Spike and nucleocapsid antibody dynamics following SARS-CoV-2 infection and vaccination: Implications for sourcing COVID-19 convalescent plasma from routinely collected blood donations.

IF 2.5 3区 医学 Q2 HEMATOLOGY Transfusion Pub Date : 2024-10-07 DOI:10.1111/trf.18017
Clara Di Germanio, Xutao Deng, Brendan G Balasko, Graham Simmons, Rachel Martinelli, Eduard Grebe, Mars Stone, Bryan R Spencer, Paula Saa, Elaine A Yu, Marion C Lanteri, Valerie Green, David Wright, Isaac Lartey, Steven Kleinman, Jefferson Jones, Brad J Biggerstaff, Paul Contestable, Michael P Busch
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Abstract

Background: COVID-19 convalescent plasma (CCP) remains a treatment option for immunocompromised patients; however, the current FDA qualification threshold of ≥200 BAU/mL of spike antibody appears to be relatively low. We evaluated the levels of binding (bAb) and neutralizing antibodies (nAb) on serial samples from repeat blood donors who were vaccinated and/or infected to inform criteria for qualifying CCP from routinely collected plasma components.

Methods: Donors were categorized into four groups: (1) infected, then vaccinated, (2) vaccinated then infected during the delta, or (3) omicron waves, (4) vaccinated without infection. IgG Spike and total Nuclecapsid bAb were measured, along with S variants and nAb titers using reporter viral particle neutralization.

Results: Mean S IgG bAb peaks after infection alone were lower than after primary and booster vaccinations, and higher after delta and omicron infection in previously vaccinated donors. Half-lives for S IgG ranged from 34 to 66 days after first infection/vaccination events and up to 108 days after second events. The levels of S IgG bAb and nAb were similar across different variants, except for omicron, which were lower. Better correlations of nAb with bAb were observed at higher levels (hybrid immunity) than at the current FDA CCP qualifying threshold.

Discussion: Routine plasma donations from donors with hybrid immunity had high S bAb and potent neutralizing activity for 3-6 months after infection. In donations with high (>4000 BAU/mL) S IgG, >95% had high nAb titers (>500) against ancestral and variant S, regardless of COVID-19 symptoms. These findings provide the basis for test-based criteria for qualifying CCP from routine blood donations.

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感染 SARS-CoV-2 和接种疫苗后的尖峰抗体和核壳抗体动态:从常规献血中获取 COVID-19 康复血浆的意义。
背景:COVID-19 康复血浆(CCP)仍是免疫力低下患者的一种治疗选择;然而,目前美国食品药品管理局规定的尖峰抗体≥200 BAU/mL的合格阈值似乎相对较低。我们评估了接种过疫苗和/或感染过疫苗的重复献血者的序列样本中结合抗体(bAb)和中和抗体(nAb)的水平,以了解从常规采集的血浆成分中鉴定 CCP 的标准:将献血者分为四组:(1) 先感染后接种;(2) 先接种后在δ波或(3) Ω波期间感染;(4) 接种后未感染。使用报告病毒颗粒中和法测定 IgG Spike 和总核头状病毒 bAb,以及 S 变种和 nAb 滴度:结果:单独感染后的平均 S IgG bAb 峰值低于初次接种和加强接种后的峰值,而在先前接种过疫苗的供体中,δ和ω感染后的峰值较高。第一次感染/接种后 S IgG 的半衰期为 34 到 66 天,第二次感染/接种后可达 108 天。不同变异株的 S IgG bAb 和 nAb 水平相似,但奥米克龙变异株较低。在较高水平(混合免疫)下观察到的 nAb 与 bAb 的相关性优于目前 FDA CCP 的合格阈值:讨论:具有混合免疫力的捐献者所捐献的常规血浆在感染后 3-6 个月内具有较高的 S bAb 和较强的中和活性。在具有高 S IgG(>4000 BAU/mL)的捐献者中,无论是否出现 COVID-19 症状,>95% 的人都具有针对祖先和变异 S 的高 nAb 滴度(>500)。这些发现为制定基于检测的常规献血中 CCP 的合格标准提供了依据。
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来源期刊
Transfusion
Transfusion 医学-血液学
CiteScore
4.70
自引率
20.70%
发文量
426
审稿时长
1 months
期刊介绍: TRANSFUSION is the foremost publication in the world for new information regarding transfusion medicine. Written by and for members of AABB and other health-care workers, TRANSFUSION reports on the latest technical advances, discusses opposing viewpoints regarding controversial issues, and presents key conference proceedings. In addition to blood banking and transfusion medicine topics, TRANSFUSION presents submissions concerning patient blood management, tissue transplantation and hematopoietic, cellular, and gene therapies.
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