结核病和乙型肝炎疫苗在预防特应性皮炎中的保护作用:前瞻性队列研究的中期结果报告

Veronika A. Petrova, L. Namazova-Baranova, M. Fedoseenko, D. Rusinova
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引用次数: 0

摘要

背景。研究表明,在出生后的头几个小时或几天内接种疫苗可将免疫反应从宫内Th2转向th1型激活,并降低特应性疾病的风险。然而,我们没有找到关于这一主题的前瞻性研究的公开数据。本研究的目的是确定在生命最初几小时/天内接种结核病和乙型肝炎疫苗与婴儿特应性皮炎发展之间存在负相关关系。对2021年4月~ 6月出生并在1个门诊就诊的患儿队列进行连续前瞻性研究。对307例婴儿记录(F. 112/y)、疫苗接种记录卡(F. 063/y)、产前和分娩记录(F. 113/y-20,第3节)和新生儿出院摘要的数据进行了分析。评估儿童疫苗接种状况(到接种结核病和乙型肝炎疫苗时)、过敏性疾病发展危险因素的存在以及特应性皮炎的存在。在妇产医院接种BCG-M的婴儿在1岁前被诊断出AD的可能性明显低于晚接种或根本未接种的婴儿(分别为15.2%对66%和35.7%;P < 0.01)。在妇产医院接种结核病疫苗的具有过敏性疾病危险因素的儿童发生AD的可能性低于晚接种或未接种的儿童(分别为18%、75%和62.5%);P < 0.01)。在妇产医院接种乙肝疫苗的儿童12月龄诊断为AD的比例明显低于晚接种或未接种的儿童(分别为17.6%、44.9%和31.8%);P < 0.01)。发生变应性疾病风险儿童的这一比例分别为24%、50%和44.4% (p = 0.043)。也有研究表明,与未接种疫苗的个体或仅接种一种疫苗的个体相比,在新生儿早期及时接种两种疫苗可显著降低一般婴儿人群发生阿尔茨海默病的风险(优势比[or] 0.374;95%置信区间[CI] 0.253 ~ 0.552;P < 0.01)。在有过敏风险的儿童中,及时接种疫苗的发病率较低(20.8% vs 53.3%;Or = 0.252;95% ci 0.145-0.440;Or = 0.374;95% ci为0,253-0,552;p < 0.01)。所得结果可能表明,及时预防接种结核病和乙型肝炎疫苗,特别是有过敏风险的儿童,可能会降低AD发展的风险。这项研究目前正在进行中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Protective Role of Vaccination against Tuberculosis and Hepatitis B in Prevention of Atopic Dermatitis: Report on Intermediate Results of Prospective Cohort Study
Background. Studies have shown that vaccination in the first hours/days after birth shifts the immune response from intrauterine Th2 towards Th1-type activation and reduces the risk of atopic conditions. However, we did not find published data from prospective studies on this topic.Objective. The aim of the study is to define the presence of negative correlation between vaccination against tuberculosis and hepatitis B in the first hours/days of life and atopic dermatitis development in infants.Methods. Continuous prospective study of children cohort born from April to June 2021 and observed in one outpatient’s clinic was carried out. Data from 307 infant’s records (F. 112/y), vaccination record cards (F. 063/y), prenatal and delivery records (F. 113/y-20, section № 3), and neonatal discharge summaries were analyzed for the decreed period. The child vaccination status (by the time of vaccination against tuberculosis and hepatitis B), presence of risk factors for allergic disease development, and presence of atopic dermatitis were evaluated.Results. Atopic dermatitis (AD) was significantly less likely to be diagnosed by the age of 1 year in infants from the group of BCG-M vaccinated at maternity hospital than in those vaccinated later or not vaccinated at all (15.2% versus 66% and 35.7%, respectively; p < 0,01). AD was less likely to develop in children with risk factors for allergic disease who were vaccinated against tuberculosis in the maternity hospital than in those vaccinated later or unvaccinated at all (18, 75 and 62.5%, respectively; p < 0.01). The ratio of children with diagnosed AD by the age of 12 months was significantly less in the group of children vaccinated against hepatitis B in the maternity hospital than in those vaccinated later or unvaccinated at all (17.6, 44.9 and 31.8%, respectively; p < 0.01). These ratios for children with risk of allergic disease development were 24%, 50% and 44.4%, respectively (p = 0.043). It has also been shown that timely vaccination with both vaccines in the early neonatal period significantly reduces the risk of AD in general infant population compared to non-vaccinated individuals or those who had only one vaccine (odds ratio [OR] 0.374; 95% confidence interval [CI] 0.253-0.552; p < 0.01). Whereas the disease development in children with allergic risk is less likely with timely vaccination (20.8% versus 53.3%; OR = 0.252; 95% CI 0.145–0.440; OR = 0.374; 95% CI 0,253–0,552; p < 0,01).Conclusion. The obtained results may indicate possible risk reduction for AD development due to timely preventive vaccination against tuberculosis and hepatitis B, especially in children with allergic risk. The study is currently ongoing. 
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