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新型肽的设计与合成及其用于选择性检测癌细胞的研究

Design and synthesis of a novel peptide for selective detection of cancer cells.

机构信息

Organic and Bioorganic Chemistry Laboratory, CSIR-Central Leather Research Institute, Chennai, India.

Biological Materials Laboratory, CSIR-Central Leather Research Institute, Chennai, India.

出版信息

Chem Biol Drug Des. 2020 Jun;95(6):610-623. doi: 10.1111/cbdd.13675. Epub 2020 Apr 8.

DOI:10.1111/cbdd.13675
PMID:32147880
Abstract

Using a minimalist approach, an 11-residue peptide (Peptide 1) tagged with rhodamine fluorophore was designed and synthesized for selective detection of cancer cells. Peptide 1 contains RGD and NGR motifs to bind, respectively, integrins and aminopeptidase CD13, which are over expressed in cancer cells. Surface tension measurements revealed that peptide 1 possess surface-active property owing to the overall hydrophobicity and cationic nature of the peptide. Peptide 1 displays cancer cell-selective binding at ≤5.0 µM concentrations, while peptide 2 (randomized sequence of 1) shows non-selective binding to normal and cancer cells. Fluorescence microscopy and FACS analysis demonstrated the intracellular localization of peptide 1 in three different cancer cell lines, confirming the role of RGD and NGR motifs. Cytotoxicity assay exhibited the viability of normal and cancer cells up to 100 µM concentrations of peptide 1. Steady-state fluorescence measurements disclosed the preferential interactions of the peptide 1 with anionic POPC/POPG bilayers rather than with zwitterionic POPC lipid bilayers. Circular dichroism studies showed minimal changes in the secondary structure of peptide 1 upon binding with the anionic lipid bilayers. Peptide 1 is largely unordered, non-toxic, and useful for identification of cancer cells. Peptide 1 provides a template for designing drug-loaded peptides for targeted delivery into cancer cells.

摘要

采用简约主义方法,设计并合成了一种带有罗丹明荧光团的 11 残基肽(肽 1),用于选择性检测癌细胞。肽 1 包含 RGD 和 NGR 基序,分别与癌细胞中过度表达的整合素和氨肽酶 CD13 结合。表面张力测量表明,由于肽的整体疏水性和阳离子性质,肽 1 具有表面活性。肽 1 在 ≤5.0 μM 浓度下表现出对癌细胞的选择性结合,而肽 2(肽 1 的随机序列)对正常和癌细胞表现出非选择性结合。荧光显微镜和流式细胞术分析表明,肽 1 在三种不同的癌细胞系中具有细胞内定位,证实了 RGD 和 NGR 基序的作用。细胞毒性测定显示,正常和癌细胞在高达 100 μM 浓度的肽 1 下仍具有活力。稳态荧光测量表明,肽 1 优先与阴离子 POPC/POPG 双层而不是两性离子 POPC 脂质双层相互作用。圆二色性研究表明,肽 1 与阴离子脂质双层结合时,二级结构几乎没有变化。肽 1 是无毒性的,且对识别癌细胞有用。肽 1 为设计用于靶向递送至癌细胞的载药肽提供了模板。

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