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Bispecific light T-cell engagers for gene-based immunotherapy of epidermal growth factor receptor (EGFR)-positive malignancies

机译:基于表皮生长因子受体(EGFR)的基因基因免疫治疗的双特异性轻型T细胞烘焙剂 - 阳性恶性肿瘤

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摘要

The recruitment of T-cells by bispecific antibodies secreted from adoptively transferred, gene-modified autologous cells has shown satisfactory results in preclinical cancer models. Even so, the approach's translation into the clinic will require incremental improvements to its efficacy and reduction of its toxicity. Here, we characterized a tandem T-cell recruiting bispecific antibody intended to benefit gene-based immunotherapy approaches, which we call the light T-cell engager (LiTE), consisting of an EGFR-specific single-domain V-HH antibody fused to a CD3-specific scFv. We generated two LiTEs with the anti-EGFR V-HH and the anti-CD3 scFv arranged in both possible orders. Both constructs were well expressed in mammalian cells as highly homogenous monomers in solution with molecular weights of 43 and 41 kDa, respectively. In situ secreted LiTEs bound the cognate antigens of both parental antibodies and triggered the specific cytolysis of EGFR-expressing cancer cells without inducing T-cell activation and cytotoxicity spontaneously or against EGFR-negative cells. Light T-cell engagers are, therefore, suitable for future applications in gene-based immunotherapy approaches.
机译:通过从普通转移分泌的基因改性的自体细胞分泌的双特异性抗体募集T细胞已显示出令人满意的导致临床前癌症模型。即便如此,该方法的翻译进入诊所将需要增量改善其疗效和减少其毒性。在这里,我们表征了促进旨在促进基于基于基因的免疫疗法方法的双特异性抗体,其呼叫轻型T细胞(Lite),由融合的EGFR特异性单结构域V-HH抗体组成CD3特定的SCFV。我们使用反eGFR V-HH生成了两个亮度,并在可能的订单中排列的防CD3 SCFV。两种构建体在哺乳动物细胞中均为高度均匀的单体,分子量分别为43和41kDa。原位分泌的Lites与亲本抗体的同源抗原结合并引发了表达EGFR表达癌细胞的特异性细胞解,而不自发地诱导T细胞活化和细胞毒性或针对EGFR阴性细胞。因此,轻型T细胞烘焙器适用于基于基因的免疫疗法方法中的未来应用。

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