Norhayati Mohd N, Ho Jacqueline J, Azman Mohd Y
Department of Family Medicine, Universiti Sains Malaysia, School of Medical Sciences, Health Campus, Kubang Kerian, Kelantan, Malaysia, 16150.
Cochrane Database Syst Rev. 2017 Oct 17;10(10):CD010089. doi: 10.1002/14651858.CD010089.pub3.
Acute otitis media (AOM) is one of the most common infectious diseases in children. It has been reported that 64% of infants have an episode of AOM by the age of six months and 86% by one year. Although most cases of AOM are due to bacterial infection, it is commonly triggered by a viral infection. In most children AOM is self limiting, but it does carry a risk of complications. Since antibiotic treatment increases the risk of antibiotic resistance, influenza vaccines might be an effective way of reducing this risk by preventing the development of AOM.
To assess the effectiveness of influenza vaccine in reducing the occurrence of acute otitis media in infants and children.
We searched the Cochrane Central Register of Controlled Trials (CENTRAL), MEDLINE, Embase, CINAHL, LILACS, Web of Science, the WHO International Clinical Trials Registry Platform, and ClinicalTrials.gov (15 February 2017). We also searched the reference lists of included studies to identify any additional trials.
Randomised controlled trials comparing influenza vaccine with placebo or no treatment in infants and children aged younger than six years. We included children of either sex and of any ethnicity, with or without a history of recurrent AOM.
Two review authors independently screened studies, assessed trial quality, and extracted data. We performed statistical analyses using the random-effects and fixed-effect models and expressed the results as risk ratio (RR), risk difference (RD), and number needed to treat for an additional beneficial outcome (NNTB) for dichotomous outcomes, with 95% confidence intervals (CI).
We included 11 trials (6 trials in high-income countries and 5 multicentre trials in high-, middle-, and low-income countries) involving 17,123 children aged 6 months to 6 years. Eight trials recruited participants from a healthcare setting. Ten trials (and all four trials that contributed to the primary outcome) declared funding from vaccine manufacturers. Four trials reported adequate allocation concealment, and 10 trials reported adequate blinding of participants and personnel. Attrition was low for eight trials included in the analysis.The primary outcome showed a small reduction in at least one episode of AOM over at least six months of follow-up (4 trials, 3134 children; RR 0.84, 95% CI 0.69 to 1.02; RD -0.04, 95% CI -0.08 to -0.00; NNTB 25, 95% CI 12.5 to 100; low-quality evidence).The subgroup analyses (i.e. number of courses and types of vaccine administered) showed no differences.There was a reduction in the use of antibiotics in vaccinated children (2 trials, 1223 children; RR 0.70, 95% CI 0.59 to 0.83; RD -0.11, 95% CI -0.16 to -0.06; moderate-quality evidence).We were unable to demonstrate whether there was any difference in the utilisation of health care. The use of influenza vaccine resulted in a significant increase in fever (7 trials, 10,615 children; RR 1.15, 95% CI 1.06 to 1.24; RD 0.02, 95% CI 0.00 to 0.04; low-quality evidence), rhinorrhoea (6 trials, 10,563 children; RR 1.17, 95% CI 1.07 to 1.29; RD 0.09, 95% CI 0.01 to 0.16; low-quality evidence), but no difference in pharyngitis. No major adverse events were reported.Differing from the protocol, the original publication of the review included a subgroup analysis of AOM episodes by season, and the secondary outcome 'types of influenza vaccine' was changed to a subgroup analysis. For this update, we removed the subgroup analyses for trial setting, season, and utilisation of health care due to the small number of trials involved. We removed Belshe 2000 from primary and secondary outcomes (courses of vaccine and types of vaccine) because it reported episodes of AOM per person. We did not perform a subgroup analysis by type of adverse event. We have reported each type of adverse event as a separate analysis.
AUTHORS' CONCLUSIONS: Influenza vaccine results in a small reduction in AOM. The observed reduction in the use of antibiotics needs to be considered in light of current recommended practices aimed at avoiding antibiotic overuse. Safety data from these trials were limited. The benefits may not justify the use of influenza vaccine without taking into account the vaccine efficacy in reducing influenza and safety data. We judged the quality of the evidence to be low to moderate. Additional research is needed.
急性中耳炎(AOM)是儿童最常见的传染病之一。据报道,64%的婴儿在6个月大时曾患过一次AOM,1岁时这一比例为86%。尽管大多数AOM病例是由细菌感染引起的,但通常由病毒感染引发。在大多数儿童中,AOM是自限性的,但确实存在并发症风险。由于抗生素治疗会增加抗生素耐药性风险,流感疫苗可能是通过预防AOM发生来降低这种风险的有效方法。
评估流感疫苗在降低婴幼儿和儿童急性中耳炎发生率方面的有效性。
我们检索了Cochrane对照试验中心注册库(CENTRAL)、医学期刊数据库(MEDLINE)、荷兰医学文摘数据库(Embase)、护理学与健康领域数据库(CINAHL)、拉丁美洲和加勒比地区卫生科学数据库(LILACS)、科学引文索引(Web of Science)、世界卫生组织国际临床试验注册平台以及美国国立医学图书馆临床试验数据库(ClinicalTrials.gov,检索截至2017年2月15日)。我们还检索了纳入研究的参考文献列表,以识别任何其他试验。
比较流感疫苗与安慰剂或未治疗对6岁以下婴幼儿和儿童影响的随机对照试验。我们纳入了任何性别、种族的儿童,无论有无复发性AOM病史。
两位综述作者独立筛选研究、评估试验质量并提取数据。我们使用随机效应模型和固定效应模型进行统计分析,并将结果表示为风险比(RR)、风险差(RD)以及二分结果的额外有益结局所需治疗人数(NNTB),并给出95%置信区间(CI)。
我们纳入了11项试验(6项在高收入国家进行,5项在高、中、低收入国家进行的多中心试验),涉及17123名6个月至6岁的儿童。8项试验从医疗机构招募参与者。10项试验(以及所有对主要结局有贡献的4项试验)声明接受了疫苗制造商的资助。4项试验报告了充分的分配隐藏,10项试验报告了对参与者和工作人员的充分盲法。分析中纳入的8项试验的失访率较低。主要结局显示,在至少6个月的随访中,至少发生一次AOM的情况略有减少(4项试验,3134名儿童;RR 0.84,95%CI 0.69至1.02;RD -0.04,95%CI -0.08至-0.00;NNTB 25,95%CI 12.5至100;低质量证据)。亚组分析(即接种疫苗的疗程数和类型)未显示差异。接种疫苗的儿童使用抗生素的情况有所减少(2项试验,1223名儿童;RR 0.70,95%CI 0.59至0.83;RD -0.11,95%CI -0.16至-0.06;中等质量证据)。我们无法证明在医疗保健利用方面是否存在差异。使用流感疫苗导致发热显著增加(7项试验,10615名儿童;RR 1.15,95%CI 1.06至1.24;RD 0.02,95%CI 0.00至0.04;低质量证据)、流涕显著增加(6项试验,10563名儿童;RR 1.17,95%CI 1.07至1.29;RD 0.09,95%CI 0.01至0.16;低质量证据),但在咽炎方面无差异。未报告重大不良事件。与方案不同的是,该综述的原始发表纳入了按季节对AOM发作的亚组分析,次要结局“流感疫苗类型”改为亚组分析。对于本次更新,由于涉及的试验数量较少,我们删除了关于试验设置、季节和医疗保健利用的亚组分析。我们将Belshe 2000从主要和次要结局(疫苗疗程和疫苗类型)中排除,因为它报告的是每人的AOM发作情况。我们未按不良事件类型进行亚组分析。我们已将每种不良事件作为单独分析进行报告。
流感疫苗可使AOM略有减少。鉴于目前旨在避免抗生素过度使用的推荐做法,需要考虑观察到的抗生素使用减少情况。这些试验的安全性数据有限。在不考虑疫苗预防流感的功效和安全性数据的情况下,其益处可能不足以证明使用流感疫苗的合理性。我们判断证据质量为低到中等。需要进一步研究。
