Department of Clinical Sciences, Pediatrics, Umeå University, Umeå, Sweden.
Pediatr Infect Dis J. 2009 Oct;28(10):e276-82. doi: 10.1097/INF.0b013e3181b48ca3.
The immunogenicity of the 10-valent pneumococcal nontypeable Haemophilus influenzae protein D-conjugate vaccine (PHiD-CV) was determined following a simplified 2-dose priming and the more commonly employed 3-dose priming both followed by a booster dose.
A total of 351 healthy subjects were primed with PHiD-CV at either 3 and 5 or 3, 4 and 5 months of age followed in all subjects by a booster dose at 11 to 12 months of age. Serotype-specific pneumococcal responses were measured by 22F-inhibition ELISA and opsonophagocytic assays 1 month following primary and booster vaccinations.
Depending on the serotype, the percentages of subjects reaching the ELISA antibody threshold of 0.2 microg/mL were 92.8% to 98.0% following 2 primary doses and 96.1% to 100% following 3 primary doses except for serotype 6B (55.7% and 63.1%, respectively) and serotype 23F (69.3% and 77.6%, respectively). Opsonophagocytic activity (OPA) could be measured in 74.4% to 100% and 88.9% to 100% of the subjects after the 2-dose or 3-dose priming, respectively, except for serotype 1 (60.8% and 62.9%, respectively). In both groups, robust increases in ELISA antibodies and OPA titers were observed for all serotypes after the booster dose. Higher postprimary and postbooster ELISA antibody levels and OPA titers were observed for most serotypes following the 3+1 schedule.
PHiD-CV was immunogenic in both schedules, but further effectiveness data are needed to fully understand the public health benefit to be expected from these schedules in terms of prevention against invasive and mucosal infections.
在简化的 2 剂初免程序和更为常用的 3 剂初免程序之后,均进行了加强免疫,研究人员评估了 10 价肺炎球菌/无荚膜流感嗜血杆菌蛋白 D 结合疫苗(PHiD-CV)的免疫原性。
351 名健康受试者分别在 3 月龄和 5 月龄或 3、4、5 月龄时接种 PHiD-CV 进行初免,所有受试者均在 11 至 12 月龄时进行加强免疫。初免和加强免疫后 1 个月,通过 22F 抑制 ELISA 和调理吞噬试验检测血清型特异性肺炎球菌应答。
根据血清型的不同,在接受 2 剂初免后,达到 ELISA 抗体阈值(0.2μg/mL)的受试者百分比为 92.8%至 98.0%,接受 3 剂初免后为 96.1%至 100%,但血清型 6B(分别为 55.7%和 63.1%)和 23F(分别为 69.3%和 77.6%)除外。在接受 2 剂或 3 剂初免后,分别有 74.4%至 100%和 88.9%至 100%的受试者可检测到调理吞噬活性(OPA),但血清型 1 除外(分别为 60.8%和 62.9%)。在两组中,加强免疫后,所有血清型的 ELISA 抗体和 OPA 效价均显著增加。在 3+1 免疫程序中,大多数血清型的初免后和加强免疫后的 ELISA 抗体水平和 OPA 效价更高。
PHiD-CV 在两种免疫程序中均具有免疫原性,但需要进一步的有效性数据,以全面了解这些免疫程序在预防侵袭性和黏膜感染方面预期带来的公共卫生效益。
