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冈比亚儿童中额外的早期麻疹疫苗的免疫影响:3 岁时加强免疫的反应。

Immunological impact of an additional early measles vaccine in Gambian children: responses to a boost at 3 years.

机构信息

Medical Research Council Laboratories, Banjul, Gambia.

出版信息

Vaccine. 2012 Mar 28;30(15):2543-50. doi: 10.1016/j.vaccine.2012.01.083. Epub 2012 Feb 5.

Abstract

BACKGROUND

Measles vaccine in early infancy followed by a dose at 9 months of age protects against measles and enhances child survival through non-specific effects. Little is known of immune responses in the short or long term after booster doses.

METHODS

Infants were randomized to receive measles vaccine at 9 months of age (group 1) or 4 and 9 months of age (group 2). Both groups received a boost at 36 months of age. T-cell effector and memory responses using IFN-γ ELIspot and cytokine assays and antibody titres using a haemagglutination-inhibition assay were compared at various times.

RESULTS

Vaccination at 4 months of age elicited antibody and CD4 T-cell mediated immune responses .Two weeks after vaccination at 9 months of age group 2 had much higher antibody titres than group1 infants; cell-mediated effector responses were similar. At 36 months of age group 2 antibody titres exceeded protective levels but were 4-fold lower than group 1; effector and cytokine responses were similar. Re-vaccination resulted in similar rapid and high antibody titres in both groups (median 512); cellular immunity changed little. At 48 months of age group 2 antibody concentrations remained well above protective levels though 2-fold lower than group 1; T-cell memory was readily detectable and similar in both groups.

CONCLUSIONS

An additional early measles vaccine given to children at 4 months of age induced a predominant CD4 T-cell response at 9 months and rapid development of high antibody concentrations after booster doses. However, antibody decayed faster in these children than in the group given primary vaccination at 9 months of age. Cellular responses after 9 months were generally insignificantly different.

摘要

背景

在婴儿早期接种麻疹疫苗,然后在 9 个月大时再接种一剂,可以预防麻疹,并通过非特异性作用提高儿童的生存率。关于加强剂量后短期或长期的免疫反应,知之甚少。

方法

婴儿被随机分配在 9 个月大时(第 1 组)或 4 个月和 9 个月大时(第 2 组)接种麻疹疫苗。两组均在 36 个月时进行加强接种。使用 IFN-γ ELIspot 和细胞因子测定法检测 T 细胞效应和记忆应答,以及使用血凝抑制测定法检测抗体滴度,比较了不同时间点的情况。

结果

4 个月大时接种疫苗可引起抗体和 CD4 T 细胞介导的免疫反应。第 2 组在 9 个月大时接种疫苗两周后,抗体滴度明显高于第 1 组婴儿;细胞介导的效应应答相似。36 个月时,第 2 组的抗体滴度超过了保护水平,但比第 1 组低 4 倍;效应和细胞因子应答相似。加强接种后,两组的抗体滴度均迅速升高(中位数为 512),且相似;细胞免疫变化不大。48 个月时,第 2 组的抗体浓度仍远高于保护水平,尽管比第 1 组低 2 倍;T 细胞记忆在两组中均易被检测到,且相似。

结论

在 4 个月大时给儿童额外接种一剂麻疹疫苗,可在 9 个月大时引起主要的 CD4 T 细胞反应,并在加强接种后迅速产生高抗体浓度。然而,这些儿童的抗体衰减速度比在 9 个月大时接受初次接种的组更快。9 个月后,细胞反应一般无显著差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9cee/3401374/6dc0415fd57c/gr1.jpg

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