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首页> 外文期刊>Cancer letters >An EGF receptor targeting Ranpirnase-diabody fusion protein mediates potent antitumour activity in vitro and in vivo
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An EGF receptor targeting Ranpirnase-diabody fusion protein mediates potent antitumour activity in vitro and in vivo

机译:靶向Ranpirnase-双抗体融合蛋白的EGF受体在体内和体外介导有效的抗肿瘤活性

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Cytotoxic ribonucleases such as the leopard frog derivative Ranpirnase (Onconase (R)) have emerged as a valuable new class of cancer therapeutics. Clinical trials employing single agent Ranpirnase in cancer patients have demonstrated significant clinical activity and surprisingly low immunogenicity. However, dose-limiting toxicity due to unspecific uptake of the RNase into non-cancerous cells is reached at relatively low concentrations of > 1 mg/m(2). We have in the present study generated a dimeric anti-EGFR Ranpirnase-diabody fusion protein capable to deliver two Ranpirnase moieties per molecule to EGFR-positive tumour cells. We show that this compound mediated far superior efficacy for killing EGFR-positive tumour cells than a monomeric counterpart. Most importantly, cell killing was restricted to EGFR-positive target cells and no dose-limiting toxicity of Ranpirnase-diabody was observed in mice. These data indicate that by targeted delivery of Ranpirnase non-selective toxicity can be abolished and suggests Ranpirnase-diabody as a promising new drug for therapeutic interventions in EGFR-positive cancers. (c) 2014 Elsevier Ireland Ltd. All rights reserved.
机译:细胞毒性核糖核酸酶,例如豹蛙衍生物Ranpirnase(Onconase(R))已经成为一种有价值的新型癌症治疗剂。在癌症患者中使用单药Ranpirnase的临床试验证明了显着的临床活性和令人惊讶的低免疫原性。然而,由于相对低的浓度> 1 mg / m(2),达到了由于RNase非特异性摄取进入非癌细胞的剂量限制毒性。在本研究中,我们已经生成了一种二聚体抗EGFR Ranpirnase-双抗体融合蛋白,该蛋白能够将每个分子的两个Ranpirnase部分传递至EGFR阳性肿瘤细胞。我们表明,该化合物介导的杀死EGFR阳性肿瘤细胞的功效远胜于单体同类药物。最重要的是,细胞杀伤仅限于EGFR阳性靶细胞,在小鼠中未观察到Ranpirnase-双抗体的剂量限制性毒性。这些数据表明,通过Ranpirnase的靶向递送,可以消除非选择性毒性,并表明Ranpirnase-双价抗体是治疗EGFR阳性癌症的有希望的新药物。 (c)2014爱思唯尔爱尔兰有限公司。保留所有权利。

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