利用减毒活轮状病毒疫苗(Rotarix™)作为感染挑战模型的初步研究。
A pilot study on use of live attenuated rotavirus vaccine (Rotarix™) as an infection challenge model.
机构信息
Research Division, Centre for Infectious Disease Research in Zambia, Lusaka, Zambia.
Research Division, Centre for Infectious Disease Research in Zambia, Lusaka, Zambia.
出版信息
Vaccine. 2020 Oct 27;38(46):7357-7362. doi: 10.1016/j.vaccine.2020.09.023. Epub 2020 Oct 5.
BACKGROUND
Rotavirus remains the commonest cause of dehydrating diarrhoea, particularly in developing countries. Human infection challenge studies in children in these countries offers an opportunity to rapidly evaluate new vaccine candidates that may have improved efficacy. We evaluated use of Rotarix™ as a live-attenuated challenge agent.
METHODS
We undertook an open label, exploratory study in infants receiving two standard doses of Rotarix™ at 6 and 10 weeks of age in a cohort of 22 Zambian infants. The first vaccine dose was considered as primary vaccination, and the second at day 28 as a live-attenuated virus challenge. Saliva, stool and serum samples were collected on days 0, 3, 5, 7, 14, and 28 following each dose. The primary outcome was stool shedding of rotavirus, determined by NSP2 qPCR. We calculated mean shedding index as average of natural logarithm of viral copies per gram of stool.
FINDINGS
After the first dose, viral shedding was high at day 3, peaked by day 5. After the second dose, viral shedding at day 3 was low and reduced gradually in most infants until day 14. Mean shedding index was significantly lower post dose 2 across all infants and timepoints (5.0 virus copies/g of stool [95%CI: 0.3-9.7] vs 10.4 virus copies/g of stool [95%CI: 6.2-14.6]; p-value < 0.0001; rho = 0.20, SD = 4.97. Seroconversion at day 28 was associated with a mean reduction of -1.03 (95%CI = -8.07, 6.01) in viral shedding after challenge dose but this was not statistically significant (p = 0.774). A borderline positive correlation between fold-change in IgA titre at day 28 from day 0 in saliva and serum was observed; Spearman's correlation coefficient, r = 0.69; p = 0.086.
INTERPRETATION
Shedding after the 'challenge' dose was reduced compared with the first dose, consistent with the induction of mucosal immunity by the first dose. This supports the use of Rotarix vaccine as a live-attenuated infection challenge.
FUNDING
Medical Research Council (UK) through the HIC-Vac Network.
背景
轮状病毒仍然是导致脱水性腹泻的最常见原因,特别是在发展中国家。在这些国家,对儿童进行人类感染挑战研究为快速评估新的候选疫苗提供了机会,这些疫苗可能具有更高的疗效。我们评估了 Rotarix™作为减毒活挑战剂的用途。
方法
我们在 22 名赞比亚婴儿的队列中进行了一项开放性、探索性研究,这些婴儿在 6 和 10 周龄时接受了两剂标准剂量的 Rotarix™。第一剂被认为是基础免疫,第二剂在第 28 天作为减毒活病毒挑战。在每次剂量后第 0、3、5、7、14 和 28 天收集唾液、粪便和血清样本。主要结局是通过 NSP2 qPCR 检测粪便中轮状病毒的脱落。我们计算了平均脱落指数,即粪便中病毒拷贝数的自然对数的平均值。
结果
在第一剂后,第 3 天病毒脱落量很高,第 5 天达到高峰。在第二剂后,第 3 天的病毒脱落量较低,大多数婴儿的病毒脱落量逐渐减少,直到第 14 天。所有婴儿和所有时间点的第 2 剂后平均脱落指数均显著降低(5.0 病毒拷贝/g 粪便[95%CI:0.3-9.7] vs 10.4 病毒拷贝/g 粪便[95%CI:6.2-14.6];p 值<0.0001;rho=0.20,SD=4.97)。第 28 天的血清转换与挑战剂量后病毒脱落的平均减少量-1.03(95%CI=-8.07,6.01)相关,但无统计学意义(p=0.774)。在唾液和血清中,第 28 天与第 0 天相比,IgA 滴度的变化呈正相关,Spearman 相关系数 r=0.69;p=0.086。
解释
与第一剂相比,“挑战”剂量后的脱落减少,这与第一剂诱导黏膜免疫一致。这支持将 Rotarix 疫苗用作减毒活感染挑战。
资金
英国医学研究理事会(通过 HIC-Vac 网络)。
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