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引入7价肺炎球菌结合疫苗后澳大利亚婴儿的潜在载体启动效应。

Potential carrier priming effect in Australian infants after 7-valent pneumococcal conjugate vaccine introduction.

作者信息

Tashani Mohamed, Jayasinghe Sanjay, Harboe Zitta B, Rashid Harunor, Booy Robert

机构信息

Mohamed Tashani, Sanjay Jayasinghe, Harunor Rashid, Robert Booy, National Centre for Immunisation Research and Surveillance of Vaccine Preventable Diseases, the Children's Hospital at Westmead, Sydney 2145, Australia.

出版信息

World J Clin Pediatr. 2016 Aug 8;5(3):311-8. doi: 10.5409/wjcp.v5.i3.311.

DOI:10.5409/wjcp.v5.i3.311
PMID:27610348
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4978625/
Abstract

AIM

To investigate evidence of clinical protection in infants after one dose of 7-valent pneumococcal conjugate vaccine (7vPCV) owing to carrier priming.

METHODS

Using Australian National Notifiable Diseases Surveillance System data, we conducted a descriptive analysis of cases of vaccine type invasive pneumococcal disease (VT-IPD) during "catch-up" years, when 7vPCV was carrier primed by prior administration of DTPa vaccine. We compared the number of VT-IPD cases occurring 2-9 wk after a single dose of 7vPCV (carrier primed), with those < 2 wk post vaccination, when no protection from 7vPCV was expected yet. Further comparison was conducted to compare the occurrence of VT-IPD cases vs non-VT-IPD cases after a single carrier-primed dose of 7vPCV.

RESULTS

We found four VT-IPD cases occurring < 2 wk after one carrier primed dose of 7vPCV while only one case occurred 2-9 wk later. Upon further comparison with the non-VT-IPD cases that occurred after one carrier primed dose of 7vPCV, two cases were detected within 2 wk, whereas seven occurred within 2-9 wk later; suggesting a substantial level of protection from VT-IPD occurring from 2 wk after carrier-primed dose of 7vPCV.

CONCLUSION

This data suggest that infants may benefit from just one dose of 7vPCV, likely through enhanced immunity from carrier priming effect. If this is proven, an adjusted 2-dose schedule (where the first dose of PCV is not given until after DTPa) may be sufficient and more cost-effective.

摘要

目的

研究一剂7价肺炎球菌结合疫苗(7vPCV)因载体预激发而对婴儿产生临床保护作用的证据。

方法

利用澳大利亚国家法定传染病监测系统的数据,我们对“补种”年份期间疫苗型侵袭性肺炎球菌疾病(VT-IPD)病例进行了描述性分析,在此期间,7vPCV通过先前接种百白破疫苗进行载体预激发。我们比较了单剂7vPCV(载体预激发)接种后2-9周发生的VT-IPD病例数与接种后<2周发生的病例数,接种后<2周时预计7vPCV尚无保护作用。进一步比较了单剂载体预激发的7vPCV接种后VT-IPD病例与非VT-IPD病例的发生情况。

结果

我们发现,一剂载体预激发的7vPCV接种后<2周发生了4例VT-IPD病例,而2-9周后仅发生1例。与单剂载体预激发的7vPCV接种后发生的非VT-IPD病例进一步比较,2周内检测到2例,而2-9周后发生7例;这表明载体预激发剂量的7vPCV接种2周后对VT-IPD有显著保护作用。

结论

该数据表明,婴儿可能仅接种一剂7vPCV即可获益,可能是通过载体预激发效应增强了免疫力。如果得到证实,调整后的2剂接种程序(第一剂PCV直到接种百白破后才接种)可能就足够了,且更具成本效益。

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