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首页> 外文期刊>Oncoimmunology. >Vectorization in an oncolytic vaccinia virus of an antibody, a Fab and a scFv against programmed cell death-1 (PD-1) allows their intratumoral delivery and an improved tumor-growth inhibition
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Vectorization in an oncolytic vaccinia virus of an antibody, a Fab and a scFv against programmed cell death-1 (PD-1) allows their intratumoral delivery and an improved tumor-growth inhibition

机译:抗体的溶瘤疫苗病毒中的升级性,Fab和SCFV针对编程的细胞死亡-1(PD-1)允许其肿瘤内递送和改善的肿瘤生长抑制

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摘要

We report here the successful vectorization of a hamster monoclonal IgG (namely J43) recognizing the murine Programmed cell death-1 (mPD-1) in Western Reserve (WR) oncolytic vaccinia virus. Three forms of mPD-1 binders have been inserted into the virus: whole antibody (mAb), Fragment antigen-binding (Fab) or single-chain variable fragment (scFv). MAb, Fab and scFv were produced and assembled with the expected patterns in supernatants of cells infected by the recombinant viruses. The three purified mPD-1 binders were able to block the binding of mPD-1 ligand to mPD-1 in vitro. Moreover, mAb was detected in tumor and in serum of C57BL/6 mice when the recombinant WR-mAb was injected intratumorally (IT) in B16F10 and MCA 205 tumors. The concentration of circulating mAb detected after IT injection was up to 1,900-fold higher than the level obtained after a subcutaneous (SC) injection (i.e., without tumor) confirming the virus tropism for tumoral cells and/or microenvironment. Moreover, the overall tumoral accumulation of the mAb was higher and lasted longer after IT injection of WR-mAb1, than after IT administration of 10 mu g of J43. The IT injection of viruses induced a massive infiltration of immune cells including activated lymphocytes (CD8(+) and CD4(+)). Interestingly, in the MCA 205 tumor model, WR-mAb1 and WR-scFv induced a therapeutic control of tumor growth similar to unarmed WR combined to systemically administered J43 and superior to that obtained with an unarmed WR. These results pave the way for next generation of oncolytic vaccinia armed with immunomodulatory therapeutic proteins such as mAbs.
机译:我们在此报告仓鼠单克隆IgG(即J43)的成功向量化识别西方储备(WR)溶瘤疫苗病毒中的鼠程序化细胞死亡-1(MPD-1)。已将三种形式的MPD-1粘合剂插入病毒中:全抗体(MAB),片段抗原结合(Fab)或单链可变片段(SCFV)。制备MAB,Fab和SCFV并用重组病毒感染的细胞上清液中的预期图案组装。三种纯化的MPD-1粘合剂能够阻断MPD-1配体的结合在体外。此外,当在B16F10和MCA 205肿瘤中妥善注射重组WR-MAB时,在肿瘤中检测MAB和C57BL / 6小鼠的血清。在注射后检测到循环mAb的浓度高于皮下(SC)注射(即,没有肿瘤)获得的水平高达1,900倍,证实肿瘤细胞和/或微环境的病毒性覆谱。此外,MAb的整体肿瘤积累较高并在注射WR-MAB1后持续时间,而不是在施用10μgJ43之后。 IT注射病毒诱导了免疫细胞的大规模渗透,包括活性淋巴细胞(CD8(+)和CD4(+))。有趣的是,在MCA 205肿瘤模型中,WR-MAB1和WR-SCFV诱导对肿瘤生长的治疗性控制类似于非武装的WR组合以系统施用的J43,优于用非武装的WR获得。这些结果铺平了下一代葡萄酒疫苗武装的免疫调节治疗蛋白如mAb。

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  • 来源
    《Oncoimmunology.》 |2016年第10期|共14页
  • 作者单位

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Inst Gustave Roussy Canc Campus GRCC Villejuif France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

    Transgene SA 400 Blvd Gonthier Parc Innovat CS80166 F-67405 Illkirch Graffenstaden France;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

    Monoclonal antibody; oncolytic virotherapy; PD-1; vaccinia virus; vectorization;

    机译:单克隆抗体;溶溶解的病毒;PD-1;痘苗病毒;矢量化;

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