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Modular Pore-Forming Immunotoxins with Caged Cytotoxicity Tailored by Directed Evolution

机译:模块化孔隙形成免疫毒素,具有通过定向演进量身定制的笼式细胞毒性

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摘要

Immunotoxins are proteins containing a cell-targeting element linked to a toxin that are under investigation for next-generation cancer treatment. However, these agents are difficult to synthesize, chemically heterogeneous, expensive, and show toxicity toward healthy cells. In this work, we describe the synthesis and characterization of a new type of immunotoxin that showed exquisite selectivity toward targeted cells. In our construct, targeting molecules were covalently attached or genetically fused to oligomeric pore-forming toxins. The activity of the immunotoxin was then caged by fusing a soluble protein to the transmembrane domain and activated via cleavage with furin, which is a protease that is overexpressed in many cancer cells. During the several coupling steps, directed evolution allowed the efficient synthesis of the molecules in E. coli cells, as well as selection for further specificity toward targeted cells. The final construct showed no off-target activity, while acquiring an additional degree of specificity toward the targeted cells upon activation. The pore-forming toxins described here do not require internalization to operate, while the many protomeric subunits can be individually modified to refine target specificity.
机译:免疫毒素是含有与在下一代癌症治疗的毒素中连接的细胞靶向元素的蛋白质。然而,这些试剂难以合成,化学异质,昂贵,并向健康细胞显示毒性。在这项工作中,我们描述了一种新型免疫毒素的合成和表征,其对靶向细胞显示出精确的选择性。在我们的构建体中,将靶向分子共价附着或遗传地融合给低聚孔形成毒素。然后通过将可溶性蛋白质融合到跨膜结构域并通过用Furin的切割而活化,通过肉蛋白激活免疫毒素的活性,这是在许多癌细胞中过表达的蛋白酶。在几个耦合步骤期间,定向进化允许有效地合成大肠杆菌细胞中的分子,以及对靶向细胞的进一步特异性的选择。最终构建体显示出不靶向活性,同时在激活后获得靶向靶细胞的额外特异性。这里描述的孔形成毒素不需要内化以操作,而许多蛋白质亚基可以单独修改以细化目标特异性。

著录项

  • 来源
    《ACS Chemical Biology》 |2018年第11期|共8页
  • 作者单位

    Univ Groningen Groningen Biomol Sci &

    Biotechnol Inst NL-9747 AG Groningen Netherlands;

    Univ Groningen Groningen Biomol Sci &

    Biotechnol Inst NL-9747 AG Groningen Netherlands;

    Univ Groningen Groningen Biomol Sci &

    Biotechnol Inst NL-9747 AG Groningen Netherlands;

    Univ Lisbon Fac Med Inst Med Mol Ave Prof Egas Moniz P-1649028 Lisbon Portugal;

    Univ Lisbon Fac Med Inst Med Mol Ave Prof Egas Moniz P-1649028 Lisbon Portugal;

    Univ Groningen Groningen Biomol Sci &

    Biotechnol Inst NL-9747 AG Groningen Netherlands;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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