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可抵御新冠病毒XBB变种的强效双价纳米抗体构建体。

Potent bivalent nanobody constructs that protect against the SARS-CoV-2 XBB variant.

作者信息

Halfmann Peter J, Lee Jeong Soo, McArthur Nikki, Gupta Ojas, Kawaoka Yoshihiro, Kane Ravi S

机构信息

Department of Pathobiological Sciences, Influenza Research Institute, School of Veterinary Medicine, University of Wisconsin, Madison, WI, USA.

School of Chemical & Biomolecular Engineering, Georgia Institute of Technology, Atlanta, GA, USA.

出版信息

Npj Viruses. 2025 Mar 13;3(1):19. doi: 10.1038/s44298-025-00101-4.

Abstract

Most antibody-based therapeutics approved for SARS-CoV-2 treatment have shown greatly reduced neutralization activity against emerging Omicron variants. To target recent Omicron variants, we developed XBB-specific antibody-like therapeutics by screening a yeast surface-displayed single-domain antibody library against the receptor binding domain of the XBB spike protein. Three lead nanobodies, XNb 4.13, XNb 4.14, and XNb 4.15, were selected based on their binding affinity to the XBB spike protein and were fused to a mouse Fc domain. While all three constructs showed sub-nanomolar binding affinities to the XBB S protein, XNb 4.13-Fc and XNb 4.14-Fc also neutralized XBB in vitro. Intraperitoneal injection of XNb 4.13-Fc and XNb 4.14-Fc and intranasal delivery of XNb 4.13-Fc protected transgenic mice from a challenge with XBB virus with a significant reduction in viral lung titers post-infection. These antibody-like constructs identified using yeast surface display have potential as therapeutics that can protect against SARS-CoV-2 XBB variants.

摘要

大多数被批准用于治疗新冠病毒的基于抗体的疗法,对新出现的奥密克戎变种的中和活性已大幅降低。为了针对近期的奥密克戎变种,我们通过用酵母表面展示的单域抗体文库针对XBB刺突蛋白的受体结合域进行筛选,开发了XBB特异性抗体样疗法。基于它们与XBB刺突蛋白的结合亲和力,选择了三种先导纳米抗体XNb 4.13、XNb 4.14和XNb 4.15,并将它们与小鼠Fc结构域融合。虽然所有三种构建体对XBB S蛋白都显示出亚纳摩尔级的结合亲和力,但XNb 4.13-Fc和XNb 4.14-Fc在体外也能中和XBB。腹腔注射XNb 4.13-Fc和XNb 4.14-Fc以及鼻内递送XNb 4.13-Fc可保护转基因小鼠免受XBB病毒攻击,感染后病毒肺滴度显著降低。利用酵母表面展示鉴定出的这些抗体样构建体有潜力作为预防新冠病毒XBB变种的治疗药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b06/11906887/2916def8e664/44298_2025_101_Fig1_HTML.jpg

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