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转染色体牛产生的抗汉坦病毒出血热综合征人IgG具有强大的汉坦病毒中和活性且在动物模型中具有保护作用。

Anti-HFRS Human IgG Produced in Transchromosomic Bovines Has Potent Hantavirus Neutralizing Activity and Is Protective in Animal Models.

作者信息

Perley Casey C, Brocato Rebecca L, Wu Hua, Bausch Christoph, Karmali Priya P, Vega Jerel B, Cohen Melanie V, Somerville Brandon, Kwilas Steven A, Principe Lucia M, Shamblin Joshua, Chivukula Padmanabh, Sullivan Eddie, Hooper Jay W

机构信息

Virology Division, United States Army Medical Research Institute of Infectious Diseases, Frederick, MD, United States.

SAB Biotherapeutics Inc., Sioux Falls, SD, United States.

出版信息

Front Microbiol. 2020 May 7;11:832. doi: 10.3389/fmicb.2020.00832. eCollection 2020.

Abstract

We explored an emerging technology to produce anti-Hantaan virus (HTNV) and anti-Puumala virus (PUUV) neutralizing antibodies for use as pre- or post-exposure prophylactics. The technology involves hyperimmunization of transchomosomic bovines (TcB) engineered to express human polyclonal IgG antibodies with HTNV and PUUV DNA vaccines encoding GG glycoproteins. For the anti-HTNV product, TcB was hyperimmunized with HTNV DNA plus adjuvant or HTNV DNA formulated using lipid nanoparticles (LNP). The LNP-formulated vaccine yielded fivefold higher neutralizing antibody titers using 10-fold less DNA. Human IgG purified from the LNP-formulated animal (SAB-159), had anti-HTNV neutralizing antibody titers >100,000. SAB-159 was capable of neutralizing pseudovirions with monoclonal antibody escape mutations in G and G demonstrating neutralization escape resistance. SAB-159 protected hamsters from HTNV infection when administered pre- or post-exposure, and limited HTNV infection in a marmoset model. An LNP-formulated PUUV DNA vaccine generated purified anti-PUUV IgG, SAB-159P, with a neutralizing antibody titer >600,000. As little as 0.33 mg/kg of SAB-159P protected hamsters against PUUV infection for pre-exposure and 10 mg/kg SAB-159P protected PUUV-infected hamsters post-exposure. These data demonstrate that DNA vaccines combined with the TcB-based manufacturing platform can be used to rapidly produce potent, human, polyclonal, escape-resistant anti-HTNV, and anti-PUUV neutralizing antibodies that are protective in animal models.

摘要

我们探索了一种新兴技术,用于生产抗汉坦病毒(HTNV)和抗普马拉病毒(PUUV)的中和抗体,用作暴露前或暴露后预防药物。该技术涉及对经基因工程改造以表达人多克隆IgG抗体的转基因牛(TcB)进行超免疫,使用编码G糖蛋白的HTNV和PUUV DNA疫苗。对于抗HTNV产品,用HTNV DNA加佐剂或用脂质纳米颗粒(LNP)配制的HTNV DNA对TcB进行超免疫。用LNP配制的疫苗使用的DNA量减少10倍,中和抗体滴度提高了五倍。从用LNP配制的动物(SAB-159)中纯化的人IgG,其抗HTNV中和抗体滴度>100,000。SAB-159能够中和在G和G中具有单克隆抗体逃逸突变的假病毒,证明其具有中和逃逸抗性。在暴露前或暴露后给予SAB-159可保护仓鼠免受HTNV感染,并在狨猴模型中限制HTNV感染。用LNP配制的PUUV DNA疫苗产生了纯化的抗PUUV IgG,即SAB-159P,其中和抗体滴度>600,000。低至0.33 mg/kg的SAB-159P可在暴露前保护仓鼠免受PUUV感染,而10 mg/kg的SAB-159P可在暴露后保护感染PUUV的仓鼠。这些数据表明,DNA疫苗与基于TcB的生产平台相结合,可用于快速生产强效、人源、多克隆、抗逃逸的抗HTNV和抗PUUV中和抗体,这些抗体在动物模型中具有保护作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fb52/7252588/be5644294bea/fmicb-11-00832-g001.jpg

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