肺炎球菌血清型分布以及现有和在研肺炎球菌疫苗的覆盖情况

PNEUMOCOCCAL SEROTYPE DISTRIBUTION AND COVERAGE OF EXISTING AND PIPELINE PNEUMOCOCCAL VACCINES.

作者信息

King Laura M, Andrejko Kristin L, Kobayashi Miwako, Xing Wei, Cohen Adam L, Self Wesley H, Resser J Jackson, Whitney Cynthia G, Baughman Adrienne, Kio Mai, Grijalva Carlos G, Traenkner Jessica, Rouphael Nadine, Lewnard Joseph A

机构信息

School of Public Health, University of California, Berkeley, Berkeley, California, United States.

Division of Bacterial Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, United States.

出版信息

medRxiv. 2024 Dec 13:2024.12.12.24318944. doi: 10.1101/2024.12.12.24318944.

DOI:10.1101/2024.12.12.24318944

PMID:39711720

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11661329/

Abstract

BACKGROUND

(pneumococcus) causes invasive pneumococcal disease (IPD) and non-invasive acute respiratory infections (ARIs). Three pneumococcal conjugate vaccines (PCVs) are recommended in the United States with additional products in clinical trials. We aimed to estimate 1) proportions of IPD cases and pneumococcal ARIs caused by serotypes targeted by existing and pipeline PCVs and 2) annual U.S. pneumococcal burdens potentially preventable by PCVs.

METHODS

We estimated serotype distribution and proportions of non-invasive pneumococcal ARIs (AOM [children only], sinusitis, non-bacteremic pneumonia) and IPD attributable to serotypes targeted by each PCV using Markov chain Monte Carlo approaches incorporating data from studies of serotype distribution in ARIs and Active Bacterial Core Surveillance (ABCs) data. We then estimated annual numbers of outpatient-managed pneumococcal ARIs, non-bacteremic pneumococcal pneumonia hospitalizations, and IPD cases potentially preventable by PCVs in the United States by multiplying pneumococcal disease incidence rates by PCV-targeted proportions of disease and vaccine effectiveness estimates.

RESULTS

In children, PCV15, PCV20, PCV24, PCV25, and PCV31 serotypes account for 16% (95% confidence interval: 15-17%), 31% (30-32%), 34% (32-35%), 43% (42-44%), and 68% (67-69%) of pneumococcal acute otitis media cases, respectively. In adults, PCV15, PCV20, PCV21, PCV24, PCV25, and PCV31 serotypes account for 43% (38-47%), 52% (47-57%), 69% (64-73%), 65% (61-70%), 62% (57-67%), and 87% (83-90%) of pneumococcal non-bacteremic pneumonia cases. For IPD, 42-85% of pediatric and 42-94% of adult cases were due to PCV-targeted serotypes. PCV-preventable burdens encompassed 270 thousand-3.3 million outpatient-managed ARIs, 2-17 thousand non-bacteremic pneumonia hospitalizations, and 3-14 thousand IPD cases in the United States annually.

CONCLUSIONS

Across pneumococcal conditions, coverage and preventable burdens were lowest for PCV15 and highest for PCV31, with PCV21 also targeting sizeable burdens of adult disease. Serotype distribution across syndromes may inform vaccine formulations and policy.

摘要

背景

肺炎球菌可引起侵袭性肺炎球菌病（IPD）和非侵袭性急性呼吸道感染（ARI）。美国推荐使用三种肺炎球菌结合疫苗（PCV），还有其他产品正在进行临床试验。我们旨在估计：1）现有和在研PCV所针对血清型引起的IPD病例和肺炎球菌ARI的比例；2）美国每年可能通过PCV预防的肺炎球菌负担。

方法

我们采用马尔可夫链蒙特卡罗方法，结合ARI血清型分布研究数据和主动细菌核心监测（ABCs）数据，估计每种PCV所针对血清型导致的非侵袭性肺炎球菌ARI（仅儿童的急性中耳炎、鼻窦炎、非菌血症性肺炎）和IPD的血清型分布及比例。然后，我们通过将肺炎球菌疾病发病率乘以PCV所针对疾病的比例和疫苗效力估计值，来估计美国每年门诊管理的肺炎球菌ARI、非菌血症性肺炎球菌肺炎住院病例以及可能通过PCV预防的IPD病例数。

结果

在儿童中，PCV15、PCV20、PCV24、PCV25和PCV31血清型分别占肺炎球菌急性中耳炎病例的16%（95%置信区间：15 - 17%）、31%（30 - 32%）、34%（32 - 35%）、43%（42 - 44%）和68%（67 - 69%）。在成人中，PCV15、PCV20、PCV21、PCV24、PCV25和PCV31血清型分别占肺炎球菌非菌血症性肺炎病例的43%（38 - 47%）、52%（47 - 57%）、69%（64 - 73%）、65%（61 - 70%）、62%（57 - 67%）和87%（83 - 90%）。对于IPD，42% - 85%的儿科病例和42% - 94%的成人病例由PCV所针对的血清型引起。在美国，PCV可预防的负担包括每年27万 - 330万门诊管理的ARI、2000 - 17000例非菌血症性肺炎住院病例以及3000 - 14000例IPD病例。

结论

在各种肺炎球菌疾病中，PCV15的覆盖率和可预防负担最低，PCV31最高，PCV21也针对相当比例的成人疾病负担。各综合征的血清型分布可为疫苗配方和政策提供参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b59/11661329/8bc37640e691/nihpp-2024.12.12.24318944v1-f0001.jpg

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肺炎球菌血清型分布以及现有和在研肺炎球菌疫苗的覆盖情况

PNEUMOCOCCAL SEROTYPE DISTRIBUTION AND COVERAGE OF EXISTING AND PIPELINE PNEUMOCOCCAL VACCINES.

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