血清转化为SARS-CoV-2后再感染的风险:一项基于人群的倾向评分匹配队列研究

A. Leidi, F. Koegler, R. Dumont, Richard Dubos, M. Zaballa, G. Piumatti, M. Coen, Amandine Berner, P. Darbellay Farhoumand, P. Vetter, N. Vuilleumier, L. Kaiser, D. Courvoisier, A. Azman, I. Guessous, S. Stringhini
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引用次数: 40

摘要

重要性:检测严重急性呼吸综合征冠状病毒2 (SARS-CoV-2)感染后产生的针对Spike蛋白的特异性IgG抗体的血清学检测正在广泛应用于研究和临床实践。然而,免疫反应对未来感染的保护持续时间和有效性仍需在大量人群中进行评估。目的:与血清阴性对照相比,估计以人群为基础的样本中血清阳性个体新获得性SARS-CoV-2感染的发生率。设计:回顾性纵向倾向评分匹配队列研究。背景:在第一波大流行之后的2020年4月至6月期间,在日内瓦州(瑞士)进行了一项血清流行率调查,包括以人群为基础的人口代表性样本。纳入血清流行率调查的每个人都与国家集中登记处联系起来,该登记处汇编了自大流行开始以来病毒学证实的SARS-CoV-2感染情况。参与者:使用包括年龄、性别、免疫缺陷、体重指数、吸烟状况和教育水平在内的倾向评分,将12岁及以上的抗刺长IgG抗体与血清阴性对照进行1:2匹配。暴露:SARS-CoV-2血清阳性。主要结局和措施:我们的主要结局是病毒学确诊的SARS-CoV-2感染,从2020年4月至6月的血清学状态评估到第二波大流行结束(2021年1月)。此外,还分析了感染率、检测率和阳性检测比例。结果:在8344名血清调查参与者中,筛选出498名血清阳性个体,并与996名血清阴性对照进行配对。平均随访35.6周(标准差:3.2)后,498例血清阳性受试者中有7例(1.4%)出现SARS-CoV-2检测阳性,其中5例(1.0%)被认为是再感染。相比之下,在34.7 (SD 3.2)周的平均随访期间,血清阴性个体的感染率明显更高(15.5%,154/996),对应于血清阳性受试者的SARS-CoV-2检测阳性的危险降低94% (95%CI 86%至98%,P<0.001)。结论及相关性:SARS-CoV-2感染后血清转化对持续至少8个月的病毒污染具有保护作用。这些发现可以帮助全球卫生当局确定疫苗分配的优先次序。
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Risk of reinfection after seroconversion to SARS-CoV-2: A population-based propensity-score matched cohort study
Importance: Serological assays detecting specific IgG antibodies generated against the Spike protein following Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection are being widely deployed in research studies and clinical practice. However, the duration and the effectiveness of the protection conferred by the immune response against future infection remains to be assessed in a large population. Objective: To estimate the incidence of newly acquired SARS-CoV-2 infections in seropositiveindividuals from a population-based sample as compared to seronegative controls. Design: Retrospective longitudinal propensity-score matched cohort study. Setting: A seroprevalence survey including a population-based representative sample of the population from the canton of Geneva (Switzerland) was conducted between April and June 2020, immediately after the first pandemic wave. Each individual included in the seroprevalence survey was linked to a state centralized registry compiling virologically confirmed SARS-CoV-2 infections since the beginning of the pandemic. Participants: Participants aged twelve years old and over, who developed anti-spike IgG antibodies were matched one-to-two to seronegative controls, using a propensity-score including age, gender, immunodeficiency, body mass index, smoking status and education level. Exposure: SARS-CoV-2 seropositivity. Main outcomes and measures: Our primary outcome was virologically confirmed SARS-CoV-2 infections which occurred from serological status assessment in April-June 2020 to the end of the second pandemic wave (January 2021). Additionally, incidence of infections, rate of testing and proportion of positive tests were analysed. Results: Among 8344 serosurvey participants, 498 seropositive individuals were selected and matched with 996 seronegative controls. After a mean follow-up of 35.6 (Standard Deviation, SD: 3.2) weeks, 7 out of 498 (1.4%) seropositive subjects had a positive SARS-CoV-2 test, of which 5 (1.0%) were considered as reinfections. By contrast, infection rate was significantly higher in seronegative individuals (15.5%, 154/996) during a similar mean follow-up of 34.7 (SD 3.2) weeks, corresponding to a 94% (95%CI 86% to 98%, P<0.001) reduction in the hazard of having a positive SARS-CoV-2 test for seropositive subjects. Conclusions and relevance: Seroconversion after SARS-CoV-2 infection confers protection to successive viral contamination lasting at least 8 months. These findings could help global health authorities establishing priority for vaccine allocation.
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