) 0 (0) 3 (43)

Chapter 5 Discussion

Main findings

The IgNiTE trial was the first ever RCT that aimed to evaluate early IVIG treatment in children with encephalitis, irrespective of cause. IgNiTE failed to meet its primary objective due to recruitment difficulties resulting in a small sample size. The study was halted after recruitment of 18 participants due to withdrawal of funding despite proposed alternative strategies to deliver on the study objectives, using a modified protocol. Alternative funding could not be secured; therefore, the trial was ended.

Due to the small sample size, no group comparisons have been conducted and it is impossible to reach any conclusions regarding the efficacy of IVIG in encephalitis. Thus, we comment only on possible trends seen at data analysis. A summary of participant recruitment and flow through the trial is provided by Figure 2.

Results

Primary outcome

Overall, 50% of participants achieved the primary outcome (i.e. GOS-E Peds score of ≤2 indicating a good recovery) while 28% made a poor recovery, experiencing some degree of disability at 12 months after randomisation. The remaining 22% of participants did not undergo assessment at this timepoint. The proportion of participants who made a good recovery at 12 months after randomisation was the same between the study groups.

Secondary outcomes

Clinical outcomes

The duration of ventilation and length of ICU stay were similar between both groups. Participants in the IVIG group had a longer median hospital stay compared with participants in the control group (12 days vs. 8 days). Overall, 17% of participants had a new diagnosis of epilepsy following the encephalitis illness, with a trend towards a higher proportion in the placebo group than the IVIG group.

Disability assessment

Disability was assessed using the GOS-E Peds and LOS questionnaires. A total of 33% of all participants in the study made full recovery (i.e. LOS of > 4) whereas 44% had minor to severe sequelae (LOS ≤ 4) at 12 months after randomisation, and 22% did not have LOS data collected at this timepoint. When assessed using the GOS-E Peds at 6 months, 44% of all participants made a good recovery (GOS-E peds ≤ 2) while 39% experienced moderate to severe disability (GOS-E peds > 2) and 17% did not undergo a GOS-E Peds assessment at this timepoint. The proportion of participants experiencing neurological sequelae based on both the LOS assessment at 12 months and GOS-E Peds assessment at 6 months tended to be higher in the placebo group compared with the IVIG group.

Assessment of quality of life

There was a trend towards higher PedsQL scores (indicating better quality of life) in participants in the IVIG group compared with those in the placebo group.

Assessment of gross motor functioning

The proportion of participants experiencing impairment of gross motor functioning was generally higher in the IVIG group compared with the placebo group; however, this may be influenced by the high number of participants who did not have this assessment at 4–8 weeks or 12 months post-randomisation (61% and 56%, respectively).

Assessment of adaptive skills

There was a tendency towards a higher proportion of participants with adaptive skills scores close to the average for the normative population in the IVIG group compared with the placebo group. The proportion of participants with scores below the average for the normative population was similar for both the IVIG group and placebo group, although similar data were not available for over half of all participants (56%) which may influence these results.

Assessment of cognitive functioning

This was assessed using various age-appropriate cognitive scales. When the main composite outcomes were assessed, there was a trend towards a higher proportion of participants in the IVIG group with normal level of cognition at 12 months compared with those in the placebo group.

Safety

One participant in the IVIG group experienced an AESI but this was deemed unrelated to the study treatment, No SAEs were reported in the IVIG group compared to ten SAEs reported in three participants in the placebo group. No deaths were recorded in both study groups.

Interpretation

The findings demonstrate that the morbidity from encephalitis is significant with 28–45% of participants experiencing some degree of disability at 12 months after the acute presentation. It appears that encephalitis patients treated with IVIG have a better quality of life experience and a lesser degree of disability than patients not treated with IVIG, although we cannot exclude the potential influence of missing assessments on these results. IVIG (Privigen) has been extensively researched in other patient populations and its side effect profile is well known. There were no safety concerns relating to IVIG in this study.

Lessons learned

IgNiTE was conducted to a high standard and all outcomes were ascertained appropriately. Notwithstanding the challenges with recruitment, there are several lessons to be learned that could be applied to future trials.

One of the challenges encountered was significant delays with site opening. For trials of rare conditions like encephalitis, a multicentre design is crucial to optimise recruitment. Given the broad clinical spectrum of encephalitis, a multicentre approach also ensures that the study population is truly representative of the real-world cohort of patients since recruitment from only large hospitals is likely to select only those patients with severe disease. While trial set-up can be straightforward, particularly at large tertiary or quaternary hospitals with a lot of experience in conducting RCTs, it can be a more challenging process for smaller hospitals with limited prior involvement in research and the site set-up process can be slow. It had been envisaged that by 21 months from commencing the IgNiTE trial, all planned 30 sites would have opened to recruitment but the delays with site opening meant that this was not achieved. For some sites, this was due to non-availability of research nurses, lack of pharmacy capacity, changes to PI, and delays in obtaining research and development approval. For future trials, such delays should be anticipated, and contingency plans made such as extending the study recruitment period, to account for such delays.

We observed a lower than anticipated incidence of encephalitis. At the time that IgNiTE was set up, there were minimal data on the incidence of encephalitis in the UK. Based on previously published UK data, we estimated the number of paediatric admissions to be 2 per year in district general hospitals and 10 per year in tertiary paediatric hospitals. However, our experience was different with a significantly lower number of actual numbers recruited when compared with the estimates, even during the autumn/winter months when the natural peak in incidence is to be expected. One reason for this could be the disparity between the entry criteria used in the study and the more pragmatic but less stringent approach to making a clinical diagnosis of encephalitis. A proposal to mitigate the recruitment challenge encountered in IgNiTE, which included revision to the sample size to allow recruitment of a smaller but adequately powered sample size, extension to the recruitment period and an increase to the number of participating sites was unsuccessful. For large full-scale trials of rare conditions like childhood encephalitis, incorporating a pilot phase with clear feasibility objectives, clear analytical plans and explicit stop-go criteria is likely to enhance the success of such trials. Furthermore, different methodologies should be explored when designing trials of rare diseases, as improvements in biomarkers increasingly enable sub-phenotyping of conditions, thus further reducing individual disease sample sizes.

For trials of a condition like encephalitis for which the clinical presentation can be non-specific, in-depth consideration should be given to the choice of an appropriate entry criteria. Having a robust set of entry criteria provides guidance on eligibility (and) provides homogeneity in the cohort recruited. This enables a clearer definition of the target population that would benefit from IMP if a treatment effect is established, but can limit generalisability of the study findings to the wider patient population. The impact that having very stringent entry criteria could have on recruitment should be considered. In IgNiTE, a strict entry set based on the International Encephalitis Consortium case definition was used since this approach automatically selects a population that provides the best opportunity to observe a treatment effect. However, this case definition, which is intended for use in research trials, differs from the diagnostic approach routinely used in clinical practice where a lower threshold is applied. This meant that some patients who met the threshold for a clinician diagnosis of encephalitis diagnosis did not meet the criteria for entry into the IgNiTE trial or did not do so within the timelines for administering the first dose of study treatment and were therefore excluded. Given the challenges with recruitment, one approach could have been to use a less stringent set of entry criteria. Although this approach might have contributed to increasing recruitment, given the non-specific presentation of encephalitis, it would have encouraged enrolment of patients with an alternative diagnosis which could dilute the true effect of the study treatment. Assessing the impact of using a set of inclusion criteria that slightly differs from what is routinely used in clinical practice could be undertaken in the pilot phase to inform decisions for the larger trial.

A further consideration for any future trials investigating treatments for childhood encephalitis is how best to optimise the consent rate. The immediate period following hospital admission and/or diagnosis of encephalitis is a sensitive one for the family and especially if the child is admitted to the ICU. Therefore, a longer period of time is likely to be required by the family to consider information about the study to allow them to reach a decision regarding participation, particularly for trials involving an IMP. While it is crucial that families are given sufficient time to decide regarding enrolling their child to a research trial, where there is a time window for recruitment, as was the case in IgNiTE, delays in reaching a decision could mean that the patient becomes ineligible. Gaining the trust of parents/guardians and providing them with a reasonable degree of reassurance regarding the safety of trial procedures are important to mitigate such delays. Several ways to achieve this include maintaining clarity and consistency in the message provided to parents/guardians about a study. This can be difficult to achieve especially on the ICU, where there is a high level of patient/family contact with multiple health professionals, some of whom may not have adequate knowledge of the trial or may have individual biases. One strategy could be for families to be approached only by key individuals who not only have an established relationship with the family but also have adequate knowledge of the study. Other strategies could include branding the trial with key, easy-to-understand messages, and the use of informed consent videos to provide clarity and consistency for families. Furthermore, introducing the study in stages is likely to limit information overload for families which could impact on their understanding of the trial and decision to participate. An approach could be to provide families with a shorter version of the participant information sheet which highlights the main aspects of the study followed by the full version alongside having adequate clinical and research staff support for any queries or concerns that may arise.

For a time-sensitive trial like IgNiTE, where the study treatment has to be administered within a specific time window, it is important to have a large pool of site staff who are trained in the study procedures available at all times to ensure that eligible patients are approached in a timely fashion, since delays could result in potential participants becoming ineligible for the study. The experience from the IgNiTE trial was that most ward staff nurses did not have good clinical practice (GCP) training and due to the clinical demands and workload in the NHS, it can be challenging to achieve in-depth full GCP training upfront. In IgNiTE, we took a pragmatic approach and provided face-to-face GCP training for site staff through the use of study specific training slides, which meant that ad hoc training could be provided to staff to enable them carry out specific study tasks during their clinical shift. Further strategies that could be considered include the use of training videos or other virtual training platforms so that the clinical staff are able to complete the relevant training at a convenient time. Ultimately, incorporating GCP into routine clinical staff training will undoubtedly be beneficial and will increase the pool of clinical staff that are available to support research trials.

For any RCT, it is crucial that clinicians are in a state of both clinical and personal equipoise. In IgNiTE, some participants who met the inclusion criteria were excluded due to prior receipt or planned administration of IVIG as part of routine care. This observation suggests an increased willingness of clinicians to administer IVIG to children with encephalitis and possibly a perceived lack of equipoise in the use of IVIG in encephalitis. For future trials, appointing trial ambassadors at each site to emphasise the importance of the study, and continued, active engagement of clinical teams are fundamental.

The use of placebo as the control arm in RCTs investigating medicinal products has become commonplace and is necessary to provide a clear picture regarding the efficacy of the treatment being studied. Consideration should be given to the choice of placebo. For IgNiTE, the placebo that was used was a 0.9% saline and 0.1% human albumin mix. Addition of albumin was deemed necessary to make the placebo visually identical to IVIG. However, this resulted in a considerable reduction in shelf life from 3 years for 0.9% saline to 6 months for the final placebo product, so batch manufacturing of the placebo in alignment with the demand from sites was necessary to minimise wastage. However, with the slow recruitment, there was wastage of stock held at the individual sites. For future trials of rare conditions that involve use of an IMP, having a central hub to hold a small number of the study treatment which can be subsequently dispensed to sites depending on demand, could be considered. The success of such strategy will hugely rely on having a robust IMP management process and establishing effective communication lines between study teams.

Strengths and limitations

ImmunoglobuliN in the Treatment of Encephalitis was the first RCT that aimed to evaluate the efficacy of IVIG in children with encephalitis, irrespective of aetiology. The strengths include the expertise of the trial management team, the robust study design, and the use of validated outcome measures. Furthermore, the trial design and oversight were heavily informed by patient and public involvement and there was a strong focus on equality, diversity and inclusion, with children being actively involved in the consent process.

The major limitation of the study was that it was unable to answer the important question regarding the role of IVIG in the treatment of childhood encephalitis, due to not achieving the anticipated sample size.

Implications for health care

Up to half of children with encephalitis experience short to long-term difficulties and there is the unmet need to identify strategies to improve outcomes. There is strong observational evidence to support a beneficial role of IVIG for some forms of encephalitis. However, further research is required to assess the efficacy of IVIG in the context of childhood encephalitis of all causes.

Results of a recent single-arm open-label trial in adults suggest that IVIG improved neurological function in patients with autoimmune encephalitis,62 and a randomised double-blind placebo-controlled trial evaluating the efficacy of IVIG in autoimmune encephalitis in adults in the UK is now under way. 84 However, it is uncertain whether the findings of these adult trials could be reliably translated to autoimmune encephalitis in children, and it the role of early IVIG treatment in infective encephalitis in children remains unanswered.

Recommendations for research

Further studies are needed to determine the precise role of IVIG in encephalitis, and if a treatment effect is established, ascertain the optimum dose, timing of administration and cost-effectiveness. Recommendations on aspects of trial design, conduct and delivery that could be considered for future trials have been highlighted. Consideration should be given to adopting a multinational approach to support timely trial delivery.

Chapter 6 Conclusions

The IgNiTE trial failed to meet recruitment goals therefore the crucial question about the role of IVIG in encephalitis remains unanswered. Given the cost of IVIG and its scarcity, balanced against the significant morbidity that encephalitis places, it is important to answer this question. Future trials are needed to determine the efficacy of IVIG in childhood encephalitis.

Acknowledgements

The study is supported by the NIHR Biomedical Research Centre, which is based at University of Oxford and was coordinated through the Oxford Vaccine Group, University of Oxford. The authors would like to thank all the participants, families, and healthcare professionals for their involvement in the study. The authors would also like to thank CSL Behring for providing the IVIG and funds for manufacturing the placebo.

Contributions of authors

Mildred A Iro (https://orcid.org/0000-0002-9894-6149) (Clinical Research Fellow) was the lead doctor for the trial and prepared the first version, and had input in the design of the trial.

Manish Sadarangani (https://orcid.org/0000-0002-9985-6452) (Paediatric Infectious Diseases and Immunology doctor) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Michael Absoud (https://orcid.org/0000-0002-0577-1897) (Paediatric Neurologist) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Liberty Cantrell (https://orcid.org/0000-0001-5413-7641) (Statistician) conducted analyses for the trial.

Wui K Chong (https://orcid.org/0000-0002-4335-3864) (Neuroradiologist) is a named investigator on the IgNiTE trial.

Christopher Clark (https://orcid.org/0000-0002-8237-6065) (Professor of Neuroimaging) is a named investigator on the IgNiTE trial.

Ava Easton (https://orcid.org/0000-0002-1739-2915) (Chief Executive of The Encephalitis Society) is a named investigator on the IgNiTE trial.

Victoria Gray (https://orcid.org/0000-0002-5828-6369) (Clinical psychologist) is a named investigator on the IgNiTE trial.

Matilda Hill (https://orcid.org/0000-0002-1566-2512) (Paediatric Clinical Research Fellow) prepared subsequent revisions of the manuscript.

Rachael Kneen (https://orcid.org/0000-0002-8729-4122) (Paediatric Neurologist) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Ming Lim (https://orcid.org/0000-0001-7738-8910) (Paediatric Neurologist) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Xinxue Lu (https://orcid.org/0000-0003-1107-0365) (Statistician) conducted analyses for the trial.

Mike Pike (https://orcid.org/0000-0002-9943-3011) (Paediatric Neurologist) conceptualised the trial and is a named investigator on the IgNiTE trial.

Tom Solomon (https://orcid.org/0000-0001-7266-6547) (Professor of Neurology) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Angela Vincent (https://orcid.org/0000-0003-2395-8695) (Professor of Immunology) is a named investigator on the IgNiTE trial.

Louise Willis (https://orcid.org/0000-0003-3115-5964) (Research Nurse) was the lead nurse for the trial.

Ly-Mee Yu (https://orcid.org/0000-0003-0331-7364) (Statistician) is a named investigator on the IgNiTE trial and had input in the design of the trial.

Andrew J Pollard (https://orcid.org/0000-0001-7361-719X) (Professor of Paediatric Infection and Immunity) conceptualised the trial and is a named investigator on the IgNiTE trial.

All authors contributed significantly to the design of the trial, with specific additional contributions from each co-author within their area of expertise. All authors contributed to the manuscript and have approved the final manuscript for publication.

Ignite Study Team

Trial Management Group

Andrew J Pollard (Chief Investigator), Ming Lim, Tom Solomon, Rachel Kneen, Michael Absoud, Mike Pike, Manish Sadarangani, Wui K Chong, Christopher Clarke, Victoria Gray

Trial coordinating team (Oxford)

Mildred A Iro (Clinical Research Fellow), Louise Willis (Research Nurse/Project Manager), David Kerr, Sophie Bradshaw, Svetlana Mica, Simon Kerridge, Emma Plested, Yama Mujadidi

IMP management

Shakeel Herwitker, Mandy Wan

Trial Steering Committee

Claire Cameron, Ming Lim, Adilia Warris, Federico Martinon-Torres, Mike Bale, Sonia Bale, Alan Percival and Ava Easton

Data Monitoring and Ethics Committee

Chris Warlow (Chairperson), Jo Haviland (statistician), David Pace and Simon Nadel

Statistics team

Ly-Mee Yu, Merryn Voysey, Xinxue Liu, Liberty Cantrell

Laboratory team (Oxford)

Sagida Bibi, Amy Beveridge, Amber Thompson, Daniel O’Connor, Sarosh R Irani, Patrick Waters

Neuropsychological assessment support

Lauren Burke, Victoria Gray

Oxford Vaccine Group

Emma Plested, Parvinder Alley

Recruitment sites

Name of hospital Principal Investigator
Oxford University Hospitals Andrew J Pollard
Great Ormond Street Hospital Sanjay Bhate
Alder Hey Children’s Hospital Rachel Kneen
St George’s Hospital Paul Heath
Barts and the London (Royal London) Anna Riddell
Guy’s and St Thomas’s – Evelina Ming Lim
Sheffield Children’s Hospital Archana Desurkar
NHS Grampian Elma Stephen
Heart of England Steve Welch
Pennine – North Manchester Children’s Hospital Paddy McMaster
Ninewells (Tayside Health Board) Alice Jollands
Royal Hospital for Sick Children, Edinburgh Jay Shetty
University Hospitals Bristol Kayal Vijayakumar
Imperial – St Mary’s Hospital Leena Mewasingh
Nottingham University Hospitals William Whitehouse
Hull Royal Infirmary Vishal Mehta
University Hospitals of North Midland John Alexander
Leeds Teaching Hospital John Livingston
Royal Preston Hospital Christian de Goede
York Teaching Hospital Dominic Smith
Royal Cornwall Hospitals Andrew Collinson

Publications

Hill M, Iro M, Sadarangani M, Absoud M, Cantrell L, Chong K, et al.; IgNiTE study team. Intravenous immunoglobulin treatment in childhood encephalitis (IgNiTE): a randomised controlled trial. BMJ Open. 2023 Nov 9;13(11):e072134. https://doi.org/10.1136/bmjopen-2023-072134. PMID: 37945292; PMCID: PMC10649701.

Funding

This award was funded by the National Institute for Health and Care Research (NIHR) Efficacy and Mechanism Evaluation programme (NIHR award ref: 12/212/15) and is published in full in Efficacy and Mechanism Evaluation; Vol. 11, No. 6. See the NIHR Funding and Awards website for further award information. CSL Behring provided the study IMP (IVIG) and funded manufacture of placebo and the supply and distribution of IMP and placebo through an Interlaken Award to the Chief Investigator.

Data-sharing statement

All data requests should be submitted to the corresponding author for consideration. Access to anonymised data may be granted following review.

Patient data

This work uses data provided by patients and collected by the NHS as part of their care and support. Using patient data is vital to improve health and care for everyone. There is huge potential to make better use of information from people’s patient records, to understand more about disease, develop new treatments, monitor safety, and plan NHS services. Patient data should be kept safe and secure, to protect everyone’s privacy, and it’s important that there are safeguards to make sure that they are stored and used responsibly. Everyone should be able to find out about how patient data are used. #datasaveslives You can find out more about the background to this citation here: https://understandingpatientdata.org.uk/data-citation.

Ethics statement

This IgNiTE trial was conducted in compliance with the principles of the Declaration of Helsinki (1996), in full conformity with the International Conference on Harmonisation of Technical Requirements for Registration of Pharmaceuticals for Human Use (ICH) Guidelines for Good Clinical Practice (CPMP/ICH/135/95 July 1996), the Research Governance Framework and the Medicines for Human Use (Clinical Trial) Regulations 2004. Ethics approval was granted by the UK National Research Ethics Service (NRES) committee on 29 December 2014 (South Central – Oxford A; REC 14/SC/1416). Clinical trial authorisation granted via the Medicines and Healthcare Products Regulatory Agency (MHRA) notification scheme (Ref: 21584/0337/001-0001). Written approval from local Research and Development (R&D) departments at each participating site was obtained before recruitment was commenced at each site.

Information governance statement

The University of Oxford is committed to handling all personal information in line with the UK Data Protection Act (2018) and the General Data Protection Regulation (EU GDPR) 2016/679. Under the Data Protection legislation, the University of Oxford is the Data Controller, and you can find out more about how we handle personal data, including how to exercise your individual rights and the contact details for our Data Protection Officer here https://compliance.admin.ox.ac.uk/contact.

Department of Health and Social Care disclaimer

This publication presents independent research commissioned by the National Institute for Health and Care Research (NIHR). The views and opinions expressed by authors in this publication are those of the authors and do not necessarily reflect those of the NHS, the NIHR, MRC, NIHR Coordinating Centre, the EME programme or the Department of Health and Social Care.

This monograph was published based on current knowledge at the time and date of publication. NIHR is committed to being inclusive and will continually monitor best practice and guidance in relation to terminology and language to ensure that we remain relevant to our stakeholders.

Disclaimer

This manuscript presents independent research. The views and opinions expressed by authors in this publication are those of the authors and do not necessarily reflect those of the NHS, the NIHR, the MRC, the EME programme or the Department of Health and Social Care. If there are verbatim quotations included in this publication the views and opinions expressed by the interviewees are those of the interviewees and do not necessarily reflect those of the authors, those of the NHS, the NIHR, the EME programme or the Department of Health and Social Care.

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Appendix 1 Schedule of visits

T0 T1 T1 + 24h T2 T2 + 24-48h T2 + 7d T3 T4 T5 T6
Eligibility assessment X
Informed consenta X Xb Xb Xb
Confirm consent X X X
Demographics X
Medical history X X X X X X
Obtain relevant clinical information X X X X X X X
Enrolment X Xc
Randomisation X Xc
Scavenged samplesd X X X X X X X X
Additional (research) sample if consent obtained) X Xc X Xc X Xe
Mandatory full blood count Xc,f
Study drug administration and monitoring X X
SAE assessment X X X X X X Xg
Completion of research notes and CRFd X X X X X X X
Questionnaire completions X X X
Research MRI scan (if consent obtained)h X
Neuropsychologist assessment X

FBC, full blood count.

Consent and assent was obtained from all participants when clinically appropriate during the study.

Participant consent (if 16 years and if not previously obtained).

Where not previously done.

Identification of scavenged samples and entry of clinical information into the research notes and CRF was an ongoing process that occured throughout the study. As appropriate, any required information was entered as soon as they became available.

To avoid an extra visit solely for this purpose, the ‘6 month research sample’ could have been obtained at any routine follow up clinical appointments that occured after the participant had been discharged.

Where a participant was transferred to a non-IgNiTE participating hospital before this time point, a recommendation was made for the FBC to be done at the receiving hospital. If the transfer occured after the first dose of the study drug had been given and before the second dose was due, the recommendation was that the FBC was done at 24–48 hours after the first dose.

Only deaths, serious adverse reactions and pregnancies required reporting beyond 6 months post randomisation.

May not have been required if a routine follow up MRI scan was planned, depending on timing of this. See Radiological evaluation

Note

See Study design for timelines. Baseline research sample could be obtained at either T0 or T1 while the T1 + 24 h blood sample could be obtained just before the 2nd dose of the study drug if this is being given at 24 hours after the first dose.

Appendix 2 Recruiting hospital sites, duration they were open and estimate vs. actual recruitment

Site Number of whole months open Estimated recruitment for number of months open Actual recruitment
Oxford University Hospitals 21 7–8 3
Great Ormond Street Hospital 19 2–3 1
Alder Hey Children’s Hospital 18 11–12 3
St George’s Hospital 18 4–5 1
Barts and the London (Royal London) 17 2–3 0
Guy’s and St Thomas’s – Evelina 16 10–11 2
Sheffield Children’s Hospital 16 1–2 1
NHS Grampian 16 4–5 2
Heart of England 16 3–4 1
Pennine – North Manchester Children’s Hospital 15 4–5 1
Ninewells (Tayside Health Board) 15 0–1 0
Royal Hospital for Sick Children, Edinburgh 14 2–3 0
University Hospitals Bristol 13 3–4 0
Imperial – St Mary’s Hospital 11 5–6 1
Nottingham University Hospitals 11 1–2 1
Hull Royal Infirmary 7 1–2 1
University Hospitals of North Midland 6 1–2 0
Leeds Teaching Hospital 6 2–3 0
Royal Preston Hospital 5 0–1 0
York Teaching Hospital 4 0–1 0
Royal Cornwall Hospitals 2 1–2 0

Appendix 3 Hospital sites intended to be opened, site opening times and date of first recruitment across sites

No. Site SIV date Date opened Date of 1st recruit
01 Oxford University Hospitals 26 August 2015 23 December 2015 24 February 2016
02 Guy’s and St Thomas’s – Evelina 6 October 2015 19 May 2016 30 November 2016
03 St George’s Hospital 12 October 2015 22 May 2016 27 October 2016
04 Alder Hey Children’s Hospital 16 November 2015 30 March 2016 19 May 2017
05 University Hospitals Bristol 24 November 2015 25 August 2016 N/A
06 North Manchester Children’s Hospital 30 November 2015 30 June 2016 19 May 2017
07 University Hospital Southampton 10 December 2015 N/A N/A
08 Great Ormond Street Hospital 14 December 2015 1 March 2016 21 September 2016
09 Barts and the London (Royal London) 15 January 2016 4 May 2016 N/A
10 Sheffield Children’s Hospital 14 January 2016 26 May 2016 25 May 2017
11 NHS Grampian 24 February 2016 7 June 2016 24 November 2016
12 Ninewells (Tayside Health Board) 25 February 2016 17 June 2016 N/A
13 Heart of England 2 March 2016 1 June 2016 15 February 2017
14 South Tees – James Cook Hospital 7 March 2016 N/A N/A
15 Birmingham Children’s Hospital 21 March 2016 N/A N/A
16 Royal Hospital for Sick Children, Edinburgh 21 April 2016 22 July 2016 N/A
17 Imperial – St Mary’s Hospital 20 June 2016 11 October 2016 13 February 2017
18 Cambridge – Addenbrooke’s 9 August 2016 N/A N/A
19 Nottingham University Hospitals 1 September 2016 7 November 2016 22 November 2016
20 University Hospitals of North Midland 19 September 2016 9 March 2017 N/A
21 Hull Royal Infirmary 27 October 2016 9 February 2017 27 February 2017
22 Leeds Teaching Hospital 24 October 2016 16 March 2017 N/A
23 York Teaching Hospital 31 October 2016 11 May 2017 N/A
24 Central Manchester University Hospital 29 November 2016 N/A N/A
25 Royal Cornwall Hospitals 15 December 2016 18 July 2017 N/A
26 Royal Preston Hospital 26 January 2017 13 April 2017 N/A
27 Leicester Royal Infirmary 22 August 2017 N/A N/A
28 Royal Berkshire Hospital 09 June 2017 N/A N/A
29 Royal Exeter and Devon 30 June 2017 N/A N/A

SIV, site initiation visit.

List of abbreviations

ABAS-II
Adaptive Behaviors Assessment System-Second Edition
ADEM
acute demyelinating encephalomyelitis
AE
adverse event
AESI
adverse event of special interest
AR
adverse reaction
CI
chief investigator
CONSORT
Consolidated Standards of Reporting Trials
CRF
case report form
CSF
cerebrospinal fluid
CT
clinical trials
FSIQ
Full-Scale IQ
GCP
good clinical practice
GMFCS
gross motor function classification system
GOS-E
Glasgow Outcome Scale-Extended
ICH
international conference of harmonisation
ICU
intensive care unit
ID
identification
IgNiTE
ImmunoglobuliN in the Treatment of Encephalitis
IMP
investigational medicinal product
ITT
intention-to-treat
IVIG
intravenous immunoglobulin
IQR
interquartile range
JE
Japanese encephalitis
LOS
Liverpool Outcome Score
MHRA
Medicines and Healthcare products Regulatory Agency
MRI
magnetic resonance imaging
MOG
myelin oligodendrocyte glycoprotein
NHS
National Health Service
NIHR
National Institute for Health and Care Research
NMDAR
N-methyl-D-aspartate receptor
NRES
National Research Ethics Service
PedsQL
Paediatric Quality of Life
PI
principal investigator
PRI
Perceptual Reasoning Index
PSI
Processing Speed Index
RCT
Randomised controlled trial
REC
Research Ethics Committee
SAE
serious adverse event
SAR
serious adverse reaction
SDQ
Strengths and Difficulties Questionnaire
TMF
trial master file
TSC
Trial Steering Committee
VCI
Verbal Comprehension Index
VSI
Visual Spatial Index
WCC
white cell count
WMI
working memory index

Encephalitis (inflammation of the brain) is a serious but rare condition affecting approximately 5 in 100,000 children in England. Encephalitis can have a big impact on affected children and their families. Approximately 12 out of 100 affected children will die and half of those that survive experience varying difficulties in the long term; these might include problems with memory, physical disabilities, seizures and changes in how they think and behave.

There is some evidence that a treatment called intravenous immunoglobulin may benefit people affected by encephalitis. Intravenous immunoglobulin contains antibodies obtained from blood donations by different people, which is used to treat some types of inflammation. However, there have been no research studies investigating the effect of intravenous immunoglobulin when used in large numbers of children with all types of encephalitis. Furthermore, although intravenous immunoglobulin is sometimes used to treat children with encephalitis, it is often given after other treatments have been unsuccessful. Outcomes from encephalitis are determined largely by the amount of brain inflammation; it would therefore seem logical that giving a treatment early in the illness to limit the inflammation would be beneficial.

In the ImmunoglobuliN in the Treatment of Encephalitis study, we aimed to find out whether giving intravenous immunoglobulin to children with encephalitis early in the illness can help them get better more quickly and reduce the difficulties they experience later on. Half of the children in the trial received intravenous immunoglobulin and the other half received an inactive medicine, known as placebo, in addition to the normal care they would receive in a hospital. We aimed to compare the recovery and outcomes between children in these two groups.

This trial was stopped early due to withdrawal of funding, as fewer children than expected were enrolled into the study. Too few children were enrolled for us to be sure whether intravenous immunoglobulin benefits children with encephalitis. However, the trial findings highlight the impact of encephalitis on affected children, with around half of children demonstrating ongoing difficulties 1 year after the illness.

Background

There is significant mortality and morbidity from encephalitis in children despite the current standard of care. Thus, strategies to improve outcomes in patients with encephalitis are urgently required.

Theoretical and empirical evidence suggest a beneficial role of intravenous immunoglobulin (IVIG) for viral and auto-immune forms of encephalitis. Therefore, we set up a prospective randomised controlled trial (RCT) to ascertain the efficacy of early IVIG treatment for all-cause encephalitis in children.

In the study, children with encephalitis were randomised to receive two doses of either IVIG or placebo within five working days from the suspicion of an encephalitis diagnosis, in addition to normal standard of care. They were then followed up for 12 months after randomisation.

We hypothesised that IVIG could have therapeutic benefit for children with encephalitis when administered early in the illness.

Objectives

The primary objective was to evaluate the efficacy of early IVIG treatment in childhood encephalitis. This was assessed by comparing the proportion of children in the 2 treatment groups who made good recovery, assessed using the paediatric version of the Glasgow outcome score extended, at 12 months after randomisation.

The secondary objectives were to: (1) compare clinical, neurological, neuroimaging and neuropsychological outcomes between the treatment groups, (2) evaluate the proportion of participants with autoimmune encephalitis and (3) confirm the safety of IVIG.

Methods

Trial design

This was a phase 3b multicentre, double-blind, randomised, placebo-controlled trial to evaluate the early use IVIG in childhood encephalitis.

Setting

Participants were recruited from 21 NHS Hospitals in the UK.

Participants

Inclusion criteria

Participants were eligible if

  • they were aged between 6 weeks and 16 years

  • they met the case definition for possible encephalitis based on the International Encephalitis Consensus

  • parents/guardians provided written informed consent, or assent if appropriate.

Exclusion criteria

The exclusion criteria included: (1) a high clinical suspicion of bacterial meningitis, (2) prior receipt of IVIG during the admission or known contraindication to IVIG, (3) traumatic brain injury, (4) history of metabolic encephalopathy, stroke, toxic or hypertensive encephalopathy, (5) pre-existing demyelinating disorder, (6) significant renal impairment, (7) hypercoagulable state, (8) hyperprolinaemia, (9) participation in another research trial involving an immunomodulatory treatment, (10) known to be pregnant, (11) any significant disease or clinical research that would impact on participation, or interfere with compliance with study requirements.

Randomisation

Participants were randomly assigned 1 : 1 ratio to receive 2 doses (1 g/kg/dose) of either IVIG or matching placebo, in addition to standard care. Randomisation was stratified by age and receipt of steroid treatment.

Interventions

Two doses of 1 g/kg/dose of either IVIG or a matching volume of placebo were given 24–36 hours apart, with the first dose administered as soon as possible after enrolment and within five working days from the suspicion of an encephalitis diagnosis.

The active treatment (IVIG) used in the study was Privigen (100 mg/ml solution), manufactured and provided by CSL Behring. The placebo was a mixture of 0.9% saline + 0.1% human albumin solution, manufactured at the Royal Broadgreen and Liverpool Aseptic Production Unit, Liverpool, UK, under current good manufacturing practice conditions and its Manufacturer’s Importer’s Authorisation licence. The addition of albumin to saline was necessary to make the placebo visually identical to IVIG.

Blinding

Participants, treating clinicians, parents/guardians and outcome assessors were blinded to the allocated treatment.

Primary outcome

The primary outcome was good recovery (i.e. score of ≤2) on the paediatric version of the Glasgow Outcome Score-Extended (GOS-E Peds) at 12 months after randomisation.

Secondary outcomes

Clinical, neurological and neuropsychological outcomes

Multiple clinical and neurological measures were collected during the hospital admission, at 4–8 weeks after discharge from acute care, and at 6 and 12 months after randomisation. A blinded neuropsychologist assessment of cognitive function was carried out at 12 months after randomisation.

Radiological outcomes

Brain magnetic resonance imaging (MRI) findings at 6 months after randomisation were compared with imaging results obtained during the acute illness.

Safety data

Safety and adverse events (AEs) data were collected until 12 months after randomisation.

Identification of immune-mediated encephalitis

Presence of specific auto-antibodies in serum was assessed.

Statistical methods

The analyses were performed on the intention-to-treat population; this included all participants who were randomised, irrespective of study treatment received. In the analysis of the AEs, all participants who received study treatment were included. Since 20% of participants were recruited before the trial was halted, all analyses are descriptive.

Results

Recruitment took place between 23 December 2015 and 26 September 2017. Recruitment was paused in September 2017 following withdrawal of funding due to slower than anticipated recruitment. Despite strategies implemented to improve recruitment, funding was not reinstated. Attempts at securing alternative funding were unsuccessful; therefore, the trial was closed on 24 October 2017.

Participants and demographics

At the time of halting the study, 18 participants had been randomised (IVIG n = 10; placebo n = 8). One participant each from the IVIG and placebo groups were withdrawn from the study before receipt of study treatment and one participant in the placebo arm refused a second dose of study treatment. Therefore 16 participants (IVIG n = 9; placebo n = 7) received at least one dose of the study treatment and 15 participants (IVIG n = 9, placebo n = 6) received two full doses of the study treatment.

One participant in the placebo group was lost to follow up after the 6 months visit and 1 participant in the IVIG group withdrew consent prior to the visit 12 months after randomisation.

The median age at randomisation was 4.09 years [interquartile range (IQR) = 2.0–11.8], 44% were male and 89% were of white ethnicity. Baseline characteristics were well matched across treatment arms.

Primary outcome

At 12 months after randomisation, 9 participants [50%; IVIG n = 5 (50%); placebo n = 4 (50%)] made a good recovery (score ≤2 on the GOS-E Peds) and 5 participants [28%; IVIG n = 3 (30%), placebo n = 2 (25%)] made a poor recovery (score > 2). Four participants (22%; IVIG n = 2 (20%), placebo n = 2 (25%)] did not undergo a GOS-E Peds assessment at 12 months after randomisation.

Secondary outcomes

Inpatient data

Ten participants [56%; IVIG n = 5 (50%), placebo = 5 (63%)] were admitted to intensive care, and nine of these [90%; IVIG n = 4 (80%), placebo n = 5(100%)] required invasive ventilation, for a median duration of two days (IQR 2.0–3.0). The median length of stay on intensive care was 4.5 days (3.0–6.8) and the overall median length of hospitalisation for acute care was 11 days (7.8–19.5).

Epilepsy diagnosis

Three participants [17%; IVIG n = 1 (10%), placebo n = 2 (25%)] had a new diagnosis of epilepsy during the study period. Five participants [28%; IVIG n = 2 (20%), placebo n = 3 (38%)] had incomplete data for this outcome.

Glasgow Outcome Score-Extended-Peds at 6 months after randomisation

Eight participants [44%; IVIG n = 4 (40%), placebo n = 4 (50%)] made a good recovery at 6 months after randomisation, whereas seven participants [39%; IVIG n = 4 (50%), placebo n = 3 (38%)] made a poor recovery. Three participants [17%; IVIG n = 2 (20%), placebo n = 1 (13%)] did not undergo a GOS-E Peds assessment at 6 months after randomisation.

Liverpool outcome score

At 4–8 weeks after discharge from acute care, 5 participants [28%; IVIG n = 3 (30%), placebo n = 2 (25%)] made a full recovery [defined as a Liverpool Outcome Score (LOS) of >4], whereas 10 participants [56%; IVIG n = 5 (50%), placebo n = 5 (63%)] had minor to severe sequelae. Three participants [17%; IVIG n = 2 (20%); placebo n = 1 (13%)] did not have LOS data collected at this timepoint.

At 12 months after randomisation, six participants [33%; IVIG n = 4 (40%), placebo n = 2 (25%)] made full recovery on the LOS assessment, while 8 participants [44%; IVIG n = 4 (40%), placebo n = 4 (50%)] reported minor to severe sequelae. Four participants [22%; IVIG n = 2 (20%); placebo n = 2 (25%)] did not have LOS data collected at this timepoint.

Paediatric quality of life assessment

Paediatric quality of life scores were available for seven participants [39%; IVIG n = 5 (50%), placebo n = 2 (25%)] at 4–8 weeks after discharge from acute care and for eight participants [44%; IVIG n = 6 (60%), placebo n = 2 (25%)] at 12 months post randomisation.

At 4–8 weeks after discharge from acute care, the mean PedsQL score was 77.9 (standard deviation, SD, 11.10) and 56.5 (SD 7.8) for the IVIG and placebo group, respectively. At 12 months, mean PedsQL scores were 79.9 (SD 21.6) and 63.7 (SD 30.1) for the IVIG and placebo groups, respectively.

Gross motor function classification system

At 4–8 weeks after discharge from acute care, seven participants [39%; IVIG n = 5 (50%); placebo n = 2 (25%)] had mild impairment of gross motor functioning. These data were not available for 11 participants [61%; IVIG n = 5 (50%), placebo n = 6 (75%)] at this timepoint.

At 12 months after randomisation, eight participants [44%; IVIG n = 6 (60%); placebo n = 2 (25%)] experienced mild or severe impairment of gross motor function. These data were not available for ten participants [56%; IVIG n = 4 (40%), placebo n = 6 (75%)] at this timepoint.

Strengths and difficulties assessment

Strengths and Difficulties Questionnaire (SDQ) results were available for seven participants (IVIG n = 5, placebo n = 2) at 4–8 weeks after discharge from acute care and eight participants (IVIG n = 6, placebo n = 2) at 12 months after randomisation.

At 4–8 weeks after discharge from acute care, five participants [28%; IVIG n = 4 (40%); placebo n = 1 (13%)] had a close to average SDQ score, one participant [6%, IVIG n = 1 (10%), placebo n = 0] had a slightly raised SDQ score and one participant [6%, IVIG n = 0, placebo n = 1 (13%)] had a very high SDQ score.

At 12 months after randomisation, the same number of participants had a close to average score and slightly raised score, but two participants [11%; IVIG n = 1 (10%), placebo n = 1 (13%)] had a very high SDQ score.

Adaptive Behaviors Assessment System – second edition

At 4–8 weeks after discharge from acute care, five participants [28%; IVIG n = 4 (40%), placebo n = 1 (13%)] had an Adaptive Behaviors Assessment System-second edition (ABAS-II) score that was either similar or higher than the average score of the normative population. At the same time point, three participants [17%; IVIG n = 2 (20%), placebo n = 1 (13%)] had a score that was lower than the average score. Ten participants [56%; IVIG n = 4 (40%), placebo n = 6 (75%)] did not have ABAS-II assessment at this timepoint.

At 12 months after randomisation, the same number of participants had a score that was below the average, but four participants [22%; IVIG n = 3 (30%), placebo n = 1 (13%)] had a score that was either similar or higher than the average score, and 11 participants [61%; IVIG n = 5 (50%), placebo n = 6 (75%)] did not have ABAS-II assessment at this timepoint.

Neuropsychology assessment

Thirteen participants (72%; IVIG n = 8 (80%); placebo n = 5 (63%)] had blinded neuropsychology assessment at 12 months after randomisation; four [30%; IVIG n = 2 (25%), placebo n = 2 (40%)] of these participants were unable to complete the full battery of assessments due to attention or behavioural needs. Five participants [28%; IVIG n = 2 (20%), placebo n = 3 (38%)] did not undergo neuropsychology assessment.

Five participants [28%; IVIG n = 4 (40%), placebo n = 1 (13%)] had a score of ≥85 (indicating normal development) for Full-Scale IQ, six [33%; IVIG n = 4 (40%); placebo n = 2 (25%)] for Verbal Comprehension Index (VCI), five [28%; IVIG n = 4 (40%), placebo n = 1 (13%)] for visual spatial; four [22%; IVIG n = 4 (40%), placebo n = 0 (0%)] for working memory index (WMI); and four [22%; IVIG n = 3 (30%); placebo n = 1 (13%)] for Perceptual Reasoning Index (PRI). Two participants (one in each treatment arm) were assessed using the Bayley scale of infant and toddler development, one participant (IVIG arm) had severe neurodevelopmental impairment while the other (placebo arm) had a normal neurodevelopmental outcome.

Neuroimaging

Nineteen acute neuroimaging scans were available for 13 participants. Five scans (for five unique participants) had abnormal findings; all of these were MRI scans. Four of the abnormal scans showed bilateral lesions. There were nine follow-up scans for eight unique participants of which six scans (for five unique participants) were normal and unchanged from the acute scan. Three follow-up scans (for three unique participants) had abnormal findings; two of these were unchanged from the acute scans and an acute scan was not available for comparison one participant.

Autoantibody testing

Twelve participants had autoantibody testing. One participant (placebo n = 1) was positive for LGI1 antibodies, and one participant (placebo n = 1) was positive for myelin oligodendrocyte glycoprotein (MOG) antibodies. Two additional participants (IVIG n = 2) were positive for IgG to live neurons, indicating the presence of IgG antibodies binding to neurons, but negative for antibodies to the specific antigens tested for in the study.

Safety reporting

One participant in the IVIG group reported an AE of special interest; the participant developed a fever during IVIG infusion; however, this was judged to be unrelated to the study treatment. Ten serious AEs occurred in three participants in the placebo group and none in the IVIG group. None of the serious adverse events (SAEs) were judged to be related to the study treatment. No deaths occurred during the study period.

Conclusions

ImmunoglobuliN in the Treatment of Encephalitis (IgNiTE) was the first RCT to prospectively evaluate the efficacy of IVIG in childhood encephalitis. It was anticipated that data from IgNiTE would provide definitive evidence on which to base the management of children with encephalitis in the UK and worldwide. However, due to slow recruitment, the trial was terminated early. Therefore, the trial did not reach its pre-determined sample size and was underpowered, making it impossible to reach a conclusion on the role of IVIG in treatment of childhood encephalitis.

Nonetheless, IgNiTE has highlighted several key learning points. Firstly, IgNiTE has demonstrated the feasibility of setting up a large multi-centre trial efficacy trial in a cohort of children with a rare condition such as encephalitis. Secondly, data from IgNiTE, albeit derived from a small sample size, suggest the safety of IVIG and provide some insight into the burden that encephalitis places on children and the NHS. Over half of the study participants were admitted to the intensive care unit with 90% of those admitted requiring invasive ventilation, with a prolonged overall length of hospitalisation. In addition, a notable proportion of children experienced some degree of disability at follow-up, highlighting the need to prioritise studies aimed at identifying strategies to alleviate the burden from this rare but debilitating disease.

For future studies aimed at addressing the efficacy of early IVIG treatment in childhood encephalitis, consideration should be given to practical challenges with setting up RCTs for rare diseases. These include the necessity to recruit from multiple sites to achieve the sample size, the importance of clinical equipoise amongst treating clinicians, and the trade-off between having a stringent but robust set of entry criteria and the impact of this on recruitment.

Trial registration

This trial is registered as Clinical Trials.gov (NCT02308982) and ISRCTN15791925.

Funding

This award was funded by the National Institute for Health and Care Research (NIHR) Efficacy and Mechanism Evaluation (EME) programme (NIHR award ref: 12/212/15) and is published in full in Efficacy and Mechanism Evaluation; Vol. 11, No. 6. See the NIHR Funding and Awards website for further award information.

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