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感染MB-003抗体鸡尾酒疗法的非人灵长类动物中埃博拉病毒逃逸变体的出现

Emergence of Ebola Virus Escape Variants in Infected Nonhuman Primates Treated with the MB-003 Antibody Cocktail.

作者信息

Kugelman Jeffrey R, Kugelman-Tonos Johanny, Ladner Jason T, Pettit James, Keeton Carolyn M, Nagle Elyse R, Garcia Karla Y, Froude Jeffrey W, Kuehne Ana I, Kuhn Jens H, Bavari Sina, Zeitlin Larry, Dye John M, Olinger Gene G, Sanchez-Lockhart Mariano, Palacios Gustavo F

机构信息

Center for Genome Sciences, United States Army Medical Research Institute of Infectious Diseases (USAMRIID), Fort Detrick, Frederick, MD 21702, USA.

Molecular and Translational Sciences Division, United States Army Medical Research Institute of Infectious Diseases (USAMRIID), Fort Detrick, Frederick, MD 21702, USA.

出版信息

Cell Rep. 2015 Sep 29;12(12):2111-20. doi: 10.1016/j.celrep.2015.08.038. Epub 2015 Sep 10.

Abstract

MB-003, a plant-derived monoclonal antibody cocktail used effectively in treatment of Ebola virus infection in non-human primates, was unable to protect two of six animals when initiated 1 or 2 days post-infection. We characterized a mechanism of viral escape in one of the animals, after observation of two clusters of genomic mutations that resulted in five nonsynonymous mutations in the monoclonal antibody target sites. These mutations were linked to a reduction in antibody binding and later confirmed to be present in a viral isolate that was not neutralized in vitro. Retrospective evaluation of a second independent study allowed the identification of a similar case. Four SNPs in previously identified positions were found in this second fatality, suggesting that genetic drift could be a potential cause for treatment failure. These findings highlight the importance selecting different target domains for each component of the cocktail to minimize the potential for viral escape.

摘要

MB - 003是一种源自植物的单克隆抗体混合物,在治疗非人类灵长类动物的埃博拉病毒感染方面效果显著,但在感染后1天或2天开始使用时,无法保护6只动物中的2只。在观察到两组基因组突变导致单克隆抗体靶点出现5个非同义突变后,我们对其中一只动物的病毒逃逸机制进行了表征。这些突变与抗体结合减少有关,后来证实存在于一种在体外未被中和的病毒分离株中。对第二项独立研究的回顾性评估发现了一个类似病例。在这第二例死亡病例中,在先前确定的位置发现了4个单核苷酸多态性,这表明基因漂移可能是治疗失败的一个潜在原因。这些发现凸显了为混合物的每个成分选择不同靶域以尽量减少病毒逃逸可能性的重要性。

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