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引用次数: 0

摘要

SARS-CoV2组粒变异亚谱系在世界范围内迅速传播,主要是由于它们的免疫逃避特性。这使得很大一部分人口面临严重疾病的风险,并强调需要抗sars - cov -2药物,以有效对抗易感患者的新菌株。骆驼纳米体由于其高稳定性、易于大规模生产和通过吸入给药的潜力而成为有吸引力的治疗候选者。在这里,我们对rbd特异性纳米体W25进行了表征,该纳米体是我们之前从羊驼中分离出来的,与所有其他SARS-CoV2变体相比,它对Omicron谱系BA.1表现出优越的中和活性。对W25与SARS-CoV2刺突表面糖蛋白复合物的结构分析表明,W25与之前批准用于紧急使用的任何抗体未覆盖的RBD表位结合。此外,我们发现W25还能结合来自新出现的更具传染性的Omicron BA.2谱系的刺突蛋白,具有小摩尔亲和力。W25在多种SARS-CoV-2变异感染模型中的预防和治疗作用的体内评估,以及W25在小鼠中的生物分布分析,显示了良好的临床前特性。总之,这些数据支持W25的优先级,以进一步的临床开发。
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Title
: The SARS-CoV2 Omicron variant sub-lineages spread rapidly through the world, mostly due to their immune-evasive properties. This has put a significant part of the population at risk for severe disease and underscores the need for anti-SARS-CoV-2 agents that are effective against emergent strains in vulnerable patients. Camelid nanobodies are attractive therapeutic candidates due to their high stability, ease of large-scale production and potential for delivery via inhalation. Here, we characterize the RBD-specific nanobody W25, which we previously isolated from an alpaca, and show superior neutralization activity towards Omicron lineage BA.1 in comparison to all other SARS-CoV2 variants. Structure analysis of W25 in complex with the SARS-CoV2 spike surface glycoprotein shows that W25 engages an RBD epitope not covered by any of the antibodies previously approved for emergency use. Furthermore, we show that W25 also binds the spike protein from the emerging, more infectious Omicron BA.2 lineage with picomolar affinity. In vivo evaluation of W25 prophylactic and therapeutic treatments across multiple SARS-CoV-2 variant infection models, together with W25 biodistribution analysis in mice, demonstrates favorable preclinical properties. Together, these data endorse prioritization of W25 for further clinical development.
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