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Genetic Diversity of Meningococcal Serogroup B Vaccine Antigens among Carriage Isolates Collected from Students at Three Universities in the United States 2015–2016

机译:脑膜炎球菌血清血清群B疫苗抗原在美国三所大学中学生中收集的支架分离疫苗抗原的遗传多样性2015-2016

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摘要

Carriage evaluations were conducted during 2015 to 2016 at two U.S. universities in conjunction with the response to disease outbreaks caused by Neisseria meningitidis serogroup B and at a university where outbreak and response activities had not occurred. All eligible students at the two universities received the serogroup B meningococcal factor H binding protein vaccine (MenB-FHbp); 5.2% of students (181/3,509) at one university received MenB-4C. A total of 1,514 meningococcal carriage isolates were obtained from 8,905 oropharyngeal swabs from 7,001 unique participants. Whole-genome sequencing data were analyzed to understand MenB-FHbp’s impact on carriage and antigen genetic diversity and distribution. Of 1,422 isolates from carriers with known vaccination status (726 [51.0%] from MenB-FHbp-vaccinated, 42 [3.0%] from MenB-4C-vaccinated, and 654 [46.0%] from unvaccinated participants), 1,406 (98.9%) had intact fHbp alleles (716 from MenB-FHbp-vaccinated participants). Of 726 isolates from MenB-FHbp-vaccinated participants, 250 (34.4%) harbored FHbp peptides that may be covered by MenB-FHbp. Genogroup B was detected in 122/1,422 (8.6%) and 112/1,422 (7.9%) isolates from MenB-FHbp-vaccinated and unvaccinated participants, respectively. FHbp subfamily and peptide distributions between MenB-FHbp-vaccinated and unvaccinated participants were not statistically different. Eighteen of 161 MenB-FHbp-vaccinated repeat carriers (11.2%) acquired a new strain containing one or more new vaccine antigen peptides during multiple rounds of sample collection, which was not statistically different (P = 0.3176) from the unvaccinated repeat carriers (1/30; 3.3%). Our findings suggest that lack of MenB vaccine impact on carriage was not due to missing the intact fHbp gene; MenB-FHbp did not affect antigen genetic diversity and distribution during the study period.
机译:在2015年至2016年,在两所美国大学期间进行了运输评估,与疾病爆发的反应结合诸如爆发和反应活动的疾病爆发造成的疾病爆发。两所大学的所有符合条件的学生都接受了血清群体B脑膜炎因子H结合蛋白质疫苗(MENB-FHBP);一所大学的5.2%的学生(181/3,509)收到MENB-4C。从7,001名独特参与者的8,905名口咽拭子中获得了总共1,514个脑膜炎术载体分离物。分析全基因组测序数据以了解MeNB-FHBP对携带和抗原遗传多样性和分布的影响。来自具有已知疫苗接种状态的载体的1,422个分离物(726 [51.0%]来自MeNB-FHBP接种疫苗,42 [3.0%]来自MeNB-4C接种疫苗,来自未接触的参与者的654 [46.0%]),1,406(98.9%)完整的FHBP等位基因(716来自Menb-FHBP接种的参与者)。 726个分离株来自MeNB-FHBP接种的参与者,250(34.4%)可能被MENB-FHBP覆盖的患者含有覆盖的FHBP肽。在122 / 1,422(8.6%)和112 / 1,422(7.9%)分别检测到GenoGroup B分别从MeNB-FHBP接种疫苗和未接受的参与者分离。 MeNB-FHBP接种和未接受的参与者之间的FHBP亚家族和肽分布并没有统计学不同。 161个MeNB-FHBP接种的重复载体(11.2%)在多轮样品收集期间获得含有一种或多种新疫苗抗原肽的新菌株,其从未涂上的重复载体(1)没有统计学上不同(P = 0.3176) / 30; 3.3%)。我们的研究结果表明,缺乏对托架的疫苗造成的影响不是由于缺少完整的FHBP基因; MENB-FHBP在研究期间没有影响抗原遗传多样性和分布。

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