aa Vesikari 2006a.
| Methods | Double‐blind RCT assessing efficacy and safety of CAIV‐T in children. Multicentre trial conducted in Belgium, Finland, the UK, Israel, Spain during the period 2 October 2000 to 31 May 2002. Follow‐up for each year lasted until 31 May and was a composite of phone calls, home and visit clinics. Coding as well as randomisation carried out centrally and assigned by a blind investigator on the basis of a pre‐printed randomisation schedule. Both ITT and PP populations were defined. Analyses were carried out only for outcomes occurring in periods of viral circulation in the different centre areas. | |
| Participants | 1616 healthy children aged 6 to 35 months attending day care (at least 12 hours weekly) in 1 of the centres who continued to be healthy during year 2 were included in the primary analysis (951 vaccine and 665 placebo recipients). 1784 children were originally randomised on 3:2 basis. There was considerable attrition between the year 1 ITT population (1059 in the active arm and 725 in the placebo arm) and the year 2 PP population (640 and 450, respectively), with 65 dropouts in the placebo arm and 132 in the intervention arm (calculated from the flow diagram of population, which does not add up). Table 1 reports 174 of the 1616 PP population as aged 6 to 12 months, 598 aged 12 to 23 months, and 844 aged 24 months or more. | |
| Interventions | CAIV‐T (Wyeth) containing A/New Caledonia/20/99 (H1N1), A/Sydney/05/97 (H3N2), and B/Yamanashi/166/98 in year 1 and A/New Caledonia/20/99 (H1N1), A/Panama/2007/99 (H3N2), and B/Victoria/504/2000 or sterile physiological solution placebo. For technical reasons, antigens in year 1 were similar to those recommended, and in year 2 they were those recommend by WHO. Dose was 0.2 mL in each nostril twice in year 1 (approximately 35 days apart) and once in year 2. Spray applicators were preloaded centrally and all identical. In year 1 the match was good, in year 2 the match was not so good because of drifted variants and the appearance of 2 different strains of influenza B vaccine. | |
| Outcomes |
Serological
Children with fever (rectal 38 °C or more and oral 37.5 °C or more), wheezing shortness of breath, pulmonary congestion, pneumonia, or ear infection got a nasal swab and those with 2 or more of the following: runny nose, nasal congestion, sore throat, cough, muscle aches, chills, irritability, decreased activity, or vomiting Effectiveness Influenza caused by subtypes antigenically similar to those contained in the vaccine (primary endpoint) and by those drifted from the recommended ones (secondary endpoint)
Safety Parents/guardians kept diary card to record axillary or rectal temperature, runny nose or nasal congestion, sore throat, cough, vomiting, activity level, appetite, irritability, headache, chills, muscle pain, and antipyretic medication use, unscheduled physician contacts for 11 consecutive days from vaccination and throughout the study any unscheduled event that required healthcare contact or study termination. Fevers were classified as mild, moderate, or severe (equal to or more than 37.5 °C, 38.6 °C, and 40 °C axillary respectively or 38 °C, 39.1 °C, and 40 °C rectally). Adverse events are reported in a mixture of table and text format. We have extracted the AEs for up to 11 days postvaccination, but the text reports no significant difference between those occurring within 11 days of vaccination and those occurring throughout the surveillance period. These are classed as possible, probable, or definitely caused by vaccination, but the definition of the association is unclear: "Lower respiratory tract illnesses reported as serious AEs from receipt of the first dose of study medication through the end of the first influenza surveillance period were also similar between treatment groups (pneumonia: 11 CAIV‐T recipients and 9 placebo recipients; bronchitis: 3 CAIV‐T recipients and 1 placebo recipient; bronchospasm: 2 CAIV‐T recipients and 2 placebo recipients; bronchiolitis: 1 CAIV‐T recipient and 2 placebo recipients) In participants 6 to 12 months of age, lower respiratory tract infections reported as serious AEs were pneumonia (2 CAIV‐T recipients and 1 placebo recipient), bronchitis (2 CAIV‐T recipients and 0 placebo recipients) and bronchospasm (1 CAIV‐T recipient and 0 placebo recipients). Serious AEs judged to be possibly, probably, or definitely related to study vaccination were reported for 9 CAIV‐T recipients (pneumonia and AOM, 2 recipients; bronchopneumonia, 2 recipients; pneumonia, 1 recipient; bronchiolitis, 1 recipient; bronchitis and AOM, 1 recipient; idiopathic thrombocytopenic purpura, 1 recipient; and fever, acute respiratory tract infection, dehydration and AOM, 1 recipient) and 5 placebo recipients (1 each for pneumonia and constipation; cough, wheeze and lung consolidation; pneumonia; idiopathic thrombocytopenic purpura; and hypersensitivity, erythema and periorbital edema). There were no statistically significant differences in serious AEs between treatment groups during the second influenza surveillance period. Six lower respiratory tract illnesses were reported, all among CAIV‐T recipients (5 cases of pneumonia and 1 of bronchospasm). 2 cases of pneumonia were judged to be possibly, probably, or definitely related to study vaccination. A total of 4 participants (2 CAIV‐T recipients and 2 placebo recipients) were withdrawn from the study because of AEs. No deaths occurred during the study period" |
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| Funding Source | Industry | |
| Notes | The authors conclude that "cold‐adapted influenza vaccine‐trivalent was well tolerated and effective in preventing culture‐confirmed influenza illness in children as young as 6 months of age who attended day care". Formally this is a very well‐reported study following CONSORT guidelines. There are however numerous discrepancies in the text. Vaccine was not available until the end of November in year 2, and it is unclear what effect this had (immunisation was completed on 21 December, in the case of Israel this was after the beginning of viral circulation). In addition, the centres went from 70 in year 1 to 62 in year 2 for unexplained reasons. A major unexplained problem is seen in Table 7 (harm events reporting). 2 figures are shown for the 6 columns (vaccine and placebo by dose by year of the trial) representing "the number of subjects with known values" and then presumably the randomised denominator (which does not fit with either ITT or PP numbers). The figures show runny nose as significantly higher in dose 1 year 1 recipients, which could explain the high attrition between dose 1 year 1 and single dose year 2 (from 1021 to 631). | |
| Risk of bias | ||
| Bias | Authors' judgement | Support for judgement |
| Random sequence generation (selection bias) | Low risk | Adequate |
| Allocation concealment (selection bias) | Low risk | Adequate |
| Blinding (performance bias and detection bias) All outcomes | Low risk | Adequate |
| Incomplete outcome data (attrition bias) All outcomes | Low risk | The proportion of missing outcomes compared with observed event risk is not enough to have a clinically relevant impact on the intervention effect estimate. |
| Summary assessments | Low risk | Plausible bias unlikely to seriously alter the results. |