SARS-CoV-2抗体升高可区分早期新冠病毒感染中的重症病例

Elevated SARS-CoV-2 Antibodies Distinguish Severe Disease in Early COVID-19 Infection.

作者信息

Haddad Natalie S, Nguyen Doan C, Kuruvilla Merin E, Morrison-Porter Andrea, Anam Fabliha, Cashman Kevin S, Ramonell Richard P, Kyu Shuya, Saini Ankur Singh, Cabrera-Mora Monica, Derrico Andrew, Alter David, Roback John D, Horwath Michael, O'Keefe James B, Wu Henry M, Ian Wong An-Kwok, Dretler Alexandra W, Gripaldo Ria, Lane Andrea N, Wu Hao, Lee Saeyun, Hernandez Mindy, Engineer Vanessa, Varghese John, Le Sang, Sanz Iñaki, Daiss John L, Eun-Hyung Lee F

出版信息

bioRxiv. 2020 Dec 6:2020.12.04.410589. doi: 10.1101/2020.12.04.410589.

DOI:10.1101/2020.12.04.410589

PMID:33299998

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7724666/

Abstract

BACKGROUND

SARS-CoV-2 has caused over 36,000,000 cases and 1,000,000 deaths globally. Comprehensive assessment of the multifaceted anti-viral antibody response is critical for diagnosis, differentiation of severe disease, and characterization of long-term immunity. Initial observations suggest that severe disease is associated with higher antibody levels and greater B cell/plasmablast responses. A multi-antigen immunoassay to define the complex serological landscape and clinical associations is essential.

METHODS

We developed a multiplex immunoassay and evaluated serum/plasma from adults with RT-PCR-confirmed SARS-CoV-2 infections during acute illness (N=52) and convalescence (N=69); and pre-pandemic (N=106) and post-pandemic (N=137) healthy adults. We measured IgA, IgG, and/or IgM against SARS-CoV-2 Nucleocapsid (N), Spike domain 1 (S1), receptor binding domain (S1-RBD) and S1-N-terminal domain (S1-NTD).

RESULTS

To diagnose infection, the combined [IgA+IgG+IgM] or IgG for N, S1, and S1-RBD yielded AUC values -0.90 by ROC curves. From days 6-30 post-symptom onset, the levels of antigen-specific IgG, IgA or [IgA+IgG+IgM] were higher in patients with severe/critical compared to mild/moderate infections. Consistent with excessive concentrations of antibodies, a strong prozone effect was observed in sera from severe/critical patients. Notably, mild/moderate patients displayed a slower rise and lower peak in anti-N and anti-S1 IgG levels compared to severe/critical patients, but anti-RBD IgG and neutralization responses reached similar levels at 2-4 months.

CONCLUSION

This SARS-CoV-2 multiplex immunoassay measures the magnitude, complexity and kinetics of the antibody response against multiple viral antigens. The IgG and combined-isotype SARS-CoV-2 multiplex assay is highly diagnostic of acute and convalescent disease and may prognosticate severity early in illness.

ONE SENTENCE SUMMARY

In contrast to patients with moderate infections, those with severe COVID-19 develop prominent, early antibody responses to S1 and N proteins.

摘要

背景

新型冠状病毒2（SARS-CoV-2）已在全球导致超过3600万例感染和100万人死亡。全面评估多方面的抗病毒抗体反应对于诊断、区分重症疾病以及确定长期免疫力的特征至关重要。初步观察表明，重症疾病与更高的抗体水平和更强的B细胞/浆母细胞反应相关。采用多抗原免疫测定法来确定复杂的血清学情况及临床关联至关重要。

方法

我们开发了一种多重免疫测定法，并对急性疾病期间（N = 52）和恢复期（N = 69）经逆转录聚合酶链反应（RT-PCR）确诊为SARS-CoV-2感染的成年人以及大流行前（N = 106）和大流行后（N = 137）的健康成年人的血清/血浆进行了评估。我们检测了针对SARS-CoV-2核衣壳（N）、刺突蛋白结构域1（S1）、受体结合结构域（S1-RBD）和S1-N端结构域（S1-NTD）的IgA、IgG和/或IgM。

结果

为诊断感染，针对N、S1和S1-RBD的[IgA + IgG + IgM]组合或IgG通过ROC曲线得出的AUC值为-0.90。在症状出现后的第6至30天，与轻度/中度感染患者相比，重症/危重症患者的抗原特异性IgG、IgA或[IgA + IgG + IgM]水平更高。与抗体浓度过高一致，在重症/危重症患者的血清中观察到强烈的前带效应。值得注意的是，与重症/危重症患者相比，轻度/中度患者的抗N和抗S1 IgG水平上升较慢且峰值较低，但抗RBD IgG和中和反应在2至4个月时达到相似水平。