From the *Respiratory Diseases Branch, Division of Bacterial Diseases, National Center for Immunizations and Respiratory Diseases, Centers for Disease Control and Prevention, Atlanta, GA; †Westat Inc., Rockville, MD; ‡Epidemic Intelligence Service, Centers for Disease Control and Prevention, Atlanta, GA; §International Vaccine Access Center, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD; and ¶Institute for Child Health, University College London, London, United Kingdom.
Pediatr Infect Dis J. 2014 Jan;33 Suppl 2(Suppl 2 Optimum Dosing of Pneumococcal Conjugate Vaccine For Infants 0 A Landscape Analysis of Evidence Supportin g Different Schedules):S109-18. doi: 10.1097/INF.0000000000000078.
Pneumococcal conjugate vaccines (PCV) are being implemented globally using a variety of different schedules. The optimal schedule to maximize protection of vaccinated children against vaccine-type invasive pneumococcal disease (VT-IPD) is not known.
To assess the relative benefit of various PCV dosing schedules, we conducted a systematic review of studies published in English from 1994 to 2010 (supplemented post hoc with studies from 2011) on PCV effectiveness against VT-IPD among children targeted to receive vaccine. Data on 2-dose and 3-dose primary series, both with and without a booster ("2+0," "2+1," "3+0" and "3+1"), were included. For observational studies using surveillance data or case counts, we calculated percentage reduction in VT-IPD before and after PCV introduction.
Of 4 randomized controlled trials and 31 observational studies reporting VT-IPD among young children, none evaluated a 2+0 complete series, 7 (19%) evaluated 2+1, 4 (11%) 3+0 and 27 (75%) 3+1. Most (86%) studies were from North America or Europe. Only 1 study (observational) directly compared 2 schedules (3+0 vs. 3+1); results supported the use of a booster dose. In clinical trials, vaccine efficacy ranged from 65% to 71% with 3+0 and 83% to 94% with 3+1. Surveillance data and case counts demonstrate reductions in VT-IPD of up to 100% with 2+1 (6 studies) or 3+1 (17 studies) schedules and up to 90% with 3+0 (2 studies). Reductions were observed as early as 1 year after PCV introduction.
These data support the use of 2+1, 3+0 and 3+1 schedules, although most data of PCV impact on VT-IPD among young children are from high-income countries using 3+1. Differences between schedules for impact on VT-IPD are difficult to discern based on available data.
肺炎球菌结合疫苗(PCV)正在全球范围内使用各种不同的方案进行推广。目前尚不清楚哪种方案能最大限度地保护接种儿童免受疫苗相关侵袭性肺炎球菌病(VT-IPD)的侵害。
为了评估各种 PCV 剂量方案的相对益处,我们对 1994 年至 2010 年期间(事后补充了 2011 年的研究)以目标接种儿童为对象、评估 PCV 对 VT-IPD 有效性的研究进行了系统综述。纳入了关于 2 剂和 3 剂基础免疫系列(含和不含加强针),即“2+0”、“2+1”、“3+0”和“3+1”的研究数据。对于采用监测数据或病例计数的观察性研究,我们计算了 PCV 引入前后 VT-IPD 的减少百分比。
在 4 项随机对照试验和 31 项报告幼儿 VT-IPD 的观察性研究中,没有一项评估 2+0 完全系列,7 项(19%)评估 2+1,4 项(11%)评估 3+0,27 项(75%)评估 3+1。大多数(86%)研究来自北美或欧洲。只有 1 项研究(观察性)直接比较了 2 种方案(3+0 与 3+1);结果支持使用加强针。在临床试验中,3+0 方案的疫苗效力为 65%至 71%,3+1 方案为 83%至 94%。监测数据和病例计数显示,2+1(6 项研究)或 3+1(17 项研究)方案可使 VT-IPD 减少高达 100%,3+0(2 项研究)方案可使 VT-IPD 减少高达 90%。在 PCV 引入后 1 年内即可观察到减少。
这些数据支持使用 2+1、3+0 和 3+1 方案,尽管大多数关于 PCV 对幼儿 VT-IPD 影响的数据来自于使用 3+1 方案的高收入国家。根据现有数据,难以区分方案之间对 VT-IPD 的影响差异。
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