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首页> 外文期刊>Infection >Hepatitis B vaccination: long-term follow-up of the immune response of preterm infants and comparison of two vaccination protocols.
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Hepatitis B vaccination: long-term follow-up of the immune response of preterm infants and comparison of two vaccination protocols.

机译:乙肝疫苗接种:对早产婴儿的免疫反应进行长期随访,并比较两种疫苗接种方案。

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BACKGROUND: We conducted a 3-year follow-up study of long-term antibody persistence following vaccination of low-risk preterm infants with recombinant hepatitis B vaccine (HBV). Two three-dose protocols were compared: vaccination beginning within 24 h of birth to initial vaccination delayed until a weight of 2,000 g was reached. SUBJECTS AND METHODS: The study population included 136 children, divided into three groups: children born prematurely (< or = 35 weeks, n = 57), children born at term (> or = 37 weeks, n = 39), both groups receiving the first dose of HBV within 24 h of birth, and children born prematurely (< or = 35 weeks, n = 40), who received the first dose of HBV when a weight of 2,000 g was reached. All infants received the second hepatitis vaccination 1 month after the first, and the third dose 6 months after the first. Hepatitis B surface antibody (AntiHBs) was measured at an age of 3-3.5 years (at least 2.5 years after completion of the three-dose HBV series). An AntiHBs level of > or = 10 IU/l was considered positive. RESULTS: At 3-3.5 years of age, a higher percentage of the premature-delayed vaccination group had a positive AntiHBs level (92.5%) compared to both the premature (54.4%, p < 0.001) and full-term groups (71.8%, p < 0.05) vaccinated soon after birth. The premature-delayed vaccination group also had a significantly higher geometric mean concentration (GMC) (119 vs 14.2 IU/l, p < 0.001 and 119 vs 32.7 IU/l, p < 0.005, respectively). CONCLUSION: Delaying vaccination of premature infants against hepatitis B until a weight of 2,000 g was reached resulted in both a significantly higher percentage of children with positive antibody levels and a significantly higher GMC at 3-3.5 years of age as compared to early-vaccinated preterm and full-term infants. The known short-term advantage of delayed vaccination of preterm infants was shown to persist for at least the first 3 years of life.
机译:背景:我们对低危早产儿接种重组乙型肝炎疫苗(HBV)进行疫苗接种后,长期抗体持久性进行了为期3年的随访研究。比较了两种三剂方案:从出生后24小时内开始接种疫苗,直至最初的疫苗接种推迟到体重达到2,000 g为止。研究对象和方法:研究人群包括136名儿童,分为三组:早产儿(<或= 35周,n = 57),足月儿(>或= 37周,n = 39),两组均接受出生后24小时内首次服用HBV,早产儿(<或= 35周,n = 40),体重达到2,000 g时接受HBV首次服用。所有婴儿在第一次接种后1个月接受第二次肝炎疫苗接种,第一次接种后6个月进行第三次接种。乙型肝炎表面抗体(AntiHBs)的年龄为3-3.5岁(完成三剂HBV系列后至少2.5年)。 AntiHBs水平>或= 10 IU / l被视为阳性。结果:在3-3.5岁年龄组,早产疫苗组中抗HBs阳性的比例更高(92.5%),而早产组(54.4%,p <0.001)和足月组(71.8%) ,p <0.05)出生后不久就接种了疫苗。早产疫苗接种组的几何平均浓度(GMC)也明显更高(分别为119 vs. 14.2 IU / l,p <0.001和119 vs. 32.7 IU / l,p <0.005)。结论:与早接种早产儿相比,早产婴儿对乙型肝炎的疫苗接种直到体重达到2,000 g时,导致抗体阳性抗体儿童的百分比显着提高,并且3-3.5岁时的GMC显着提高。和足月婴儿。已显示早产儿延迟接种疫苗的已知短期优势至少可以持续到生命的最初3年。

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