痊愈者 12 个月内的 SARS-CoV-2 体液免疫反应揭示了严重程度依赖性抗体的动态变化

Maisey Schuler, Nadia Siles, Cole Maguire, Dzifa Amengor, Annalee Nguyen, Rebecca Wilen, Jacob Rogers, Sam Bazzi, Blaine Caslin, Christopher DiPasquale, Melissa Abigania, Eric Olson, Janelle Creaturo, Kerin Hurley, Todd A. Triplett, Justin F. Rousseau, Stephen M. Strakowski, Dennis Wylie, Jennifer Maynard, Lauren I. R. Ehrlich, Esther Melamed
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Methods\nWe evaluated antibody titers against SARS-CoV-2 nucleocapsid (N), spike (S), and receptor binding domain (RBD) of spike in 98 convalescent participants who experienced asymptomatic, mild, moderate or severe COVID-19 disease and in 17 non-vaccinated, non-infected controls, using four different antibody assays. Participants were sampled longitudinally at 1, 3, 6, and 12 months post-SARS-CoV-2 positive PCR test. Findings\nIncreasing acute COVID-19 disease severity correlated with higher anti-N and anti-RBD antibody titers throughout 12 months post-infection. Anti-N and anti-RBD titers declined over time in all participants, with the exception of increased anti-RBD titers post-vaccination, and the decay rates were faster in hospitalized compared to non-hospitalized participants. <50% of participants retained anti-N titers above control levels at 12 months, with non-hospitalized participants falling below control levels sooner. Nearly all hospitalized and non-hospitalized participants maintained anti-RBD titers above controls for up to 12 months, suggesting longevity of protection against severe reinfections. Nonetheless, by 6 months, few participants retained >50% of their 1-month anti-N or anti-RBD titers. Vaccine-induced increases in anti-RBD titers were greater in non-hospitalized relative to hospitalized participants. Early convalescent antibody titers correlated with age, but no association was observed between Post-Acute Sequelae of SARS-CoV-2 infection (PASC) status or acute steroid treatment and convalescent antibody titers. Interpretation\nHospitalized participants developed higher anti-SARS-CoV-2 antibody titers relative to non-hospitalized participants, a difference that persisted throughout 12 months, despite the faster decline in titers in hospitalized participants. 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摘要

摘要背景了解 SARS-CoV-2 抗体反应的动力学和持续时间对于制定减少 2019 年冠状病毒病(COVID-19)再感染的策略以及改进疫苗接种和治疗方法至关重要。方法我们使用四种不同的抗体检测方法评估了98名经历过无症状、轻度、中度或重度COVID-19疾病的康复者和17名未接种疫苗、未感染的对照者体内针对SARS-CoV-2核壳(N)、尖峰(S)和尖峰受体结合域(RBD)的抗体滴度。在 SARS-CoV-2 PCR 检测呈阳性后的 1、3、6 和 12 个月对参与者进行纵向采样。研究结果在感染后的 12 个月内,COVID-19 急性疾病严重程度的增加与抗 N 和抗 RBD 抗体滴度的升高相关。随着时间的推移,所有参与者的抗N和抗RBD滴度都在下降,但接种疫苗后抗RBD滴度上升的情况除外,而且与非住院参与者相比,住院参与者的下降速度更快。 50%的参与者在12个月时抗N滴度仍高于控制水平,而非住院参与者则更早降至控制水平以下。几乎所有住院和非住院参与者的抗RBD滴度在12个月内都保持在对照水平以上,这表明抗严重再感染的保护作用是持久的。然而,到 6 个月时,几乎没有人的抗 N 滴度或抗 RBD 滴度能保持在 1 个月时的 50%。疫苗引起的抗 RBD 滴度增加在未住院参与者中比住院参与者中更大。早期恢复期抗体滴度与年龄有关,但在SARS-CoV-2感染急性后遗症(PASC)状态或急性类固醇治疗与恢复期抗体滴度之间没有观察到任何关联。解释:与非住院参与者相比,住院参与者的抗 SARS-CoV-2 抗体滴度较高,尽管住院参与者的滴度下降较快,但这种差异在 12 个月内持续存在。在两组参与者中,至少有一半人的抗 N 滴度下降到了控制水平以下,但几乎所有参与者的抗 RBD 滴度在 12 个月内都保持在控制水平以上,这表明产生了长效抗体反应,而众所周知,长效抗体反应与 COVID-19 不同严重程度的重症保护相关。总之,我们的研究结果有助于加深人们对 COVID-19 抗体动态的了解。资助机构:奥斯汀公共卫生局、美国国立卫生研究院、巴布森诊断公司、戴尔医学院创业公司。
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SARS-CoV-2 Humoral Immune Responses in Convalescent Individuals Over 12 Months Reveal Severity-Dependent Antibody Dynamics
Abstract Background Understanding the kinetics and longevity of antibody responses to SARS-CoV-2 is critical to informing strategies toward reducing Coronavirus disease 2019 (COVID-19) reinfections, and improving vaccination and therapy approaches. Methods We evaluated antibody titers against SARS-CoV-2 nucleocapsid (N), spike (S), and receptor binding domain (RBD) of spike in 98 convalescent participants who experienced asymptomatic, mild, moderate or severe COVID-19 disease and in 17 non-vaccinated, non-infected controls, using four different antibody assays. Participants were sampled longitudinally at 1, 3, 6, and 12 months post-SARS-CoV-2 positive PCR test. Findings Increasing acute COVID-19 disease severity correlated with higher anti-N and anti-RBD antibody titers throughout 12 months post-infection. Anti-N and anti-RBD titers declined over time in all participants, with the exception of increased anti-RBD titers post-vaccination, and the decay rates were faster in hospitalized compared to non-hospitalized participants. <50% of participants retained anti-N titers above control levels at 12 months, with non-hospitalized participants falling below control levels sooner. Nearly all hospitalized and non-hospitalized participants maintained anti-RBD titers above controls for up to 12 months, suggesting longevity of protection against severe reinfections. Nonetheless, by 6 months, few participants retained >50% of their 1-month anti-N or anti-RBD titers. Vaccine-induced increases in anti-RBD titers were greater in non-hospitalized relative to hospitalized participants. Early convalescent antibody titers correlated with age, but no association was observed between Post-Acute Sequelae of SARS-CoV-2 infection (PASC) status or acute steroid treatment and convalescent antibody titers. Interpretation Hospitalized participants developed higher anti-SARS-CoV-2 antibody titers relative to non-hospitalized participants, a difference that persisted throughout 12 months, despite the faster decline in titers in hospitalized participants. In both groups, while anti-N titers fell below control levels for at least half of the participants, anti-RBD titers remained above control levels for almost all participants over 12 months, demonstrating generation of long-lived antibody responses known to correlate with protection from severe disease across COVID-19 severities. Overall, our findings contribute to the evolving understanding of COVID-19 antibody dynamics. Funding Austin Public Health, NIAAA, Babson Diagnostics, Dell Medical School Startup.
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