In vitro generated antibodies guide thermostable ADDomer nanoparticle design for nasal vaccination and passive immunization against SARS-CoV-2

Q2 Medicine Antibody Therapeutics Pub Date : 2023-10-17 DOI:10.1093/abt/tbad024
Dora Buzas, H Adrian Bunzel, Oskar Staufer, Emily J Milodowski, Grace L Edmunds, Joshua C Bufton, Beatriz V Vidana Mateo, Sathish K N Yadav, Kapil Gupta, Charlotte Fletcher, Maia Kavanagh Williamson, Alexandra Harrison, Ufuk Borucu, Julien Capin, Ore Francis, Georgia Balchin, Sophie Hall, Mirella Vivoli Vega, Fabien Durbesson, Srikanth Lingappa, Renaud Vincentelli, Joe Roe, Linda Wooldridge, Rachel Burt, J L Ross Anderson, Adrian J Mulholland, Jonathan Hare, Mick Bailey, Andrew D Davidson, Adam Finn, David Morgan, Jamie Mann, Joachim Spatz, Frederic Garzoni, Christiane Schaffitzel, Imre Berger
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引用次数: 1

Abstract

Abstract Background Due to COVID-19, pandemic preparedness emerges as a key imperative, necessitating new approaches to accelerate development of reagents against infectious pathogens. Methods Here, we developed an integrated approach combining synthetic, computational and structural methods with in vitro antibody selection and in vivo immunization to design, produce and validate nature-inspired nanoparticle-based reagents against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Results Our approach resulted in two innovations: (i) a thermostable nasal vaccine called ADDoCoV, displaying multiple copies of a SARS-CoV-2 receptor binding motif derived epitope and (ii) a multivalent nanoparticle superbinder, called Gigabody, against SARS-CoV-2 including immune-evasive variants of concern (VOCs). In vitro generated neutralizing nanobodies and electron cryo-microscopy established authenticity and accessibility of epitopes displayed by ADDoCoV. Gigabody comprising multimerized nanobodies prevented SARS-CoV-2 virion attachment with picomolar EC50. Vaccinating mice resulted in antibodies cross-reacting with VOCs including Delta and Omicron. Conclusion Our study elucidates Adenovirus-derived dodecamer (ADDomer)-based nanoparticles for use in active and passive immunization and provides a blueprint for crafting reagents to combat respiratory viral infections.
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体外生成的抗体指导抗SARS-CoV-2鼻腔疫苗接种和被动免疫的热稳定性增聚体纳米颗粒设计
背景由于2019冠状病毒病(COVID-19),大流行防范成为当务之急,需要新的方法来加速开发针对传染性病原体的试剂。方法将合成、计算和结构方法与体外抗体选择和体内免疫相结合,设计、生产和验证基于自然启发的纳米颗粒的抗严重急性呼吸综合征冠状病毒2 (SARS-CoV-2)试剂。我们的方法产生了两项创新:(i)一种称为ADDoCoV的耐热鼻疫苗,显示了SARS-CoV-2受体结合基元衍生的表位的多个拷贝;(ii)一种称为Gigabody的多价纳米颗粒超粘合剂,用于对抗SARS-CoV-2,包括免疫逃避型关注变体(VOCs)。体外生成的中和纳米体和电子冷冻显微镜证实了ADDoCoV显示的表位的真实性和可及性。由多聚纳米体组成的千兆体以微摩尔EC50阻止SARS-CoV-2病毒粒子附着。给小鼠接种疫苗会导致抗体与包括Delta和Omicron在内的VOCs发生交叉反应。我们的研究阐明了基于腺病毒衍生的十二聚体(ADDomer)的纳米颗粒用于主动和被动免疫,并为制作对抗呼吸道病毒感染的试剂提供了蓝图。
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来源期刊
Antibody Therapeutics
Antibody Therapeutics Medicine-Immunology and Allergy
CiteScore
8.70
自引率
0.00%
发文量
30
审稿时长
8 weeks
期刊最新文献
AI-based antibody discovery platform identifies novel, diverse, and pharmacologically active therapeutic antibodies against multiple SARS-CoV-2 strains. FcRider: a recombinant Fc nanoparticle with endogenous adjuvant activities for hybrid immunization. A pan-allelic human SIRPα-blocking antibody, ES004-B5, promotes tumor killing by enhancing macrophage phagocytosis and subsequently inducing an effective T-cell response. Correction to: A case study of a bispecific antibody manufacturability assessment and optimization during discovery stage and its implications. The process using a synthetic library that generates multiple diverse human single domain antibodies.
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