巴西儿童普遍接种 10 价肺炎球菌结合疫苗后血清型 19A 肺炎链球菌群体遗传结构的变化。

Jailton L C Lima, Amanda B da Silva, Amanda S Cabral, Filipe M de Miranda, Lívia D da Silva, André R A da Silva, Lúcia M Teixeira, Felipe P G Neves
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引用次数: 0

摘要

背景:2010 年在全国儿童免疫接种中引入 10 价肺炎球菌结合疫苗 (PCV10)后,疫苗血清型在青少年中的定植率和侵袭性肺炎球菌疾病 (IPD) 显著下降。然而,非疫苗血清型已经出现,血清型 19A 现在是巴西 IPD 的主要病因:我们分析了从 2010 年至 2023 年期间在巴西里约热内卢州不同医疗机构就诊的儿童和成人中分离出的 32 例血清型 19A 肺炎链球菌。分离物的菌盖类型是通过连续多重 PCR 或 cpsB 基因测序确定的。所有分离株都进行了抗菌药敏感性测试和多反应序列检测:结果:在 32 株血清型 19A 分离物中,29 株(90.6%)从 5 岁以下儿童中分离出来,3 株(9.4%)从成人中分离出来。19个(59.4%)分离株与定植有关,13个(40.6%)分离株来自疾病。所有分离株都对氯霉素、左氧氟沙星、利奈唑胺、利福平和万古霉素敏感。对磺胺甲噁唑-三甲氧苄啶(30 人;93.8%)、青霉素(24 人;75%)和红霉素(23 人;71.9%)的非敏感性(中间型+耐药型)频率最高。22个分离株(68.8%)对多种药物具有耐药性(MDR)。青霉素不敏感肺炎球菌(PNSP)的青霉素 MIC 介于 0.12 至 8.0 μg/mL 之间。红霉素的 MIC 为 0.064 至大于 256 μg/mL。头孢曲松的 MIC 为 0.023 至 4 μg/mL。最常见的基因系为 ST733(n = 7;21.9%)和 CC320(n = 25;78.1%),前者大多出现在 PCV10 引入之前和引入初期,后者大多出现在 PCV10 引入后期。CC320 中的所有 25 个分离株均为 PNSP,且大部分(n = 22; 88 %)为 MDR:我们观察到,在长期使用 PCV(主要是 PCV10)进行儿童常规免疫接种后,抗菌药敏感性谱系和基因系发生了变化,其特点是 MDR 系 CC320 的克隆扩增。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Changes in population genetic structure of serotype 19A Streptococcus pneumoniae after universal childhood use of the 10-valent pneumococcal conjugate vaccine in Brazil.

Background: The introduction of the 10-valent pneumococcal conjugate vaccine (PCV10) for nationwide childhood immunization in 2010 led to a significant reduction in colonization and invasive pneumococcal disease (IPD) by vaccine serotypes in young. However, non-vaccine serotypes have emerged, and serotype 19A is now the leading cause of IPD in Brazil.

Methods: We analyzed 32 serotype 19A isolates of Streptococcus pneumoniae recovered from children and adults who attended different health facilities in the state of Rio de Janeiro, Brazil, between 2010 and 2023. The capsular types of the isolates were determined by sequential multiplex PCR or by cpsB gene sequencing. All isolates were subjected to antimicrobial susceptibility testing and MLST.

Results: Of the 32 serotype 19A isolates, 29 (90.6 %) isolates were recovered from children aged ≤5 years and three (9.4 %) isolates were recovered from adults. Nineteen (59.4 %) isolates were associated with colonization, and 13 (40.6 %) isolates were from diseases. All isolates were susceptible to chloramphenicol, levofloxacin, linezolid, rifampin, and vancomycin. The highest frequencies of non-susceptibility (intermediate + resistant) were observed for sulfamethoxazole-trimethoprim (n = 30; 93.8 %), penicillin (n = 24; 75 %), and erythromycin (n = 23; 71.9 %). Twenty-two (68.8 %) isolates were multidrug resistant (MDR). MICs for penicillin among penicillin-non-susceptible pneumococci (PNSP) ranged from 0.12 to 8.0 μg/mL. MICs for erythromycin ranged from 0.064 to >256 μg/mL. MICs for ceftriaxone ranged from 0.023 to 4 μg/mL. The most common genetic lineages were ST733 (n = 7; 21.9 %), mostly found before and in the early years of PCV10 introduction, and CC320 (n = 25; 78.1 %), mostly found in the late-PCV10 period. All 25 isolates within CC320 were PNSP and mostly (n = 22; 88 %) MDR.

Conclusions: We observed a shift in antimicrobial susceptibility profiles and genetic lineages after long-term use of PCV, mostly PCV10, for routine childhood immunization, characterized by clonal expansion of the MDR lineage CC320.

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