Serotype Replacement After the Introduction of the 13-valent Pneumococcal Conjugate Vaccine in Ontario, Canada, 2007-2018

Allison Yeung, S. Wijayasri, Sarah E. Wilson, T. Harris, S. Buchan, S. Deeks
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Abstract

Introduction: Invasive pneumococcal disease (IPD) is a disease of public health significance in Ontario, Canada, where publicly funded pneumococcal vaccination programs target children, older adults, and people at high risk of disease. Since the implementation of pneumococcal conjugate vaccines (PCV), serotype replacement has been documented, where non-PCV serotypes replace the niche created by the reduction in vaccine-preventable serotypes. Our objective was to determine whether there has been serotype replacement or a change in IPD severity in Ontario since implementation of the childhood 13-valent (PCV13) program by assessing IPD burden over a 12-year period (2007-2018). Methods: We included all confirmed IPD cases reported in Ontario’s integrated Public Health Information System (iPHIS) and defined the pre-PCV13 era (January 2007-December 2010) and post-PCV13 era (January 2011-December 2018). We grouped IPD serotypes according to associated vaccine type: PCV13; 23-valent polysaccharide vaccine (unique PPV23); and non-vaccine-preventable (NVP). We used population data to calculate incidence and hospitalization rates (per 100,000 population) by age group, vaccine type, and era. Results: In the post-PCV13 era, PCV13-specific incidence and hospitalization rates decreased, while the incidence and hospitalizations due to unique PPV23 and NVP serotypes increased; this was consistent across all age groups. The greatest decrease in incidence (RR=0.4) and hospitalizations (RR=0.4) was observed in children <5 years with PCV13 serotypes. There were no distinct age-related trends observed for case fatality ratios; the highest CFR was observed in adults ≥65 years. Conclusion: A shift in serotype distribution was seen across all age groups; IPD incidence and hospitalization rates due to PCV13 serotypes decreased after PCV13 implementation, but this reduction was offset by the increasing burden and severity of unique PPV23 and NVP serotypes. As IPD continues to be a severe disease, continued surveillance is required to better understand the growing burden of these serotypes and emergence of non-vaccine-preventable serotypes.
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2007-2018年加拿大安大略省引入13价肺炎球菌结合疫苗后的血清型替换
简介:侵袭性肺炎球菌病(IPD)在加拿大安大略省是一种具有公共卫生意义的疾病,在那里,公共资助的肺炎球菌疫苗接种计划针对儿童、老年人和疾病高风险人群。自实施肺炎球菌结合疫苗(PCV)以来,已有血清型替代的记录,其中非PCV血清型取代了因疫苗可预防血清型减少而产生的生态位。我们的目标是通过评估12年(2007-2018年)期间的IPD负担,确定安大略省实施儿童13价(PCV13)计划以来是否存在血清型替代或IPD严重程度的变化。方法:我们纳入安大略省综合公共卫生信息系统(iPHIS)中报告的所有确诊IPD病例,并定义pcv13前时代(2007年1月- 2010年12月)和pcv13后时代(2011年1月- 2018年12月)。我们根据相关疫苗类型对IPD血清型进行分组:PCV13;23价多糖疫苗(独特的PPV23);和非疫苗可预防(NVP)。我们使用人口数据按年龄组、疫苗类型和年龄计算发病率和住院率(每10万人)。结果:后pcv13时代pcv13特异性发病率和住院率下降,而独特的PPV23和NVP血清型发病率和住院率上升;这在所有年龄组中都是一致的。PCV13血清型<5岁儿童的发病率(RR=0.4)和住院率(RR=0.4)下降最大。在病死率方面没有观察到明显的年龄相关趋势;CFR最高的是≥65岁的成年人。结论:血清型分布在所有年龄组中都发生了变化;实施PCV13后,由PCV13血清型引起的IPD发病率和住院率下降,但这种减少被独特的PPV23和NVP血清型增加的负担和严重程度所抵消。由于IPD仍然是一种严重疾病,需要继续进行监测,以更好地了解这些血清型日益增加的负担和非疫苗可预防血清型的出现。
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