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Meta-Analysis
.2021 Jun 16;6(6):CD003031.
doi: 10.1002/14651858.CD003031.pub4.

Prophylactic drug management for febrile seizures in children

Affiliations
Meta-Analysis

Prophylactic drug management for febrile seizures in children

Martin Offringa et al. Cochrane Database Syst Rev..

Abstract

Background: Febrile seizures occurring in a child older than one month during an episode of fever affect 2-4% of children in Great Britain and the United States and recur in 30%. Rapid-acting antiepileptics and antipyretics given during subsequent fever episodes have been used to avoid the adverse effects of continuous antiepileptic drugs. This is an updated version of a Cochrane Review previously published in 2017.

Objectives: To evaluate primarily the effectiveness and safety of antiepileptic and antipyretic drugs used prophylactically to treat children with febrile seizures; and also to evaluate any other drug intervention where there is a sound biological rationale for its use.

Search methods: For the latest update we searched the following databases on 3 February 2020: Cochrane Register of Studies (CRS Web), MEDLINE (Ovid, 1946 to 31 January 2020). CRS Web includes randomised or quasi-randomised controlled trials from PubMed, Embase, ClinicalTrials.gov, the World Health Organization International Clinical Trials Registry Platform (ICTRP), the Cochrane Central Register of Controlled Trials (CENTRAL), and the specialised registers of Cochrane Review Groups including the Cochrane Epilepsy Group. We imposed no language restrictions and contacted researchers to identify continuing or unpublished studies.

Selection criteria: Trials using randomised or quasi-randomised participant allocation that compared the use of antiepileptics, antipyretics or recognised Central Nervous System active agents with each other, placebo, or no treatment.

Data collection and analysis: For the original review, two review authors independently applied predefined criteria to select trials for inclusion and extracted the predefined relevant data, recording methods for randomisation, blinding, and exclusions. For the 2016 update, a third review author checked all original inclusions, data analyses, and updated the search. For the 2020 update, one review author updated the search and performed the data analysis following a peer-review process with the original review authors. We assessed seizure recurrence at 6, 12, 18, 24, 36, 48 months, and where data were available at age 5 to 6 years along with recorded adverse effects. We evaluated the presence of publication bias using funnel plots.

Main results: We included 42 articles describing 32 randomised trials, with 4431 randomised participants used in the analysis of this review. We analysed 15 interventions of continuous or intermittent prophylaxis and their control treatments. Methodological quality was moderate to poor in most studies. We found no significant benefit for intermittent phenobarbital, phenytoin, valproate, pyridoxine, ibuprofen, or zinc sulfate versus placebo or no treatment; nor for diclofenac versus placebo followed by ibuprofen, paracetamol, or placebo; nor for continuous phenobarbital versus diazepam, intermittent rectal diazepam versus intermittent valproate, or oral diazepam versus clobazam. There was a significant reduction of recurrent febrile seizures with intermittent diazepam versus placebo or no treatment at six months (risk ratio (RR) 0.64, 95% confidence interval (CI) 0.48 to 0.85; 6 studies, 1151 participants; moderate-certainty evidence), 12 months (RR 0.69, 95% CI 0.56 to 0.84; 8 studies, 1416 participants; moderate-certainty evidence), 18 months (RR 0.37, 95% CI 0.23 to 0.60; 1 study, 289 participants; low-certainty evidence), 24 months (RR 0.73, 95% CI 0.56 to 0.95; 4 studies, 739 participants; high-certainty evidence), 36 months (RR 0.58, 95% CI 0.40 to 0.85; 1 study, 139 participants; low-certainty evidence), 48 months (RR 0.36, 95% CI 0.15 to 0.89; 1 study, 110 participants; moderate-certainty evidence), with no benefit at 60 to 72 months (RR 0.08, 95% CI 0.00 to 1.31; 1 study, 60 participants; very low-certainty evidence). Phenobarbital versus placebo or no treatment reduced seizures at six months (RR 0.59, 95% CI 0.42 to 0.83; 6 studies, 833 participants; moderate-certainty evidence), 12 months (RR 0.54, 95% CI 0.42 to 0.70; 7 studies, 807 participants; low-certainty evidence), and 24 months (RR 0.69, 95% CI 0.53 to 0.89; 3 studies, 533 participants; moderate-certainty evidence), but not at 18 months (RR 0.77, 95% CI 0.56 to 1.05; 2 studies, 264 participants) or 60 to 72 months follow-up (RR 1.50, 95% CI 0.61 to 3.69; 1 study, 60 participants; very low-certainty evidence). Intermittent clobazam compared to placebo at six months resulted in a RR of 0.36 (95% CI 0.20 to 0.64; 1 study, 60 participants; low-certainty evidence), an effect found against an extremely high (83.3%) recurrence rate in the controls, a result that needs replication. When compared to intermittent diazepam, intermittent oral melatonin did not significantly reduce seizures at six months (RR 0.45, 95% CI 0.18 to 1.15; 1 study, 60 participants; very-low certainty evidence). When compared to placebo, intermittent oral levetiracetam significantly reduced recurrent seizures at 12 months (RR 0.27, 95% CI 0.15 to 0.52; 1 study, 115 participants; very low-certainty evidence). The recording of adverse effects was variable. Two studies reported lower comprehension scores in phenobarbital-treated children. Adverse effects were recorded in up to 30% of children in the phenobarbital-treated groups and 36% in benzodiazepine-treated groups. We found evidence of publication bias in the meta-analyses of comparisons for phenobarbital versus placebo (seven studies) at 12 months but not at six months (six studies); and valproate versus placebo (four studies) at 12 months. There were too few studies to identify publication bias for the other comparisons. The methodological quality of most of the included studies was low or very low. Methods of randomisation and allocation concealment often did not meet current standards, and 'treatment versus no treatment' was more commonly seen than 'treatment versus placebo', leading to obvious risks of bias. AUTHORS' CONCLUSIONS: We found reduced recurrence rates for intermittent diazepam and continuous phenobarbital, with adverse effects in up to 30% of children. The apparent benefit for clobazam treatment in one trial needs to be replicated. Levetiracetam also shows benefit with a good safety profile; however, further study is required. Given the benign nature of recurrent febrile seizures, and the high prevalence of adverse effects of these drugs, parents and families should be supported with adequate contact details of medical services and information on recurrence, first aid management, and, most importantly, the benign nature of the phenomenon.

Copyright © 2021 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.

PubMed Disclaimer

Conflict of interest statement

Martin Offringa: none known.

Richard Newton was one of the investigators of the included study (McKinlay 1989). He did not take part in the study selection, data extraction and risk of bias assessment stages for that study.

Sarah Nevitt: none known.

Katerina Vraka: none known.

Figures

1
1
Study flow diagram.
2
2
Risk of bias summary: review authors' judgements about each risk of bias item for each included study.
3
3
Funnel plot of comparison: 1 Intermittent oral or rectal diazepam versus placebo or no treatment to recurrence at 6 months.
4
4
Funnel plot of comparison: 1 Intermittent oral or rectal diazepam versus placebo or no treatment to recurrence at 12 months.
5
5
Funnel plot of comparison 2: Continuous phenobarbital versus placebo or no treatment to recurrence at 6 months: no evidence of publication bias.
6
6
Funnel plot of comparison 2: Continuous phenobarbital versus placebo or no treatment to recurrence at 12 months: evidence of publication bias.
7
7
Seizure recurrence in the control groups of the included trials; red lines indicate median recurrence rates at each time point, by control group type.
1.1
1.1. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 1: Recurrent seizure @ 6 months
1.2
1.2. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 2: Recurrent seizure @ 12 months
1.3
1.3. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 3: Recurrent seizure @ 18 months
1.4
1.4. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 4: Recurrent seizure @ 24 months
1.5
1.5. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 5: Recurrent seizure @ 36 months
1.6
1.6. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 6: Recurrent seizure @ 48 months
1.7
1.7. Analysis
Comparison 1: Intermittent oral or rectal diazepam compared to placebo or no treatment, Outcome 7: Recurrent seizure @ 60 to 72 months
2.1
2.1. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 1: Recurrent seizure @ 6 months
2.2
2.2. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 2: Recurrent seizure @ 12 months
2.3
2.3. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 3: Recurrent seizure @ 18 months
2.4
2.4. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 4: Recurrent seizure @ 24 months
2.5
2.5. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 5: Recurrent seizure @ 60 to 72 months
2.6
2.6. Analysis
Comparison 2: Continuous phenobarbital compared to placebo or no treatment, Outcome 6: Behavioural changes
3.1
3.1. Analysis
Comparison 3: Intermittent phenobarbital compared to placebo or no treatment, Outcome 1: Recurrent seizure @ 6 months
3.2
3.2. Analysis
Comparison 3: Intermittent phenobarbital compared to placebo or no treatment, Outcome 2: Recurrent seizure @ 12 months
3.3
3.3. Analysis
Comparison 3: Intermittent phenobarbital compared to placebo or no treatment, Outcome 3: Recurrent seizure @ 24 months
3.4
3.4. Analysis
Comparison 3: Intermittent phenobarbital compared to placebo or no treatment, Outcome 4: Recurrent seizure @ 60 to 72 months
4.1
4.1. Analysis
Comparison 4: Continuous oral phenytoin compared to placebo, Outcome 1: Recurrent seizure @ 12 months
5.1
5.1. Analysis
Comparison 5: Continuous oral valproate compared to placebo or no treatment, Outcome 1: Recurrent seizure @ 6 months
5.2
5.2. Analysis
Comparison 5: Continuous oral valproate compared to placebo or no treatment, Outcome 2: Recurrent seizure @ 12 months
5.3
5.3. Analysis
Comparison 5: Continuous oral valproate compared to placebo or no treatment, Outcome 3: Recurrent seizure @ 18 months
5.4
5.4. Analysis
Comparison 5: Continuous oral valproate compared to placebo or no treatment, Outcome 4: Recurrent seizure @ 24 months
6.1
6.1. Analysis
Comparison 6: Continuous oral pyridoxine compared to placebo, Outcome 1: Recurrent seizure @ 6 months
6.2
6.2. Analysis
Comparison 6: Continuous oral pyridoxine compared to placebo, Outcome 2: Recurrent seizure @ 12 months
7.1
7.1. Analysis
Comparison 7: Intermittent oral ibuprofen compared to placebo, Outcome 1: Recurrent seizure @ 6 months
7.2
7.2. Analysis
Comparison 7: Intermittent oral ibuprofen compared to placebo, Outcome 2: Recurrent seizure @ 12 months
7.3
7.3. Analysis
Comparison 7: Intermittent oral ibuprofen compared to placebo, Outcome 3: Recurrent seizure @ 24 months
8.1
8.1. Analysis
Comparison 8: Intermittent oral clobazam compared to placebo, Outcome 1: Recurrent seizure @ 6 months
9.1
9.1. Analysis
Comparison 9: Continuous zinc sulfate for 6 months compared to placebo, Outcome 1: Recurrent seizure @ 12 months
10.1
10.1. Analysis
Comparison 10: Intermittent rectal diclofenac compared to placebo followed by oral ibuprofen, paracetamol, or placebo after 8 hours, Outcome 1: Recurrent seizure @ 6 months
10.2
10.2. Analysis
Comparison 10: Intermittent rectal diclofenac compared to placebo followed by oral ibuprofen, paracetamol, or placebo after 8 hours, Outcome 2: Recurrent seizure @ 12 months
10.3
10.3. Analysis
Comparison 10: Intermittent rectal diclofenac compared to placebo followed by oral ibuprofen, paracetamol, or placebo after 8 hours, Outcome 3: Recurrent seizure @ 18 months
10.4
10.4. Analysis
Comparison 10: Intermittent rectal diclofenac compared to placebo followed by oral ibuprofen, paracetamol, or placebo after 8 hours, Outcome 4: Recurrent seizure @ 24 months
11.1
11.1. Analysis
Comparison 11: Continuous phenobarbital compared to intermittent rectal or oral diazepam, Outcome 1: Recurrent seizure @ 12 months
11.2
11.2. Analysis
Comparison 11: Continuous phenobarbital compared to intermittent rectal or oral diazepam, Outcome 2: Recurrent seizure @ 18 months
12.1
12.1. Analysis
Comparison 12: Intermittent rectal diazepam compared to intermittent rectal valproate, Outcome 1: Recurrent seizure @ 6 months
12.2
12.2. Analysis
Comparison 12: Intermittent rectal diazepam compared to intermittent rectal valproate, Outcome 2: Recurrent seizure @ 12 months
13.1
13.1. Analysis
Comparison 13: Intermittent oral diazepam compared to oral clobazam, Outcome 1: Recurrent seizure @ 12 months
14.1
14.1. Analysis
Comparison 14: Intermittent oral melatonin compared to intermittent oral diazepam, Outcome 1: Recurrent seizure @ 6 months
15.1
15.1. Analysis
Comparison 15: Intermittent oral levetiracetam compared to placebo (any antipyretics), Outcome 1: Recurrent seizure @ 12 months
See this image and copyright information in PMC

Update of

References

References to studies included in this review

Autret 1990 {published data only}
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Barghout 2019 {published data only}
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Camfield 1980 {published data only}
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Fallah 2015 {published data only}
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Garcia 1984 {published data only}
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Mackintosh 1970 {published data only}
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Mamelle 1984 {published data only}
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McKiernan 1981 {published data only}
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McKinlay 1989 {published data only}
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Mosquera 1987 {published data only}
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Ngwane 1980 {published data only}
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Pavlidou 2006 {published data only}
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Ramakrishnan 1986 {published data only}
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Rosman 1993 {published data only}
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Salehiomran 2016 {published data only}
    1. Salehiomran M, Hoseini SM, Ghabeli Juibary A. Intermittent diazepam versus continuous phenobarbital to prevent recurrence of febrile seizures: a randomized controlled trial. Iran Journal of Childhood Neurology 2016;10(1):21-4. - PMC - PubMed
Strengell 2009 {published data only}
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Taghdiri 2011 {published data only}
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Uhari 1995 {published data only}
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Van Stuijvenberg 1998 {published data only}
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Verrotti 2004 {published data only}
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Williams 1979 {published data only}
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Wolf 1977 {published data only}
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References to studies excluded from this review

Addy 1977 {published data only}
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Amouian 2013 {published data only}
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Antony 1983 {published data only}
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Fayyazi 2018 {published data only}
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Frelih 1997 {published data only}
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Galli 1977 {published data only}
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Kazemi 2013 {published data only}
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Knudsen 1978 {published data only}
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Lahat 2000 {published data only}
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Minagawa 1981 {published data only}
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Murata 2018 {published data only}
    1. Murata S, Okasora K, Tanabe T, Ogino M, Yamazaki S, Oba C, et al. Acetaminophen and febrile seizure recurrences during the same fever episode. Pediatrics November 2018;142(5):e20181009. - PubMed
Nemati 2019 {published data only}
    1. Nemati H, Talebianpour H, Lotfi F, Sepehri NZ, Keshavarz KH. Cost-effectiveness analysis of topiramate versus phenobarbital in the treatment of children with febrile seizure. Iranian Journal of Child Neurology 2019;13(4):109-20. [PMID: ] - PMC - PubMed
Rose 2005 {published data only}
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Rosman 2001 {published data only}
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References to other published versions of this review

Offringa 2007
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Offringa 2012
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Offringa 2017
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