El‐Shimi 2015.
| Methods | Three‐arm, comparative, prospective randomised study 1. Masking of randomisation: yes 2. Masking of intervention: unclear; yes according to study authors, but one group received no intervention. Thus it is unclear how this could have been achieved. 3. Completeness of follow‐up: yes 4. Masking of outcome assessment: yes | |
| Participants | 75 infants ≤ 34 weeks' gestation at birth were enrolled after parental consent.
Arginine group (N = 25): Mean (SD) birth weight was 1450 (260) grams and gestational age was 31.84 (2.3) weeks Glutamine group (N = 25): Mean (SD) birth weight was 1310 (250) grams and gestational age was 30.64 (2.3) weeks Control (no treatment) group (N = 25): Mean (SD) birth weight was 1450 (210) grams and gestational age was 31.86 (1.4) weeks Exclusion criteria: newborns with congenital malformations, chromosomal abnormalities, suspected inborn error of metabolism, sepsis, IVH grade ≥ II, undergoing intestinal surgery or having any contraindication to enteral feeding |
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| Interventions | Arginine group: Infants received L‐arginine (0.75 mmol/kg/d) with the start of enteral feedings, doubled to 1.5 mmol/kg/d (261 mg/kg/d) when 40% of enteral feeding (60 cc/kg) was reached. Arginine was supplemented until 30 days' postnatal age. The dose was administered orally or via nasogastric tube every 12 hours Glutamine group: Infants received glutamine (156 mg/kg/d) with the start of enteral feedings, doubled to 312 mg/kg/d when 40% of enteral feeding (60 cc/kg) was reached. Glutamine was supplemented until 30 days' postnatal age. The dose was divided every 12 hours and was taken orally or via nasogastric tube. Control group: Infants started enteral feeding within first week without arginine or glutamine supplementation |
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| Outcomes | NEC, all stages NEC, stage 2 NEC, stage 3 Mortality due to NEC Mortality due to any cause Arginine concentrations at baseline, at time of NEC diagnosis and at day 14 of life |
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| Notes | ||
| Risk of bias | ||
| Bias | Authors' judgement | Support for judgement |
| Random sequence generation (selection bias) | Low risk | Simple randomisation method was based on computer‐generated sequence. |
| Allocation concealment (selection bias) | Low risk | Allocation was concealed (information provided by study authors). |
| Blinding (performance bias and detection bias) All outcomes | Unclear risk | Participants, doctors and nurses evaluating outcomes were blinded to intervention allocation according to study authors; however, it is unclear how this may have been achieved when the control group received no intervention (information provided by study authors). |
| Incomplete outcome data (attrition bias) All outcomes | Low risk | All randomised participants were accounted for in the analysis. |
| Selective reporting (reporting bias) | Low risk | The registered primary outcome and the reported primary outcome were aligned. No prespecified secondary outcomes were stated. |
| Other bias | Low risk | |