Antibody Fc-binding profiles and ACE2 affinity to SARS-CoV-2 RBD variants.

IF 5.5 3区医学 Q1 IMMUNOLOGY

Medical Microbiology and Immunology Pub Date : 2023-08-01 DOI:10.1007/s00430-023-00773-w

Ebene R Haycroft, Samantha K Davis, Pradhipa Ramanathan, Ester Lopez, Ruth A Purcell, Li Lynn Tan, Phillip Pymm, Bruce D Wines, P Mark Hogarth, Adam K Wheatley, Jennifer A Juno, Samuel J Redmond, Nicholas A Gherardin, Dale I Godfrey, Wai-Hong Tham, Kevin John Selva, Stephen J Kent, Amy W Chung

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引用次数: 2

Abstract

Emerging SARS-CoV-2 variants, notably Omicron, continue to remain a formidable challenge to worldwide public health. The SARS-CoV-2 receptor-binding domain (RBD) is a hotspot for mutations, reflecting its critical role at the ACE2 interface during viral entry. Here, we comprehensively investigated the impact of RBD mutations, including 5 variants of concern (VOC) or interest-including Omicron (BA.2)-and 33 common point mutations, both on IgG recognition and ACE2-binding inhibition, as well as FcγRIIa- and FcγRIIIa-binding antibodies, in plasma from two-dose BNT162b2-vaccine recipients and mild-COVID-19 convalescent subjects obtained during the first wave using a custom-designed bead-based 39-plex array. IgG-recognition and FcγR-binding antibodies were decreased against the RBD of Beta and Omicron, as well as point mutation G446S, found in several Omicron sub-variants as compared to wild type. Notably, while there was a profound decrease in ACE2 inhibition against Omicron, FcγR-binding antibodies were less affected, suggesting that Fc functional antibody responses may be better retained against the RBD of Omicron in comparison to neutralization. Furthermore, while measurement of RBD-ACE2-binding affinity via biolayer interferometry showed that all VOC RBDs have enhanced affinity to human ACE2, we demonstrate that human ACE2 polymorphisms, E35K (rs1348114695) has reduced affinity to VOCs, while K26R (rs4646116) and S19P (rs73635825) have increased binding kinetics to the RBD of VOCs, potentially affecting virus-host interaction and, thereby, host susceptibility. Collectively, our findings provide in-depth coverage of the impact of RBD mutations on key facets of host-virus interactions.

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抗体fc结合谱和ACE2对SARS-CoV-2 RBD变体的亲和力。

新出现的SARS-CoV-2变体，特别是欧米克隆病毒，继续对全球公共卫生构成巨大挑战。SARS-CoV-2受体结合域(RBD)是突变的热点，反映了其在病毒进入ACE2界面中的关键作用。在这里，我们全面研究了RBD突变的影响，包括5个关注(VOC)或感兴趣的变体，包括Omicron (BA.2)和33个共同点突变，对IgG识别和ace2结合抑制，以及FcγRIIa和FcγRIIa结合抗体，来自两剂bnt162b2疫苗接种者和轻度covid -19恢复期受试者的血浆，在第一波使用定制设计的基于头部的39-plex阵列。与野生型相比，β和Omicron的RBD以及在几个Omicron亚变体中发现的点突变G446S的igg识别和fc γ r结合抗体降低。值得注意的是，虽然ACE2对Omicron的抑制作用显著降低，但Fcγ r结合抗体受到的影响较小，这表明与中和相比，Fc功能抗体对Omicron的RBD反应可能更好地保留。此外，虽然通过生物层干涉测量RBD-ACE2结合亲和力显示所有VOC RBD都增强了对人类ACE2的亲和力，但我们发现人类ACE2多态性E35K (rs1348114695)降低了对VOCs的亲和力，而K26R (rs4646116)和S19P (rs73635825)增加了与VOCs RBD的结合动力学，可能影响病毒与宿主的相互作用，从而影响宿主的易感性。总的来说，我们的研究结果深入报道了RBD突变对宿主-病毒相互作用关键方面的影响。

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来源期刊

Medical Microbiology and Immunology 医学-免疫学

CiteScore

10.60

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： Medical Microbiology and Immunology (MMIM) publishes key findings on all aspects of the interrelationship between infectious agents and the immune system of their hosts. The journal´s main focus is original research work on intrinsic, innate or adaptive immune responses to viral, bacterial, fungal and parasitic (protozoan and helminthic) infections and on the virulence of the respective infectious pathogens. MMIM covers basic, translational as well as clinical research in infectious diseases and infectious disease immunology. Basic research using cell cultures, organoid, and animal models are welcome, provided that the models have a clinical correlate and address a relevant medical question. The journal also considers manuscripts on the epidemiology of infectious diseases, including the emergence and epidemic spreading of pathogens and the development of resistance to anti-infective therapies, and on novel vaccines and other innovative measurements of prevention. The following categories of manuscripts will not be considered for publication in MMIM: submissions of preliminary work, of merely descriptive data sets without investigation of mechanisms or of limited global interest, manuscripts on existing or novel anti-infective compounds, which focus on pharmaceutical or pharmacological aspects of the drugs, manuscripts on existing or modified vaccines, unless they report on experimental or clinical efficacy studies or provide new immunological information on their mode of action, manuscripts on the diagnostics of infectious diseases, unless they offer a novel concept to solve a pending diagnostic problem, case reports or case series, unless they are embedded in a study that focuses on the anti-infectious immune response and/or on the virulence of a pathogen.