Monoclonal antibodies against the spike protein alter the endogenous humoral response to SARS-CoV-2 vaccination and infection

IF 15.8 1区 医学 Q1 CELL BIOLOGY
Christopher D. Petro, Andrea T. Hooper, Avery Peace, Kusha Mohammadi, Will Eagan, Sayda M. Elbashir, Anthony DiPiazza, Daniel Makrinos, Kristen Pascal, Pooja Bandawane, Mauricio Durand, Ranu Basu, Alida Coppi, Bei Wang, Jacquelynn Golubov, Seblewongel Asrat, Samit Ganguly, Ellen-Marie Koehler-Stec, Matthew F. Wipperman, George Ehrlich, Ana M. Gonzalez Ortiz, Flonza Isa, Mark G. Lewis, Hanne Andersen, Bret J. Musser, Marcela Torres, Wen-Yi Lee, Darin Edwards, Dimitris Skokos, Jamie Orengo, Matthew Sleeman, Thomas Norton, Meagan O’Brien, Eduardo Forleo-Neto, Gary A. Herman, Jennifer D. Hamilton, Andrew J. Murphy, Christos A. Kyratsous, Alina Baum
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Abstract

Increased use of antiviral monoclonal antibodies (mAbs) for treatment and prophylaxis necessitates better understanding of their impact on endogenous immunity to vaccines and viruses. The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic presented an opportunity to study immunity in individuals who received antiviral mAbs and were subsequently immunized with vaccines encoding the mAb-targeted viral spike antigen. Here, we describe the impact of administration of an antibody combination, casirivimab plus imdevimab (CAS+IMD), on immune responses to subsequent SARS-CoV-2 vaccination in humans, nonhuman primates, and mice. The presence of CAS+IMD at the time of vaccination led to a specific diminishment of vaccine-elicited pseudovirus neutralizing antibody titers without overall dampening of spike protein–directed immune responses, including antibody, B cell, and T cell responses. The impact on pseudovirus neutralizing titers extended to other therapeutic anti–spike protein antibodies when used as either monotherapy or combination therapy. The specific reduction in pseudovirus neutralizing titers was the result of epitope masking, a phenomenon where specific epitopes are bound by high-affinity antibodies and blocked from B cell recognition. Encouragingly, this reduction in pseudovirus neutralizing titers was reversible with additional booster vaccination. Moreover, by assessing the antiviral immune response in SARS-CoV-2–infected individuals treated therapeutically with CAS+IMD, we demonstrated alteration of antiviral humoral immunity in those who had received mAb therapy, but only in those individuals who had yet to start mounting their natural immune response at the time of mAb treatment. Together, these data demonstrate that antiviral mAbs can alter endogenous humoral immunity during vaccination or infection.
针对尖峰蛋白的单克隆抗体改变了接种SARS-CoV-2疫苗和感染后的内源性体液反应
由于越来越多地使用抗病毒单克隆抗体(mAbs)进行治疗和预防,因此有必要更好地了解它们对疫苗和病毒内源性免疫的影响。严重急性呼吸系统综合征冠状病毒 2(SARS-CoV-2)大流行为研究接受抗病毒 mAbs 并随后接种了编码 mAb 靶向病毒尖抗原疫苗的个体的免疫力提供了机会。在这里,我们描述了在人类、非人灵长类动物和小鼠体内施用卡西利韦单抗加伊莫德单抗(CAS+IMD)的抗体组合对随后接种 SARS-CoV-2 疫苗的免疫反应的影响。接种疫苗时使用 CAS+IMD 会导致疫苗诱导的伪病毒中和抗体滴度下降,但不会全面抑制尖峰蛋白导向的免疫反应,包括抗体、B 细胞和 T 细胞反应。对伪病毒中和抗体滴度的影响还延伸到了其他治疗性抗尖峰蛋白抗体的单一疗法或联合疗法。伪病毒中和滴度的特定降低是表位掩蔽的结果,即特定表位被高亲和力抗体结合并阻止 B 细胞识别的现象。令人鼓舞的是,假病毒中和滴度的降低在额外接种加强疫苗后是可逆的。此外,通过评估接受 CAS+IMD 治疗的 SARS-CoV-2 感染者的抗病毒免疫反应,我们发现接受过 mAb 治疗的感染者的抗病毒体液免疫发生了变化,但这种变化只发生在接受 mAb 治疗时尚未开始启动自然免疫反应的感染者身上。这些数据共同证明,抗病毒 mAb 可在疫苗接种或感染过程中改变内源性体液免疫。
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来源期刊
Science Translational Medicine
Science Translational Medicine CELL BIOLOGY-MEDICINE, RESEARCH & EXPERIMENTAL
CiteScore
26.70
自引率
1.20%
发文量
309
审稿时长
1.7 months
期刊介绍: Science Translational Medicine is an online journal that focuses on publishing research at the intersection of science, engineering, and medicine. The goal of the journal is to promote human health by providing a platform for researchers from various disciplines to communicate their latest advancements in biomedical, translational, and clinical research. The journal aims to address the slow translation of scientific knowledge into effective treatments and health measures. It publishes articles that fill the knowledge gaps between preclinical research and medical applications, with a focus on accelerating the translation of knowledge into new ways of preventing, diagnosing, and treating human diseases. The scope of Science Translational Medicine includes various areas such as cardiovascular disease, immunology/vaccines, metabolism/diabetes/obesity, neuroscience/neurology/psychiatry, cancer, infectious diseases, policy, behavior, bioengineering, chemical genomics/drug discovery, imaging, applied physical sciences, medical nanotechnology, drug delivery, biomarkers, gene therapy/regenerative medicine, toxicology and pharmacokinetics, data mining, cell culture, animal and human studies, medical informatics, and other interdisciplinary approaches to medicine. The target audience of the journal includes researchers and management in academia, government, and the biotechnology and pharmaceutical industries. It is also relevant to physician scientists, regulators, policy makers, investors, business developers, and funding agencies.
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