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A novel transferrin receptor-targeted hybrid peptide disintegrates cancer cell membrane to induce rapid killing of cancer cells

机译:靶向转铁蛋白受体的新型杂合肽分解癌细胞膜诱导癌细胞的快速杀伤

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摘要

BackgroundTransferrin receptor (TfR) is a cell membrane-associated glycoprotein involved in the cellular uptake of iron and the regulation of cell growth. Recent studies have shown the elevated expression levels of TfR on cancer cells compared with normal cells. The elevated expression levels of this receptor in malignancies, which is the accessible extracellular protein, can be a fascinating target for the treatment of cancer. We have recently designed novel type of immunotoxin, termed "hybrid peptide", which is chemically synthesized and is composed of target-binding peptide and lytic peptide containing cationic-rich amino acids components that disintegrates the cell membrane for the cancer cell killing. The lytic peptide is newly designed to induce rapid killing of cancer cells due to conformational change. In this study, we designed TfR binding peptide connected with this novel lytic peptide and assessed the cytotoxic activity in vitro and in vivo.
机译:背景转铁蛋白受体(TfR)是一种细胞膜相关糖蛋白,参与细胞对铁的吸收和细胞生长的调节。最近的研究表明,与正常细胞相比,TfR在癌细胞上的表达水平升高。该受体在恶性肿瘤中的表达水平升高,这是可及的细胞外蛋白,可以成为治疗癌症的迷人靶标。我们最近设计了一种新型的免疫毒素,称为“杂交肽”,它是化学合成的,由靶结合肽和含有富含阳离子的氨基酸成分的裂解肽组成,这些氨基酸可使细胞膜分解,从而杀死癌细胞。裂解肽是新设计的,用于诱导构象变化导致癌细胞的快速杀伤。在这项研究中,我们设计了与该新型裂解肽连接的TfR结合肽,并评估了体内和体外的细胞毒性活性。

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