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BA.5 奥密克戎亚变体再感染风险、疫苗保护效力和感染严重程度:丹麦全国基于人群的研究。

Risk of reinfection, vaccine protection, and severity of infection with the BA.5 omicron subvariant: a nation-wide population-based study in Denmark.

机构信息

Department of Infectious Disease Epidemiology and Prevention, Statens Serum Institut, Copenhagen, Denmark; Medical Reseasrch Council International Statistics and Epidemiology Group, London School of Hygiene & Tropical Medicine, London, UK.

Department of Infectious Disease Epidemiology and Prevention, Statens Serum Institut, Copenhagen, Denmark.

出版信息

Lancet Infect Dis. 2023 Feb;23(2):167-176. doi: 10.1016/S1473-3099(22)00595-3. Epub 2022 Oct 18.

Abstract

BACKGROUND

Estimates of immunity and severity for the SARS-CoV-2 omicron subvariant BA.5 are important to assess the public health impact associated with its rapid global spread despite vaccination. We estimated natural and vaccine immunity and severity of BA.5 relative to BA.2 in Denmark, a country with high mRNA-vaccination coverage and free-of-charge RT-PCR testing.

METHODS

This nation-wide population-based study in Denmark included residents aged 18 years or older who had taken an RT-PCR test between 10 April and 30 June, 2022 (ie, the outcome period), and who the national COVID-19 surveillance system identified as having information since February 2020 on RT-PCR tests, whole-genome sequencing, vaccinations, and hospitalisation with a positive RT-PCR test and COVID-19 as the main diagnosis. First, we used a case-control design, in which cases were people infected with BA.5 or BA.2 during the outcome period and controls were people who tested negative for SARS-CoV-2 infection during the outcome period. We calculated the protection provided by a previous PCR-confirmed omicron infection against BA.5 and BA.2 infection and hospitalisation among triple-vaccinated individuals. Second, we compared vaccination status in people infected with BA.5 versus BA.2 and estimated relative vaccine protection against each subvariant. Third, we compared rates of hospitalisation for COVID-19 among people infected with BA.5 versus BA.2. We estimated effects using logistic regression with adjustment for sex, age, region, PCR-test date, comorbidity and, as appropriate, vaccination and previous infection status.

FINDINGS

A total of 210 (2·4%) of 8678 of BA.5 cases, 192 (0·7%) of 29 292 of BA.2 cases, and 33 972 (19·0%) of 178 669 PCR-negative controls previously had an omicron infection, which was estimated in the adjusted analyses to offer 92·7% (95% CI 91·6-93·7) protection against BA.5 infection and 97·1% (96·6-97·5) protection against BA.2 infection. We found similarly high amounts of protection against hospitalisation owing to infection with BA.5 (96·4% [95% CI 74·2-99·5]) and BA.2 (91·2% [76·3-96·7]). Vaccine coverage (three mRNA doses vs none) was 9307 (94·2%) of 9878 among BA.5 cases and 30 581 (94·8%) of 32 272 among BA.2 cases, although in the adjusted analysis, there was a trend towards slightly higher vaccination coverage among BA.5 cases than BA.2 cases (OR 1·18 [95% CI 0·99-1·42]; p=0·064), possibly suggesting marginally poorer vaccine protection against BA.5. The rate of hospitalisation due to COVID-19 was higher among the BA.5 cases (210 [1·9%] of 11 314) than among the BA.2 cases (514 [1·4%] of 36 805), with an OR of 1·34 (95% CI 1·14-1·57) and an adjusted OR of 1·69 (95% CI 1·22-2·33), despite low and stable COVID-19 hospitalisation numbers during the study period.

INTERPRETATION

The study provides evidence that a previous omicron infection in triple-vaccinated individuals provides high amounts of protection against BA.5 and BA.2 infections. However, protection estimates greater than 90% might be too high if individuals with a previous infection were more likely than those without one to come forward for a test for reasons other than suspicion of COVID-19. Our analysis also showed that vaccine protection against BA.5 infection was similar to, or slightly weaker than, protection against BA.2 infection. Finally, there was evidence that BA.5 infections were associated with an increased risk of hospitalisation compared with BA.2 infections.

FUNDING

There was no funding source for this study.

摘要

背景

评估 SARS-CoV-2 奥密克戎变异株 BA.5 的免疫和严重程度对于评估其在全球迅速传播的情况下对公共卫生的影响非常重要,尽管有疫苗接种。我们在丹麦评估了 BA.5 相对于 BA.2 的自然和疫苗免疫以及严重程度,丹麦的 mRNA 疫苗接种率很高,并且免费提供 RT-PCR 检测。

方法

这项全国性的基于人群的研究在丹麦进行,包括在 2022 年 4 月 10 日至 6 月 30 日期间接受过 RT-PCR 检测的年龄在 18 岁或以上的居民,以及国家 COVID-19 监测系统自 2020 年 2 月以来确定的有 RT-PCR 检测、全基因组测序、疫苗接种和因阳性 RT-PCR 检测和 COVID-19 而住院的信息的人群。首先,我们使用病例对照设计,其中病例是在结果期间感染 BA.5 或 BA.2 的人,对照组是在结果期间 RT-PCR 检测结果为阴性的人。我们计算了先前经 PCR 确认的奥密克戎感染对 BA.5 和 BA.2 感染和三重接种人群住院的保护作用。其次,我们比较了感染 BA.5 与 BA.2 的人群的疫苗接种情况,并估计了每种亚变异体的相对疫苗保护作用。第三,我们比较了感染 BA.5 与 BA.2 的人群的 COVID-19 住院率。我们使用逻辑回归进行效应估计,并对性别、年龄、地区、PCR 检测日期、合并症以及适当的疫苗接种和先前感染状态进行了调整。

结果

在 210 例 BA.5 病例(2.4%)、192 例 BA.2 病例(0.7%)和 33972 例 PCR 阴性对照(19.0%)中,先前有过奥密克戎感染,调整分析估计,这种感染对 BA.5 感染的保护率为 92.7%(95%CI 91.6-93.7),对 BA.2 感染的保护率为 97.1%(96.6-97.5)。我们还发现,感染 BA.5(96.4%[95%CI 74.2-99.5])和 BA.2(91.2%[76.3-96.7])导致住院的保护作用也很高。疫苗接种率(三剂 mRNA 疫苗与无疫苗)在 BA.5 病例中为 9307(94.2%),在 BA.2 病例中为 30581(94.8%),尽管在调整分析中,BA.5 病例的疫苗接种率略有上升趋势高于 BA.2 病例(比值比 1.18[95%CI 0.99-1.42];p=0.064),这可能表明 BA.5 的疫苗保护作用略有下降。BA.5 病例(11314 例中有 210 例[1.9%])的 COVID-19 住院率高于 BA.2 病例(36805 例中有 514 例[1.4%]),比值比为 1.34(95%CI 1.14-1.57),调整后的比值比为 1.69(95%CI 1.22-2.33),尽管在研究期间 COVID-19 的住院人数较低且稳定。

解释

这项研究提供了证据,表明三重接种的个体以前感染过奥密克戎,对 BA.5 和 BA.2 感染提供了高度的保护。然而,如果以前感染过的个体比没有感染过的个体更有可能因为怀疑 COVID-19 以外的原因而接受检测,那么估计超过 90%的保护率可能过高。我们的分析还表明,BA.5 感染的疫苗保护作用与 BA.2 感染的保护作用相似,或者略弱。最后,有证据表明 BA.5 感染与 BA.2 感染相比,住院风险增加。

资助

本研究没有资金来源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1df/9578720/75d2c9b28947/gr1_lrg.jpg

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