Risk of bias for analysis 9.9 Proportion of infants with persistent seizures and/or requiring ASM at discharge.

Study

Bias

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Authors' judgement

Support for judgement

Authors' judgement

Support for judgement

Authors' judgement

Support for judgement

Authors' judgement

Support for judgement

Authors' judgement

Support for judgement

Authors' judgement

Support for judgement

Jindal 2021

Low risk of bias

Allocation concealed, sequence generation random and baseline characteristics does not reveal any imbalance between the two groups.

Low risk of bias

Though the personnel were aware of the intervention allocation, but there seems to be no deviations that arouse outside the trial context. Also all patients analysed as randomised.

Low risk of bias

Data reasonably complete for all the included patients

High risk of bias

Diagnosis of seizures was based on clinical assessment and not EEG. Hence, there is a likelihood that assessment might have been influenced by knowledge of allocation. There is no clear definition for different seizure types, how it was differentiated from non‐epiletic events and how it was assesed and by whom.

Low risk of bias

Trial analysed as per a priori registered protocol.

High risk of bias

High risk in one domain