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首页> 外文期刊>International journal of peptide research and therapeutics >Design of a Tumor Homing Cell-Penetrating Peptide for Drug Delivery
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Design of a Tumor Homing Cell-Penetrating Peptide for Drug Delivery

机译:用于药物递送的肿瘤归巢细胞穿透肽的设计

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The major drawbacks with conventional cancer chemotherapy are the lack of satisfactory specificity towards tumor cells and poor antitumor activity. In order to improve these characteristics, chemotherapeutic drugs can be conjugated to targeting moieties e.g. to peptides with the ability to recognize cancer cells. We have previously reported that combining a tumor homing peptide with a cell-penetrating peptide yields a chimeric peptide with tumor cell specificity that can carry cargo molecules inside the cells. In the present study, we have used a linear breast tumor homing peptide, CREKA, in conjunction with a cell-penetrating peptide, pVEC. This new chimeric peptide, CREKA-pVEC, is more convenient to synthesize and moreover it is better in translocating cargo molecules inside cancer cells as compared to previously published PEGA-pVEC peptide. This study demonstrates that CREKA-pVEC is a suitable vehicle for targeted intracellular delivery of a DNA alkylating agent, chlorambucil, as the chlorambucil-peptide conjugate was substantially better at killing cancer cells in vitro than the anticancer drug alone.
机译:常规癌症化学疗法的主要缺点是缺乏对肿瘤细胞的令人满意的特异性和差的抗肿瘤活性。为了改善这些特性,可以将化学治疗药物与靶向部分缀合。具有识别癌细胞能力的肽。我们以前曾报道过,将肿瘤归巢肽与可穿透细胞的肽结合可产生具有肿瘤细胞特异性的嵌合肽,该嵌合肽可在细胞内携带货物分子。在本研究中,我们将线性乳腺肿瘤归巢肽CREKA与细胞穿透肽pVEC结合使用。与以前发布的PEGA-pVEC肽相比,这种新的嵌合肽CREKA-pVEC更易于合成,而且在转运癌细胞内的货物分子方面更好。这项研究表明,CREKA-pVEC是DNA烷基化剂苯丁酸氮芥靶向细胞内递送的合适媒介物,因为苯丁酸氮芥-肽结合物在体外杀死癌细胞方面比单独使用抗癌药物要好得多。

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