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血清型特异性侵袭能力和侵袭性肺炎球菌病的持续减少。

Serotype specific invasive capacity and persistent reduction in invasive pneumococcal disease.

机构信息

Department of Pediatrics, Boston University, School of Medicine, Boston, MA, USA.

出版信息

Vaccine. 2010 Dec 16;29(2):283-8. doi: 10.1016/j.vaccine.2010.10.032. Epub 2010 Oct 26.

Abstract

Defining the propensity of Streptococcus pneumoniae (SP) serotypes to invade sterile body sites following nasopharyngeal (NP) acquisition has the potential to inform about how much invasive pneumococcal disease (IPD) may occur in a typical population with a given distribution of carriage serotypes. Data from enhanced surveillance for IPD in Massachusetts children ≤7 years in 2003/04, 2006/07 and 2008/09 seasons and surveillance of SP NP carriage during the corresponding respiratory seasons in 16 Massachusetts communities in 2003/04 and 8 of the 16 communities in both 2006/07 and 2008/09 were used to compute a serotype specific "invasive capacity (IC)" by dividing the incidence of IPD due to serotype x by the carriage prevalence of that same serotype in children of the same age. A total of 206 IPD and 806 NP isolates of SP were collected during the study period. An approximate 50-fold variation in the point estimates between the serotypes having the highest (18C, 33F, 7F, 19A, 3 and 22F) and lowest (6C, 23A, 35F, 11A, 35B, 19F, 15A, and 15BC) IC was observed. Point estimates of IC for most of the common serotypes currently colonizing children in Massachusetts were low and likely explain the continued reduction in IPD from the pre-PCV era in the absence of specific protection against these serotypes. Invasive capacity differs among serotypes and as new pneumococcal conjugate vaccines are introduced, ongoing surveillance will be essential to monitor whether serotypes with high invasive capacity emerge (e.g. 33F, 22F) as successful colonizers resulting in increased IPD incidence due to replacement serotypes.

摘要

确定肺炎链球菌(SP)血清型在鼻咽部(NP)获得后侵袭无菌部位的倾向,可能有助于了解在具有特定携带血清型分布的典型人群中,侵袭性肺炎球菌病(IPD)可能发生的程度。该数据来源于马萨诸塞州儿童(2003/04 年、2006/07 年和 2008/09 年)强化监测期间的 IPD 数据,以及 2003/04 年 16 个马萨诸塞州社区的 SP NP 携带情况监测数据和 2006/07 年和 2008/09 年的 16 个社区中的 8 个社区的数据。通过将 X 血清型引起的 IPD 发病率除以相同年龄儿童的相同血清型携带率,计算出每种血清型的特定“侵袭能力(IC)”。研究期间共采集了 206 株 IPD 和 806 株 SP NP 分离株。在具有最高侵袭能力(18C、33F、7F、19A、3 和 22F)和最低侵袭能力(6C、23A、35F、11A、35B、19F、15A 和 15BC)的血清型之间,点估计值的差异约为 50 倍。马萨诸塞州儿童目前携带的大多数常见血清型的 IC 点估计值均较低,这可能解释了在缺乏针对这些血清型的特异性保护的情况下,从 PCV 时代前开始,IPD 持续减少的原因。侵袭能力在血清型之间存在差异,随着新的肺炎球菌结合疫苗的引入,持续监测对于监测高侵袭能力的血清型是否出现(例如 33F、22F)成为成功的定植者,从而导致由于替代血清型引起的 IPD 发病率增加至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e4a1/3139683/9852de39497a/nihms292585f1.jpg

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