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针对马尔堡病毒的保护性抗体的产生与特性分析

Generation and characterization of protective antibodies to Marburg virus.

作者信息

Froude Jeffrey W, Pelat Thibaut, Miethe Sebastian, Zak Samantha E, Wec Anna Z, Chandran Kartik, Brannan Jennifer Mary, Bakken Russell R, Hust Michael, Thullier Philippe, Dye John M

机构信息

a US Army Medical Research Institute for Infectious Disease (USAMRIID) , Fort Detrick , MD , USA.

b Unite de Biotechnologie des Anticorps, Institut de Recherche Biomedicale des Armees [IRBA-CRSSA] , La Tronche , France.

出版信息

MAbs. 2017 May/Jun;9(4):696-703. doi: 10.1080/19420862.2017.1299848. Epub 2017 Mar 13.

Abstract

Marburg virus (MARV) and Ebola virus (EBOV) have been a source of epidemics and outbreaks for several decades. We present here the generation and characterization of the first protective antibodies specific for wild-type MARV. Non-human primates (NHP), cynomolgus macaques, were immunized with viral-replicon particles expressing the glycoproteins (GP) of MARV (Ci67 isolate). An antibody fragment (single-chain variable fragment, scFv) phage display library was built after four immunogen injections, and screened against the GP of MARV. Sequencing of 192 selected clones identified 18 clones with distinct V and V sequences. Four of these recombinant antibodies (R4A1, R4B11, R4G2, and R3F6) were produced in the scFv-Fc format for in vivo studies. Mice that were challenged with wild-type Marburg virus (Ci67 isolate) receiving 100 µg of scFv-Fc on days -1, 1 and 3 demonstrated protective efficacies ranging from 75-100%. The amino-acid sequences of the scFv-Fcs are similar to those of their human germline counterparts, sharing an identity ranging between 68 and 100% to human germline immunoglobulin. These results demonstrate for the first time that recombinant antibodies offer protection against wild-type MARV, and suggest they may be promising candidates for further therapeutic development especially due to their human homology.

摘要

几十年来,马尔堡病毒(MARV)和埃博拉病毒(EBOV)一直是疫情和疾病暴发的源头。我们在此展示了针对野生型马尔堡病毒的首批保护性抗体的产生及特性。用表达马尔堡病毒(Ci67分离株)糖蛋白(GP)的病毒复制子颗粒免疫非人类灵长类动物(NHP)食蟹猴。在四次注射免疫原后构建了一个抗体片段(单链可变片段,scFv)噬菌体展示文库,并针对马尔堡病毒的GP进行筛选。对192个选定克隆进行测序,鉴定出18个具有不同V和V序列的克隆。其中四种重组抗体(R4A1、R4B11、R4G2和R3F6)以scFv-Fc形式制备用于体内研究。在第-1、1和3天接受100μg scFv-Fc的经野生型马尔堡病毒(Ci67分离株)攻击的小鼠,其保护效力在75%至100%之间。scFv-Fc的氨基酸序列与其人类种系对应序列相似,与人种系免疫球蛋白的同一性在68%至100%之间。这些结果首次证明重组抗体可为野生型马尔堡病毒提供保护,并表明它们可能是进一步治疗开发的有前景的候选物,特别是由于它们与人的同源性。

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